Patent Description:
Organic light emitting diodes (OLED) are a new generation of full-color display and lighting technology. Compared to liquid crystal displays with slow response speed, small viewing angle, the need for backlighting, high energy consumption, and other shortcomings, OLED, as an autonomous light-emitting device, has the following advantages such as no need for backlighting, energy-saving, low drive voltage, fast response speed, high resolution and contrast, wide viewing angle, and outstanding low-temperature performance. OLED devices can be made thinner and can be made into a flexible structure. In addition, it has the advantages of low production cost and a simple production process and allows for large-scale production. Therefore, OLED has a wide and huge application prospect in high-end electronics and aerospace. With the gradual increase of investment, further development, and upgrading of production equipment, OLEDs have a very wide range of application scenarios and prospects in the future. Platinium complexes used in OLEDs are disclosed in <CIT>.

The core of OLED development is the design and development of light emitting materials. Currently applied OLED devices, the light emitting layer almost all use the host-guest luminescence system mechanism, that is, doping the guest light emitting material in the host. The energy system of the host material is generally larger than that of the guest light emitting material, and the energy will be transferred from the host material to the guest material so that the guest material is excited and emits light. Commonly used organic phosphorescent guest materials are typically heavy metal atoms such as iridium (III), platinum (II), palladium (II), and the like. Commonly used phosphorescent organic materials mCBP (<NUM>,<NUM>'-bis(<NUM>-carbazolyl)-biphenyl) and <NUM>, <NUM>-mCPy (<NUM>,<NUM>-bis(<NUM>-carbazolyl)-pyridine) have high efficiency and high triplet energy levels. When they are used as organic materials, triplet energy can be efficiently transferred from the light-emitting organic material to the guest phosphorescent light emitting material. However, due to the easy hole transport and difficult electron flow properties of mCBP and the poor hole transport of <NUM>,<NUM>-mCPy, the charge of the light emitting layer is not balanced, and as a result, the current efficiency of the device is reduced. Furthermore, the currently applied heavy metal phosphorescent organic complex molecules are cyclic metallic iridium(III) complex molecules with a limited number. The content of metallic platinum in the earth's crust and the annual production in the world are about ten times that of metallic iridium, and the price of IrCl<NUM>. H<NUM>O used for the preparation of iridium(III) complex phosphorescent materials is much higher than that of PtCl<NUM> used for the preparation of platinum(II) complex phosphorescent materials. In addition, the preparation of iridium(III) complex phosphorescent materials involves a four-step reaction including iridium(III)-containing dimers, iridium(III) intermediate ligand exchange, synthesis of mer-iridium(III) complex, and isomer conversion of mer-to-fac-iridium(III) complex, which greatly reduces the total yield, greatly reduces the utilization of the raw material IrCl<NUM>·H<NUM>O, and increases the cost of preparation of iridium(III) complex phosphorescent material. In contrast, the preparation of a platinum (II) complex phosphorescent material has only the last step of metallization of ligands involving the reaction of platinum salts, and the high utilization rate of platinum elements can further reduce the preparation cost of Pt(II) complex phosphorescent materials. In conclusion, the preparation cost of the Pt(II) complex phosphorescent material is much lower than that of the iridium(III) complex phosphorescent material. However, there are still some technical difficulties in the development of platinum complex materials and devices, for example, how to reduce the height of the shoulder peaks in the emission spectrum in order to improve the color purity of the molecular luminescence of the material? This issue is particularly important for blue and deep blue light emitting materials because of their significant impact on the efficiency and energy utilization of top-emitting devices for commercial applications. Therefore, there is a need to develop novel phosphorescent metal platinum (II) complexes.

In view of the above, it is an object of the present invention to provide a fused ring carbazole tetradentate metal platinum (II) complex and use thereof. The introduction of a five-membered heterocyclic system such as benzofuran or benzothiophene into the <NUM>, <NUM>-position of carbazole in the present invention can increase the ratio of the local state (LE) in the excited triplet state of the cyclic tetradentate platinum (II) complex leads to a lower shoulder peak, which improves the molecular luminescence color purity of the materials. The complex provided can be prepared as an organic electroluminescence device as a light emitting layer so that the device has excellent properties. It can increase the current efficiency of organic electroluminescence devices, improve device life, and also reduce the operating voltage of components.

In order to achieve the technical objectives above, the technical solution of the present invention is as follows.

The present invention provides a fused ring carbazole tetradentate metal platinum (II) complex having the structure shown in formula (I):
<CHM>
where X is selected from O or S; R<NUM>-R<NUM> each independently represent mono- to maximum substitution, or no substitution; R<NUM>-R<NUM> are each independently selected from the group consisting of hydrogen, deuterium, halogen, CN, C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> haloalkyl, C<NUM>-C<NUM> deuterated alkyl, C<NUM>-C<NUM> aryl, C<NUM>-C<NUM> arylsilane, and combinations thereof.

Further, R<NUM>-R<NUM> are each independently selected from the group consisting of hydrogen, deuterium, CD<NUM>, F, CF<NUM>, CN, methyl, ethyl, n-propyl, isopropyl, n-butyl, isobutyl, sec-butyl, tert-butyl, n-pentyl, isopentyl, sec-pentyl, tert-pentyl, n-hexyl, isohexyl, sec-hexyl, tert-hexyl, n-heptyl, isoheptyl, sec-heptyl, tert-heptyl, n-octyl, isooctyl, sec-octyl, tert-octyl, n-nonyl, isononyl, sec-nonyl, tert-nonyl, phenyl, biphenyl, triphenylsilane, and combinations thereof.

Further, R<NUM>, R<NUM>, and R<NUM> are each independently selected from the group consisting of hydrogen, deuterium, F, CN, methyl, tert-butyl, phenyl, and combinations thereof.

Preferably, the fused ring carbazole tetradentate metal platinum (II) complex is selected from any one of the chemical structures shown below: where "D" represents deuterium:
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Further, the present invention also provides use of the fused ring carbazole tetradentate metal platinum (II) complex having the structure shown in formula (I) above in an electronic device.

Further, the electronic device includes an organic electroluminescence device (OLED), an organic integrated circuit (O-IC), an organic field effect transistor (O-FET), an organic thin film transistor (O-TFT), an organic light emitting transistor (O-LET), an organic solar cell (O-SC), an organic optical detector, an organic photoreceptor, an organic field quenching device (O-FQD), a light emitting electrochemical cell (LEC), and an organic laser diode (O-laser).

In another aspect, the present invention also provides an organic electroluminescence device including the fused ring carbazole tetradentate metal platinum (II) complex having the structure shown in formula (I) as described above.

Further, the organic electroluminescence device includes a cathode, an anode, and an organic functional layer therebetween; the organic functional layer includes the fused ring carbazole tetradentate metal platinum (II) complex having the structure shown in formula (I) as described above.

Preferably, the organic functional layer includes a light emitting layer including the fused ring carbazole tetradentate metal platinum (II) complex having the structure shown in formula (I) as described above.

Further, the light emitting layer includes a fluorescent doping material; the fluorescent doping material is preferably a boron-containing organic molecular light emitting material.

In another aspect, the present invention also provides an organic photoelectric device including: a substrate layer; a first electrode on the substrate; an organic light emitting functional layer on the first electrode; a second electrode on the organic light emitting functional layer; wherein the organic light emitting functional layer includes the fused ring carbazole tetradentate metal platinum (II) complex as described above. For example, a platinum (II) complex may be included as a light emitting material in the organic light emitting functional layer.

Further, the organic light emitting functional layer includes any one or more fluorescent doping materials, and the fluorescent doping materials are preferably boron-containing organic molecular light emitting materials, and preferably phosphorescent sensitizable boron-containing compounds.

In the present invention, the organic photoelectric device can be fabricated by utilizing methods such as sputter coating, electron beam evaporation, vacuum evaporation, etc. to evaporate metal or oxides having electrical conductivity and alloys thereof on a substrate to form an anode; evaporating a hole-injection layer, a hole-transporting layer, a light emitting layer, an air-blocking layer, and an electron-transporting layer on the surface of the anode obtained by the preparation in a sequential order, and then evaporating a cathode at a later time. In addition to the method above, an organic electroluminescence device is fabricated on a substrate by evaporation in the order of a cathode, an organic layer, and an anode. The organic layer may also include a multilayer structure such as a hole-injection layer, a hole-transport layer, a light emitting layer, a hole-blocking layer, and an electron transport layer. In the present invention, the organic layer is prepared by solvent engineering (spin-coating, tape-casting, doctor-blading, screen-printing, ink-jet printing, or Thermal-Imaging) using a high molecular material instead of the evaporation method, reducing the number of device layers.

The present invention also provides a composition including the fused ring carbazole tetradentate metal platinum (II) complex having the structure shown in formula (I). Preferably, the composition further includes a fluorescent doping material, and the fluorescent doping materials are preferably boron-containing organic molecular light emitting materials, and preferably phosphorescent sensitizable boron-containing compounds.

The present invention also provides a formulation including the fused ring carbazole tetradentate metal platinum (II) complex having the structure shown in formula (I) as described above or a composition as described above and at least one solvent.

The solvent is not particularly limited, and an unsaturated hydrocarbon solvent such as toluene, xylene, mesitylene, tetrahydronaphthalene, decahydronaphthalene, dicyclohexane, n-butylbenzene, sec-butylbenzene, tert-butylbenzene and other unsaturated hydrocarbon solvents, halogenated saturated hydrocarbon solvents such as carbon tetrachloride, chloroform, methylene chloride, ethylene chloride, butyl chloride, butyl bromide, pentyl chloride, pentyl bromide, hexyl chloride, hexyl bromide, cyclohexyl chloride, cyclohexyl bromide, halogenated unsaturated hydrocarbon solvents such as chlorobenzene, dichlorobenzene, trichlorobenzene, ether solvents such as tetrahydrofuran and tetrahydropyran, and other halogenated solvents known to those skilled in the art, can be used.

The present invention also provides a display or lighting device comprising one or more of the organic photoelectric devices described above.

In the present invention, a tetradentate metal platinum (II) complex phosphorescent material is obtained by introducing a five-membered heterocyclic system such as benzofuran or benzothiophene at the <NUM>, <NUM>-positions of carbazole. Increasing the ratio of the local state (LE) in the excited triplet state of the cyclic tetradentate platinum (II) complex leads to a lower shoulder peak, which improves the molecular luminescence color purity of the materials. This in turn increases the device lifetime. The materials provided by the present invention all have good chemical stability and thermal stability and are easy to fabricate an evaporation-type OLED device. Organic electroluminescence devices fabricated using the compounds of the present invention as the light emitting layer show a significant improvement in both current efficiency and lifetime and a significant reduction in the start-up voltage. The combination with the fluorescent doping material (boron-containing compound) can balance the transport of holes and electrons, making the energy transfer between the subject and the object more efficient, and can improve the light color purity of the device.

The description of the constituent elements recorded below is sometimes based on representative embodiments or specific examples of the present invention, but the present invention is not limited to such embodiments or specific examples.

As used herein, the term "substituted" is intended to encompass all permissible substituents of organic compounds. In broad aspects, permissible substituents include acyclic and cyclic, branched and unbranched, carbocyclic and heterocyclic, and aromatic and nonaromatic substituents of the organic compounds. Illustrative substituents include, for example, those described below. The permissible substituents may be one or more and the same or different for appropriate organic compounds. For the purposes of the present invention, the present invention is not intended to be limited in any manner by the permissible substituents of organic compounds. Likewise, the term "substituted" or "substituted with" includes the implicit proviso that such substitution is in accordance with a permitted valence of the substituted atom and the substituent and that the substitution results in a stable compound (e.g. a compound that does not spontaneously undergo transformation such as by rearrangement, cyclization, elimination, etc.). It is also contemplated that, in certain aspects, unless expressly stated to the contrary, individual substituents can be further optionally substituted (i.e. further substituted or unsubstituted).

In defining various terms, "R<NUM>"-"R<NUM>" are used herein as a general symbol to represent various specific substituents. These symbols can be any substituents, not limited to those disclosed herein, and when they are limited in one instance to certain substituents, they can be limited in other instances to some other substituents. As used herein, "R<NUM>", "R<NUM>". "Rn" (where n is an integer) can independently have one or more of the groups listed above. For example, if R<NUM> is a straight-chain alkyl group, one hydrogen atom of the alkyl group may be optionally substituted with hydroxyl, alkoxy, alkyl, halogen, and the like. Depending on the group selected, the first group may be incorporated within the second group, or alternatively, the first group may be pendant, i.e. attached, to the second group.

The term "alkyl" as used herein is a branched or unbranched saturated hydrocarbon group of <NUM> to <NUM> carbon atoms such as methyl, ethyl, n-propyl, isopropyl, n-butyl, isobutyl, sec-butyl, tert-butyl, n-pentyl, isopentyl, sec-pentyl, neopentyl, hexyl, heptyl, hemi-, nonyl, decyl, dodecyl, tetradecyl, hexadecyl, eicosyl, tetracosyl and the like. The alkyl group may be cyclic or acyclic. The alkyl group may be branched or unbranched. The alkyl group may be substituted or unsubstituted. For example, the alkyl group may be substituted with one or more groups including, but not limited to, an optionally substituted alkyl, cycloalkyl, alkoxy, amino, halo, hydroxy, nitro, silyl, sulfo-oxo, or mercapto group as described herein.

The term "aryl" as used herein is a radical of any carbon-based aromatic group containing from <NUM> to <NUM> carbon atoms including, but not limited to, phenyl, naphthyl, phenyl group, biphenyl, phenoxyphenyl, anthracenyl, phenanthrenyl, and the like. The term "aryl" also includes "heteroaryl", which is defined as a group containing an aromatic group having at least one heteroatom incorporated within the ring of the aromatic group. Examples of heteroatoms include but are not limited to, nitrogen, oxygen, sulfur, and phosphorus. Likewise, the term "non-heteroaryl" (which is also encompassed by the term "aryl") defines groups that contain aromatic groups that is free of a heteroatom. The aryl group may be substituted or unsubstituted. The aryl group may be substituted with one or more groups including, but not limited to, alkyl, cycloalkyl, alkoxy, alkenyl, cycloalkenyl, alkynyl, cycloalkynyl, aryl, heteroaryl, aldehyde, amino, carboxyl, ester, halogen, hydroxyl, carbonyl, azido, nitro, silyl, sulfo-oxo, or thiol as described herein.

The compound disclosed herein can exhibit desirable properties and have emission and/or absorption spectra that can be modulated by the selection of appropriate ligands. In another aspect, the invention may exclude any one or more compounds, structures, or portions thereof specifically recited herein.

The compounds of the present invention can be prepared using a variety of methods, including but not limited to those described in the examples provided herein.

It is to be understood that both the foregoing general description and the following detailed description are exemplary and explanatory only and are not restrictive. The present application can be understood more readily by reference to the following detailed description and examples contained therein.

Before the present compounds, devices, and/or methods are disclosed and described, it is to be understood that they are not limited to specific synthetic methods (as otherwise indicated), or to specific reagents (as otherwise indicated), as such can, of course, vary. It is also to be understood that the terminology used in the invention is for the purpose of describing only the particular aspect and is not intended to be limiting. Although any methods and materials similar or equivalent to those described herein can be used in the practice or testing, exemplary methods and materials are described below. All starting materials and solvents of synthetic examples were purchased commercially unless otherwise specified, and the solvents were used as they were without further treatment.

The substrate of the present invention may be any substrate typically used in organic photoelectric devices. It may be a glass or transparent plastic substrate, it may be a substrate of an opaque material such as silicon or stainless steel, and it may be a flexible PI film. Different substrates have different mechanical strength, thermal stability, transparency, surface smoothness, and water resistance. The application direction is different according to the properties of the substrates. As the materials for the hole-injecting layer, the hole-transporting layer, and the electron-injecting layer, any material can be selected and used from known related materials for OLED devices, and the present invention is not particularly limited thereto.

The following examples of synthesis, compositions, devices, or methods of the compound are provided merely to provide a general approach to the industry and are not intended to limit the scope of the patent. The data (quantity, temperature, etc.) mentioned in the patent are as accurate as possible, but some errors may exist. Unless otherwise noted, the weighing is done separately, the temperature is °C, or room temperature, and the pressure is near atmospheric.

A method for the preparation of a novel compound is provided in the following examples, but the preparation of such compounds is not limited to this method. In this technical field, since the claimed compound of the present invention can be easily prepared by modification, the methods listed below or other methods can be used. The following examples are given by way of example only and are not intended to limit the scope of this patent. The temperature, catalyst, concentration, reactants, and course of reaction may be varied to select different conditions for different reactants to produce the compound.

<NUM>H NMR (<NUM>),<NUM>H NMR(<NUM>), and <NUM>C NMR(<NUM>) spectra were measured on an ANANCE III (<NUM>) NMR spectrometer. Unless otherwise specified, DMSO-d<NUM> or CDCl<NUM> containing <NUM>% TMS was used as the solvent for NMR. TMS (δ = <NUM> ppm) was used as the internal standard when CDCl<NUM> was used as the solvent for the <NUM>H NMR spectrum. TMS (δ = <NUM> ppm) or residual DMSO peak (δ = <NUM> ppm) or residual water peak (δ = <NUM> ppm) was used as an internal standard when DMSO-d<NUM> was used as solvent. In <NUM>C NMR spectra, CDCl<NUM> (δ = <NUM> ppm) or DMSO-d6 (δ = <NUM> ppm) was used as the internal standard. Determination was done on the HPLC-MS Agilent <NUM> TOF LC/MS. HRMS spectra were determined on the Agilent <NUM> TOF LC/MS type liquid chromatography-time-of-flight mass spectrometer. <NUM>H NMR spectral data: s = singlet, d = doublet, t = triplet, q = quartet, p = quintet, m = multiplet, br = broad.

Synthesis of intermediate dBr-tBuNH<NUM>: to a reaction flask were added p-tert-butylaniline (<NUM>, <NUM> mmoL, <NUM> eq. ) dissolved in dichloromethane (<NUM>), and N-bromosuccinimide (<NUM>, <NUM> mmoL, <NUM> eq. The reaction was carried out at room temperature and stopped after <NUM> hours. The reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of red liquid in <NUM>% yield, which was used directly in subsequent reactions.

Synthesis of intermediate dBr-tBuNO<NUM>: to a reaction flask were added dBr-tBuNH<NUM> (<NUM>, <NUM> mmoL, <NUM> eq. ) dissolved with N-methylpyrrolidone (<NUM>), followed by adding sodium hydride (<NUM>, <NUM> mmoL, <NUM> eq. ) and o-fluoronitrobenzene (<NUM>, <NUM> mmoL, <NUM> eq. The reaction was carried out at room temperature and stopped after <NUM> hours. The reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of yellow solid in <NUM>% yield, which was used directly in subsequent reactions.

Synthesis of intermediate dBr-tBu2NH<NUM>: to a reaction flask were added dBr-tBuNO<NUM> (<NUM>, <NUM> mmoL, <NUM> eq. ), stannous chloride (<NUM>, <NUM> mmoL, <NUM> eq. ), ethyl acetate (<NUM>) and ethanol (<NUM>). The reaction was carried out at <NUM> in an oil bath and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of white solid in <NUM>% yield, which was used directly in subsequent reactions.

Synthesis of intermediate dPh-tBuNH<NUM>: to a reaction flask were added dBr- tBu2NH<NUM> (<NUM>, <NUM> mmoL, <NUM> eq. ), phenylboronic acid (<NUM>, <NUM> mmoL, <NUM> eq. ), tetra(triphenylphosphine)palladium (<NUM>, <NUM> mmoL, <NUM> eq. ), potassium carbonate (<NUM>, <NUM> mmoL, <NUM> eq. ), dioxane (<NUM>), and water ( <NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of white solid in <NUM>% yield, <NUM>H NMR (<NUM>, DMSO) δ <NUM> (s, <NUM>), <NUM> (s, <NUM>), <NUM> (s, <NUM>), <NUM> (dd, J = <NUM>, <NUM>, <NUM>), <NUM> (td, J = <NUM>, <NUM>, <NUM>), <NUM> (td, J = <NUM>, <NUM>, <NUM>), <NUM> (dd, J = <NUM>, <NUM>, <NUM>), <NUM>-<NUM>(m, <NUM>), <NUM> -<NUM> (m, <NUM>), <NUM> (s, <NUM>), <NUM> -<NUM> (m, <NUM>).

Synthesis of intermediate dPh-5tBuNH<NUM>: to a reaction flask were added dBr- tBu2NH<NUM> (<NUM>, <NUM> mmoL, <NUM> eq. ), <NUM>, <NUM>-di-tert-butylphenylboronic acid pinacol ester (<NUM>, <NUM> mmoL, <NUM> eq. ), tetra(triphenylphosphine)palladium (<NUM>, <NUM> mmoL, <NUM> moL%), potassium carbonate (<NUM>, <NUM> mmoL, <NUM> eq. ), dioxane (<NUM>), and water (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of white solid in <NUM>% yield. <NUM>H NMR (<NUM>, DMSO) δ <NUM> (s, <NUM>), <NUM> (s, <NUM>), <NUM> (s, <NUM>), <NUM> (s, <NUM>), <NUM> (dd, J = <NUM>, <NUM>, <NUM>), <NUM> (td, J = <NUM>, <NUM>, <NUM>), <NUM> (td, J = <NUM>, <NUM>, <NUM>), <NUM> (dd, J = <NUM>, <NUM>, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (s, <NUM>).

Synthesis of intermediate dBr-NO<NUM>: to a reaction flask were added dBr-NH<NUM> (<NUM>, <NUM> mmoL, <NUM> eq. ) dissolved with N-methylpyrrolidone (<NUM>), followed by adding sodium hydride (<NUM>, <NUM> mmoL, <NUM> eq. ) and o-fluoronitrobenzene (<NUM>, <NUM> mmoL, <NUM> eq. The reaction was carried out at room temperature and stopped after <NUM> hours. The reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of yellow solid in <NUM>% yield, which was used directly in subsequent reactions.

Synthesis of intermediate dBr-2NH<NUM>: to a reaction flask were added dBr-NO<NUM> (<NUM>, <NUM> mmoL, <NUM> eq. ), stannous chloride (<NUM>, <NUM> mmoL, <NUM> eq. ), ethyl acetate (<NUM>), and ethanol (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM> hours. The reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of white solid in <NUM>% yield, which was used directly in subsequent reactions.

Synthesis of intermediate dPh-NH<NUM>: to a reaction flask were added dBr-2NH<NUM> (<NUM>, <NUM> mmoL, <NUM> eq. ), phenylboronic acid (<NUM>, <NUM> mmoL, <NUM> eq. ), tetra(triphenylphosphine)palladium (<NUM>, <NUM> mmoL, <NUM> eq. ), sodium carbonate (<NUM>, <NUM> mmoL, <NUM> eq. ), dioxane (<NUM>), and water (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM> hours. The reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of white solid in <NUM>% yield, which was used directly in subsequent reactions.

Synthesis of intermediate dPh-4tBuNH<NUM>: to a reaction flask were added dBr- 2NH<NUM> (<NUM>, <NUM> mmoL, <NUM> eq. ), <NUM>, <NUM>-di-tert-butylphenylboronic acid pinacol ester (<NUM>, <NUM> mmoL, <NUM> eq. ), tetra(triphenylphosphine)palladium (<NUM>, <NUM> mmoL, <NUM> moL%), potassium carbonate (<NUM>, <NUM> mmoL, <NUM> eq. ), dioxane (<NUM>), and water (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of white solid in <NUM>% yield, which was used directly in subsequent reactions.

Synthesis of intermediate 4O-NO<NUM>: to a reaction flask were added A-4O-B(OH)<NUM> (<NUM>, <NUM> mmoL, <NUM> eq. ), B (<NUM>, <NUM> mmoL, <NUM> eq. ), tetra(triphenylphosphine)palladium (<NUM>, <NUM> mmoL, <NUM> moL%), potassium carbonate (<NUM>, <NUM> mmoL, <NUM> eq. ), dioxane (<NUM>), and water (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of yellow solid in <NUM>% yield. <NUM>H NMR (<NUM>, DMSO) δ <NUM> (s, <NUM>), <NUM> (td, J = <NUM>, <NUM>, <NUM>), <NUM> (dd, J = <NUM>, <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (dd, J = <NUM>, <NUM>, <NUM>).

Synthesis of intermediate 4O-NH: to a reaction flask were added 4O-NO<NUM> (<NUM>, <NUM> mmoL, <NUM> eq. ), triphenylphosphine (<NUM>, <NUM> mmoL, <NUM> eq. ), and o-dichlorobenzene (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of brown solid in <NUM>% yield, which was used directly in subsequent reactions.

Synthesis of intermediate 4O-OMe: to a reaction flask were added 4O-NH (<NUM>, <NUM> mmoL, <NUM> eq. ), <NUM>-(tert-butyl)-<NUM>-chloropyridine (<NUM>, <NUM> mmoL, <NUM> eq. ), tris(dibenzylideneacetone) dipalladium (<NUM>, <NUM> mmoL, <NUM> moL%), <NUM>-(di-tert-butylphosphino) biphenyl (<NUM>, <NUM> mmoL, <NUM> moL%), sodium tert-butoxide (<NUM>, <NUM> mmoL, <NUM> eq. ), followed by adding toluene (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of brown solid in <NUM>% yield, which was used directly in subsequent reactions.

Synthesis of intermediate 4O-OH: to a reaction flask were added 4O-OMe (<NUM>, <NUM> mmoL, <NUM> eq. ), pyridine hydrochloride (<NUM>, <NUM> mmoL, <NUM> eq. ) and <NUM>,<NUM>-dimethyl-<NUM>-imidazolidinone (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of brown solid in <NUM>% yield, which was used directly in subsequent reactions.

Synthesis of intermediate tBu-4O-Cl: to a reaction flask were added 4O-OH (<NUM>, <NUM> mmoL, <NUM> eq. ), <NUM>-chloro-<NUM>-bromo-tert-butylbenzene (<NUM>, <NUM> mmoL, <NUM> eq. ), <NUM>-picolinic acid (<NUM>, <NUM> mmoL, <NUM> mmoL%), cuprous iodide (<NUM>, <NUM> mmoL, <NUM> mmoL%), potassium phosphate (<NUM>, <NUM> mmoL, <NUM> eq. ), and dimethylsulfoxide (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of white solid in <NUM>% yield. <NUM>H NMR (<NUM>, DMSO) δ <NUM> (s, <NUM>) ,<NUM> (s, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> (dd, J = <NUM>, <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>) , <NUM> - <NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>).

Synthesis of intermediate LNH-PtO6: to a reaction flask were added dPh-tBuNH<NUM> (<NUM>, <NUM> mmoL, <NUM> eq. ), tBu-4O-Cl (<NUM>, <NUM> mmoL, <NUM> eq. ), tris(dibenzylideneacetone) dipalladium (<NUM>, <NUM> mmoL, <NUM> moL%), <NUM>-(di-tert-butylphosphino) biphenyl (<NUM>, <NUM> mmoL, <NUM> moL%) and sodium tert-butoxide (<NUM>, <NUM> mmoL, <NUM> eq. ), followed by adding toluene (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of white solid in <NUM>% yield, which was used directly in subsequent reactions.

Synthesis of ligand L-PtO6: to a reaction flask was added LNH-PtO6 (<NUM>, <NUM> mmoL, <NUM> eq. ), followed by ammonium hexafluorophosphate (<NUM>, <NUM> mmoL, <NUM> eq. ) and triethyl orthoformate (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of white solid in <NUM>% yield. <NUM>H NMR (<NUM>, DMSO) δ <NUM> (s, <NUM>), <NUM> (s, <NUM>), <NUM> (s, <NUM>), <NUM> (t, J= <NUM>, <NUM>), <NUM> (t, J= <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (dd, J = <NUM>, <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J= <NUM>, <NUM>), <NUM> (s, <NUM>).

Synthesis of PtO6: to a reaction flask were added L-PtO6 (<NUM>, <NUM> mmoL, <NUM> eq. ), (<NUM>,<NUM>-cyclooctadiene) platinum (II) dichloride (<NUM>, <NUM> mmoL, <NUM> eq. ), sodium acetate (<NUM>, <NUM> mmoL, <NUM> eq. ), and diethylene glycol dimethyl ether (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of light yellow solid in <NUM>% yield. <NUM> NMR (<NUM>, DMSO-d6) δ1. <NUM> (s, <NUM>), <NUM> (s, <NUM>), <NUM> (dd, J = <NUM>, <NUM>, <NUM>), <NUM> -<NUM> (m, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> -<NUM> (m, <NUM>), <NUM> -<NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>).

Synthesis of intermediate LNH-PtO2: to a reaction flask were added dPh-NH<NUM> (<NUM>, <NUM> mmoL, <NUM> eq. ), tBu-4O-Cl (<NUM>, <NUM> mmoL, <NUM> eq. ), tris(dibenzylideneacetone) dipalladium (<NUM>, <NUM> mmoL, <NUM> moL%), <NUM>-(di-tert-butylphosphino) biphenyl (<NUM>, <NUM> mmoL, <NUM> moL%), and sodium tert-butoxide (<NUM>, <NUM> mmoL, <NUM> eq. ), followed by adding toluene (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of white solid in <NUM>% yield, which was used directly in subsequent reactions.

Synthesis of ligand L-PtO2: to a reaction flask was added LNH-PtO2 (<NUM>, <NUM> mmoL, <NUM> eq. ), ammonium hexafluorophosphate (<NUM>, <NUM> mmoL, <NUM> eq. ) and triethyl orthoformate (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of white solid in <NUM>% yield. <NUM>H NMR (<NUM>, DMSO) δ <NUM> (s, <NUM>) ,<NUM> (s, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (dd, J = <NUM>, <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (s, <NUM>).

Synthesis of Pt PtO2: to a reaction flask were added L-PtO2 (<NUM>, <NUM> mmoL, <NUM> eq. ), (<NUM>,<NUM>-cyclooctadiene) platinum (II) dichloride (<NUM>, <NUM> mmoL, <NUM> eq. ), sodium acetate (<NUM>, <NUM> mmoL, <NUM> eq. ), and diethylene glycol dimethyl ether (<NUM>). Nitrogen was bubbled to remove oxygen for <NUM>. The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of light yellow solid in <NUM>% yield. <NUM>H NMR (<NUM>, CDCl<NUM>) δ <NUM> (s, <NUM>) ,<NUM> (s, <NUM>), <NUM> (dd, J = <NUM>, <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM>-<NUM>(m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM>-<NUM>(m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>).

Synthesis of intermediate LNH-PtO5: to a reaction flask were added dPh-tBuNH<NUM> (<NUM>, <NUM> mmol, <NUM> eq. ), 4O-Cl (<NUM>, <NUM> mmol, <NUM> eq. ), tris(dibenzylideneacetone)dipalladium (<NUM>, <NUM> mmol, <NUM> mol%), <NUM>-dicyclohexylphosphino-<NUM>',<NUM>'-dimethoxy-biphenyl (<NUM>, <NUM> mmol, <NUM> mol%), and sodium tert-butoxide (<NUM>, <NUM> mmol, <NUM> eq. ), followed by adding toluene (<NUM>). The reaction was carried out at <NUM> in an oil bath and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of light green solid in <NUM>% yield, which was used directly in subsequent reactions.

Synthesis of ligand L-PtO5: to a reaction flask were added LNH-PtO5 (<NUM>, <NUM> mmol, <NUM> eq. ), ammonium hexafluorophosphate (<NUM>, <NUM> mmol, <NUM> eq. ) and triethyl orthoformate (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of white solid in <NUM>% yield. <NUM>H NMR (<NUM>, CDCl<NUM>) δ <NUM> (s, <NUM>), <NUM> (s, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> (dd, J = <NUM>, <NUM>, <NUM>), <NUM> - <NUM>(m, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (dd, J = <NUM>, <NUM>, <NUM>), <NUM> (s, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (s, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (s, <NUM>).

Synthesis of PtO5: to a reaction flask were added L-PtO5 (<NUM>, <NUM> mmoL, <NUM> eq. ), (<NUM>,<NUM>-cyclooctadiene) platinum (II) dichloride (<NUM>, <NUM> mmoL, <NUM> eq. ), sodium acetate (<NUM>, <NUM> mmoL, <NUM> eq. ), and diethylene glycol dimethyl ether (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of light yellow solid in <NUM>% yield. <NUM>H NMR (<NUM>, Chloroform-d) δ <NUM> (s, <NUM>), <NUM> (s, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (s, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>).

PtO27 was synthesized by referring to the synthesis procedure and reaction condition of compound PtO6 in Example <NUM>. The synthesis afforded the desired product LNH-PtO27, <NUM> of light green foamy solid in <NUM>% yield. The desired product L-PtO27, <NUM> of light green foamy solid, in <NUM>% yield. Molecular weight [M]+: <NUM>. The desired product PtO27, <NUM> of yellow solid in <NUM>% yield. Molecular weight [M+H]+: <NUM>.

Synthesis of intermediate 4O-Cl: to a reaction flask were added 4O-OH (<NUM>, <NUM> mmoL, <NUM> eq. ), m-chlorobromobenzene (<NUM>, <NUM> mmoL, <NUM> eq. ), <NUM>-picolinic acid (<NUM>, <NUM> mmoL, <NUM> mmoL%), cuprous iodide (<NUM>, <NUM> mmoL, <NUM> mmoL%), potassium phosphate (<NUM>, <NUM> mmoL, <NUM> eq. ), and dimethylsulfoxide (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of white solid in <NUM>% yield. <NUM>H NMR (<NUM>, DMSO) δ <NUM> (s, <NUM>), <NUM>-<NUM>(m, <NUM>), <NUM> -<NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM>-<NUM> (m, <NUM>), <NUM>-<NUM>(m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM>-<NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>).

Synthesis of intermediate LNH-PtO33: to a reaction flask were added dPh-4tBuNH<NUM> (<NUM>, <NUM> mmoL, <NUM> eq. ), 4O-Cl (<NUM>, <NUM> mmoL, <NUM> eq. ), tris(dibenzylideneacetone)dipalladium (<NUM>, <NUM> mmoL, <NUM> moL%), <NUM>-dicyclohexylphosphino-<NUM>',<NUM>'-dimethoxy-biphenyl (<NUM>, <NUM> mmoL, <NUM> moL%), and sodium tert-butoxide (<NUM>, <NUM> mmoL, <NUM> eq. ), followed by adding toluene (<NUM>). The reaction was carried out at <NUM> in an oil bath and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of white solid in <NUM>% yield, which was used directly in subsequent reactions.

Synthesis of ligand L-PtO33: to a reaction flask were added LNH-PtO33 (<NUM>, <NUM> mmoL, <NUM> eq. ), ammonium hexafluorophosphate (<NUM>, <NUM> mmoL, <NUM> eq. ) and triethyl orthoformate (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of white solid in <NUM>% yield. <NUM>H NMR (<NUM>, DMSO-d<NUM>) δ <NUM> (s, <NUM>), <NUM> (s, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> (ddd, J = <NUM>, <NUM>, <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> (dd, J = <NUM>, <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (dd, J = <NUM>, <NUM>, <NUM>), <NUM> (s, <NUM>).

Synthesis of PtO33: to a reaction flask were added L-PtO33 (<NUM>, <NUM> mmoL, <NUM> eq. ), (<NUM>,<NUM>-cyclooctadiene) platinum (II) dichloride (<NUM>, <NUM> mmoL, <NUM> eq. ), sodium acetate (<NUM>, <NUM> mmoL, <NUM> eq. ), and diethylene glycol dimethyl ether (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of light yellow solid in <NUM>% yield. <NUM>H NMR (<NUM>, DMSO-d<NUM>) δ <NUM> - <NUM> (br, <NUM>), <NUM> (s, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>).

Synthesis of intermediate LNH-PtO34: to a reaction flask were added dPh-4tBuNH<NUM> (<NUM>, <NUM> mmol, <NUM> eq. ), tBu-4O-Cl (<NUM>, <NUM> mmol, <NUM> eq. ), tris(dibenzylideneacetone)dipalladium (<NUM>, <NUM> mmol, <NUM> mol%), <NUM>-dicyclohexylphosphino-<NUM>',<NUM>'-dimethoxy-biphenyl (<NUM>, <NUM> mmol, <NUM> mol%), sodium tert-butoxide (<NUM>, <NUM> mmol, <NUM> eq. ), followed by adding toluene (<NUM>). The reaction was carried out at <NUM> in an oil bath and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of white solid in <NUM>% yield, which was used directly in subsequent reactions.

Synthesis of ligand L-PtO34: to a reaction flask was added LNH-PtO34 (<NUM>, <NUM> mmol, <NUM> eq. ), ammonium hexafluorophosphate (<NUM>, <NUM> mmol, <NUM> eq. ) and triethyl orthoformate (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of white solid in <NUM>% yield. <NUM>H NMR (<NUM>, DMSO-d<NUM>) δ <NUM> (s, <NUM>), <NUM> (s, <NUM>), <NUM> (s, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> (dd, J = <NUM>, <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (s, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (s, <NUM>).

Synthesis of PtO34: to a reaction flask were added L-PtO34 (<NUM>, <NUM> mmoL, <NUM> eq. ), (<NUM>,<NUM>-cyclooctadiene) platinum (II) dichloride (<NUM>, <NUM> mmoL, <NUM> eq. ), sodium acetate (<NUM>, <NUM> mmoL, <NUM> eq. ), and diethylene glycol dimethyl ether (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of light yellow solid in <NUM>% yield. <NUM>H NMR (<NUM>, DMSO-d<NUM>) δ <NUM> (s, <NUM>), <NUM> (s, <NUM>), <NUM> (s, <NUM>), <NUM> (dd, J = <NUM>, <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (s, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (s, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>).

Synthesis of intermediate LNH-PtO37: to a reaction flask were added dPh-5tBuNH<NUM> (<NUM>, <NUM> mmoL, <NUM> eq. ), 4O-Cl (<NUM>, <NUM> mmoL, <NUM> eq. ), tris(dibenzylideneacetone)dipalladium (<NUM>, <NUM> mmoL, <NUM> moL%), <NUM>-dicyclohexylphosphino-<NUM>',<NUM>'-dimethoxy-biphenyl (<NUM>, <NUM> mmoL, <NUM> moL%), sodium tert-butoxide (<NUM>, <NUM> mmoL, <NUM> eq. ), followed by adding toluene (<NUM>). The reaction was carried out at <NUM> in an oil bath and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of white solid in <NUM>% yield, which was used directly in subsequent reactions.

Synthesis of ligand L-PtO37: to a reaction flask was added LNH-PtO37 (<NUM>, <NUM> mmoL, <NUM> eq. ), followed by ammonium hexafluorophosphate (<NUM>, <NUM> mmoL, <NUM> eq. ) and triethyl orthoformate (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of white solid in <NUM>% yield. <NUM>H NMR (<NUM>, DMSO) δ <NUM> (s, <NUM>), <NUM> (s, <NUM>), <NUM> (s, <NUM>), <NUM> (s, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (s, <NUM>), <NUM> (s, <NUM>), <NUM> (dd, J = <NUM>, <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (s, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (s, <NUM>).

Synthesis of PtO37: to a reaction flask were added L-PtO37 (<NUM>, <NUM> mmoL, <NUM> eq. ), (<NUM>,<NUM>-cyclooctadiene) platinum (II) dichloride (<NUM>, <NUM> mmoL, <NUM> eq. ), sodium acetate (<NUM>, <NUM> mmoL, <NUM> eq. ), and diethylene glycol dimethyl ether (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of light yellow solid in <NUM>% yield. <NUM>H NMR (<NUM>, CDCl<NUM>) δ <NUM> - <NUM> (m, <NUM>), <NUM> (s, <NUM>), <NUM> (s, <NUM>), <NUM> (dd, J = <NUM>, <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (dd, J = <NUM>, <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>).

Synthesis of intermediate LNH-PtO38: to a reaction flask were added dPh-5tBuNH<NUM> (<NUM>, <NUM> mmoL, <NUM> eq. ), tBu-4O-Cl (<NUM>, <NUM> mmoL, <NUM> eq. ), tris(dibenzylideneacetone)dipalladium (<NUM>, <NUM> mmoL, <NUM> moL%), <NUM>-dicyclohexylphosphino-<NUM>',<NUM>'-dimethoxy-biphenyl (<NUM>, <NUM> mmoL, <NUM> moL%), and sodium tert-butoxide (<NUM>, <NUM> mmoL, <NUM> eq. ), followed by adding toluene (<NUM>). The reaction was carried out at <NUM> in an oil bath and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of white solid in <NUM>% yield, which was used directly in subsequent reactions.

Synthesis of ligand L-PtO38: to a reaction flask were added LNH-PtO38 (<NUM>, <NUM> mmoL, <NUM> eq. ), ammonium hexafluorophosphate (<NUM>, <NUM> mmoL, <NUM> eq. ), and triethyl orthoformate (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of white solid in <NUM>% yield. <NUM>H NMR (<NUM>, DMSO) δ <NUM> (s, <NUM>) ,<NUM> (s, <NUM>), <NUM> (s, <NUM>), <NUM> (s, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> (dd, J = <NUM>, <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> - <NUM>(m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> (d, J= <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (s, <NUM>).

Synthesis of PtO38: to a reaction flask were added L-PtO38 (<NUM>, <NUM> mmoL, <NUM> eq. ), (<NUM>,<NUM>-cyclooctadiene) platinum (II) dichloride (<NUM>, <NUM> mmoL, <NUM> eq. ), sodium acetate (<NUM>, <NUM> mmoL, <NUM> eq. ), and diethylene glycol dimethyl ether (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of light yellow solid in <NUM>% yield. <NUM>H NMR (<NUM>, DMSO) δ <NUM> (s, <NUM>), <NUM> (s, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM>(d, J = <NUM>, <NUM>), <NUM>(d, J = <NUM>, <NUM>),<NUM> (d, J = <NUM>, <NUM>), <NUM> (dd, J = <NUM>, <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>).

PtS93 was synthesized by referring to the synthesis procedure and reaction condition of compound PtS6 in Example <NUM>. The synthesis afforded the desired product LNH-PtO93, <NUM> of light green foamy solid in <NUM>% yield. The desired product L-PtO93, <NUM> of light green foamy solid, in <NUM>% yield. Molecular weight [M]+: <NUM>. The desired product Pt O93, <NUM> of yellow solid in <NUM>% yield. Molecular weight [M+H]+: <NUM>.

Synthesis of intermediate dtBu-Me-4O-OMe: to a reaction flask were added 4O-NH (<NUM>, <NUM> mmoL, <NUM> eq. ), dtBu-Me-Cl (<NUM>, <NUM> mmoL, <NUM> eq. ), tris (dibenzylideneacetone) dipalladium (<NUM>, <NUM> mmoL, <NUM> moL%), <NUM>-dicyclohexylphosphine-<NUM>',<NUM>'-dimethoxy-biphenyl (<NUM>, <NUM> mmoL, <NUM> moL%), and sodium tert-butoxide (<NUM>, <NUM> mmoL, <NUM> eq. ), followed by adding toluene (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of brown solid in <NUM>% yield, which was used directly in subsequent reactions.

Synthesis of intermediate dtBu-Me-4O-OH: to a reaction flask were added dtBu-Me-4O-OMe (<NUM>, <NUM> mmoL, <NUM> eq. ) and hydrogen bromide (<NUM>, <NUM> mmoL, <NUM> eq. The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of brown solid in <NUM>% yield, which was used directly in subsequent reactions.

Synthesis of intermediate dtBu-Me-4O-Cl: to a reaction flask were added dtBu-Me-4O-OH (<NUM>, <NUM> mmoL, <NUM> eq. ), m-chlorobromobenzene (<NUM>, <NUM> mmoL, <NUM> eq. ), <NUM>-picolinic acid (<NUM>, <NUM> mmoL, <NUM> mmoL%), cuprous iodide (<NUM>, <NUM> mmoL, <NUM> mmoL%), potassium phosphate (<NUM>, <NUM> mmoL, <NUM> eq. ), and dimethylsulfoxide (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of white solid in <NUM>% yield. <NUM>H NMR (<NUM>, DMSO) δ <NUM> (s, <NUM>), <NUM> (s, <NUM>), <NUM> (dd, J = <NUM>, <NUM>, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (s, <NUM>), <NUM>(t, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (s, <NUM>).

Synthesis of intermediate LNH-PtO107: to a reaction flask were added dPh-tBuNH<NUM> (<NUM>, <NUM> mmoL, <NUM> eq. ), dtBu-Me-4O -Cl (<NUM>, <NUM> mmoL, <NUM> eq. ), tris(dibenzylideneacetone)dipalladium (<NUM>, <NUM> mmoL, <NUM> moL%), <NUM>-dicyclohexylphosphino-<NUM>',<NUM>'-dimethoxy-biphenyl (<NUM>, <NUM> mmoL, <NUM> moL%), sodium tert-butoxide (<NUM>, <NUM> mmoL, <NUM> eq. ), followed by adding toluene (<NUM>). The reaction was carried out at <NUM> in an oil bath and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of white solid in <NUM>% yield, which was used directly in subsequent reactions.

Synthesis of ligand L-PtO107: to a reaction flask were added LNH-PtO107 (<NUM>, <NUM> mmoL, <NUM> eq. ), ammonium hexafluorophosphate (<NUM>, <NUM> mmoL, <NUM> eq. ), and triethyl orthoformate (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of white solid in <NUM>% yield. which was used directly in subsequent reactions.

Synthesis of PtO107: to a reaction flask were added L-PtO107 (<NUM>, <NUM> mmoL, <NUM> eq. ), (<NUM>,<NUM>-cyclooctadiene) platinum (II) dichloride (<NUM>, <NUM> mmoL, <NUM> eq. ), sodium acetate (<NUM>, <NUM> mmoL, <NUM> eq. ), and diethylene glycol dimethyl ether (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of light yellow solid in <NUM>% yield. <NUM>H NMR (<NUM>, CDCl<NUM>) δ <NUM> (s, <NUM>), <NUM> (s, <NUM>), <NUM> (s, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> (tt, J = <NUM>, <NUM>, <NUM>), <NUM> (s, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (s, <NUM>).

Synthesis of intermediate PhF-Me-NH: to a reaction flask were added p-fluorobenzene boronic acid (<NUM>, <NUM> mmoL, <NUM> eq. ), Br-Me-NH (<NUM>, <NUM> mmoL, <NUM> eq. ), tetra(triphenylphosphine) palladium (<NUM>, <NUM> mmoL, <NUM> moL%), potassium carbonate (<NUM>, <NUM> mmoL, <NUM> eq. ), dioxane (<NUM>), and water (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of yellow solid in <NUM>% yield, which was used directly in subsequent reactions.

Synthesis of intermediate PhF-Me-Cl: to a reaction flask were added PhF-Me-NH (<NUM>, <NUM> mmoL, <NUM> eq. ), tert-butyl nitrite (<NUM>, <NUM> mmoL, <NUM> eq. ), triethylbenzyl ammonium chloride (<NUM>, <NUM> mmoL, <NUM> eq. ), dichloromethane (<NUM>), and water (<NUM>). The reaction was carried out at room temperature and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of yellow solid in <NUM>% yield, which was used directly in subsequent reactions.

Synthesis of intermediate PhF-Me-4O-OMe: to a reaction flask were added 4O-NH (<NUM>, <NUM> mmoL, <NUM> eq. ), PhF-Me-Cl (<NUM>, <NUM> mmoL, <NUM> eq. ), tris(dibenzylideneacetone) dipalladium (<NUM>, <NUM> mmoL, <NUM> moL%), <NUM>-dicyclohexylphosphine-<NUM>', <NUM>'-dimethoxy-biphenyl (<NUM>, <NUM> mmoL, <NUM> moL%), and sodium tert-butoxide (<NUM>, <NUM> mmoL, <NUM> eq. ), followed by adding toluene (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of brown solid in <NUM>% yield, which was used directly in subsequent reactions.

Synthesis of intermediate PhF-Me-4O-OH: to a reaction flask were added PhF-Me-4O-OMe (<NUM>, <NUM> mmoL, <NUM> eq. ) and hydrogen bromide (<NUM>, <NUM> mmoL, <NUM> eq. The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of brown solid in <NUM>% yield, which was used directly in subsequent reactions.

Synthesis of intermediate PhF-Me-4O-Cl: to a reaction flask were added PhF-Me-4O-OH (<NUM>, <NUM> mmoL, <NUM> eq. ), m-chlorobromobenzene (<NUM>, <NUM> mmoL, <NUM> eq. ), <NUM>-picolinic acid (<NUM>, <NUM> mmoL, <NUM> mmoL%) cuprous iodide (<NUM>, <NUM> mmoL, <NUM> mmoL%), potassium phosphate (<NUM>, <NUM> mmoL, <NUM> eq. ), and dimethylsulfoxide (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of white solid in <NUM>% yield. which was used directly in subsequent reactions.

Synthesis of intermediate LNH-PtO109: to a reaction flask were added dPh-4tBuNH<NUM> (<NUM>, <NUM> mmoL, <NUM> eq. ), phF-Me-4O-Cl (<NUM>, <NUM> mmoL, <NUM> eq. ), tris(dibenzylideneacetone) dipalladium (<NUM>, <NUM> mmoL, <NUM> moL%), <NUM>-dicyclohexylphosphine-<NUM>', <NUM>'-dimethoxy-biphenyl (<NUM>, <NUM> mmoL, <NUM> moL%), sodium tert-butoxide (<NUM>, <NUM> mmoL, <NUM> eq. ), followed by adding toluene (<NUM>). The reaction was carried out at <NUM> in an oil bath and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of white solid in <NUM>% yield, which was used directly in subsequent reactions.

Synthesis of the ligand L-PtO109: to a reaction flask were added LNH-PtO109 (<NUM>, <NUM> mmoL, <NUM> eq. ), ammonium hexafluorophosphate (<NUM>, <NUM> mmoL, <NUM> eq. ), and triethyl orthoformate (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of white solid in <NUM>% yield. <NUM>H NMR (<NUM>, DMSO-d<NUM>) δ <NUM> (s, <NUM>), <NUM> (s, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (dd, J = <NUM>, <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (s, <NUM>).

Synthesis of PtO109: to a reaction flask were added L-PtO109 (<NUM>, <NUM> mmoL, <NUM> eq. ), (<NUM>,<NUM>-cyclooctadiene) platinum (II) dichloride (<NUM>, <NUM> mmoL, <NUM> eq. ), sodium acetate (<NUM>, <NUM> mmoL, <NUM> eq. ), and diethylene glycol dimethyl ether (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of light yellow solid in <NUM>% yield. <NUM>H NMR (<NUM>, DMSO-d<NUM>) δ <NUM> (s, <NUM>), <NUM> (s, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> (dd, J = <NUM>, <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (td, J = <NUM>, <NUM>, <NUM>), <NUM> (ddd, J = <NUM>, <NUM>, <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (dd, J = <NUM>, <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (s, <NUM>).

Synthesis of intermediate <NUM>-NO<NUM>: to a reaction flask were added A-<NUM>-B(OH)<NUM> (<NUM>, <NUM> mmoL, <NUM> eq. ), B (<NUM>, <NUM> mmoL, <NUM> eq. ), tetra(triphenylphosphine) palladium (<NUM>, <NUM> mmoL, <NUM> moL%), and potassium carbonate (<NUM>, <NUM> mmoL, <NUM> eq. ), dioxane (<NUM>), and water (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of yellow solid in <NUM>% yield, which was used directly in subsequent reactions.

Synthesis of intermediate <NUM>-NH: to a reaction flask were added <NUM>-NO<NUM> (<NUM>, <NUM> mmoL, <NUM> eq. ) and triphenylphosphine (<NUM>, <NUM> mmoL, <NUM> eq. ), and o-dichlorobenzene (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of brown solid in <NUM>% yield, which was used directly in subsequent reactions.

Synthesis of intermediate <NUM>-OMe: to a reaction flask were added <NUM>-NH (<NUM>, <NUM> mmoL, <NUM> eq. ), <NUM>-(tert-butyl)-<NUM>-chloropyridine (<NUM>, <NUM> mmoL, <NUM> eq. ), tris(dibenzylideneacetone) dipalladium (<NUM>, <NUM> mmoL, <NUM> moL%), <NUM>-(di-tert-butylphosphine) biphenyl (<NUM>, <NUM> mmoL, <NUM> moL%), sodium tert-butoxide (<NUM>, <NUM> mmoL, <NUM> eq. ), followed by adding toluene (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of brown solid in <NUM>% yield, which was used directly in subsequent reactions.

Synthesis of intermediate <NUM>-OH: to a reaction flask were added <NUM>-OMe (<NUM>, <NUM> mmoL, <NUM> eq. ), pyridine hydrochloride (<NUM>, <NUM> mmoL, <NUM> eq. ) and <NUM>,<NUM>-dimethyl-<NUM>-imidazolidinone (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of brown solid in <NUM>% yield, which was used directly in subsequent reactions.

Synthesis of intermediate tBu-<NUM>-Cl: to a reaction flask were added <NUM>-OH (<NUM>, <NUM> mmoL, <NUM> eq. ), <NUM>-chloro-<NUM>-bromo-tert-butylbenzene (<NUM>, <NUM> mmoL, <NUM> eq. ), <NUM>-picolinic acid (<NUM>, <NUM> mmoL, <NUM> mmoL%) and cuprous iodide (<NUM>, <NUM> mmoL, <NUM> mmoL%), potassium phosphate (<NUM>, <NUM> mmoL, <NUM> eq. ), and dimethyl sulfoxide (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of white solid in <NUM>% yield. <NUM>H NMR (<NUM>, DMSO) δ <NUM> (s, <NUM>), <NUM> (s, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> (dd, J =<NUM>, <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>).

Synthesis of intermediate LNH-PtS6: to a reaction flask were added dPh-tBuNH<NUM> (<NUM>, <NUM> mmoL, <NUM> eq. ), tBu-4O-Cl (<NUM>, <NUM> mmoL, <NUM> eq. ), tris(dibenzylideneacetone) dipalladium (<NUM>, <NUM> mmoL, <NUM> moL%), <NUM>-(di-tert-butylphosphino) biphenyl (<NUM>, <NUM> mmoL, <NUM> moL%), sodium tert-butoxide (<NUM>, <NUM> mmoL, <NUM> eq. ), followed by adding toluene (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of white solid in <NUM>% yield, which was used directly in subsequent reactions.

Synthesis of the ligand L-PtS6: to a reaction flask were added LNH-PtS6 (<NUM>, <NUM> mmoL, <NUM> eq. ), ammonium hexafluorophosphate (<NUM>, <NUM> mmoL, <NUM> eq. ), and triethyl orthoformate (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of white solid in <NUM>% yield, <NUM>H NMR (<NUM>, DMSO) δ <NUM> (s, <NUM>), <NUM> (s, <NUM>), <NUM> (s, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> -<NUM>(m, <NUM>), <NUM> (dd, J = <NUM>, <NUM>, <NUM>), <NUM>-<NUM>(m, <NUM>), <NUM> -<NUM>(m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (s, <NUM>).

Synthesis of PtS6: to a reaction flask were added PtS6 (<NUM>, <NUM> mmoL, <NUM> eq. ), (<NUM>,<NUM>-cyclooctadiene) platinum (II) dichloride (<NUM>, <NUM> mmoL, <NUM> eq. ), sodium acetate (<NUM>, <NUM> mmoL, <NUM> eq. ), and diethylene glycol dimethyl ether (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of light yellow solid in <NUM>% yield. <NUM>H NMR (<NUM>, CDCl<NUM>) δ <NUM> (s, <NUM>), <NUM> (s, <NUM>), <NUM> (s, <NUM>), <NUM> (dd, J = <NUM> , <NUM>, <NUM>), <NUM> -<NUM>(m, <NUM>), <NUM>-<NUM>(m, <NUM>), <NUM>-<NUM>(m, <NUM>), <NUM> (dd, J = <NUM>, <NUM>, <NUM>), <NUM> (dd, J = <NUM>, <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>).

Synthesis of intermediate LNH-PtS2: to a reaction flask were added dPh-NH<NUM> (<NUM>, <NUM> mmoL, <NUM> eq. ), tBu-<NUM>-Cl (<NUM>, <NUM> mmoL, <NUM> eq. ), tris(dibenzylideneacetone) dipalladium (<NUM>, <NUM> mmoL, <NUM> moL%), <NUM>-(di-tert-butylphosphino) biphenyl (<NUM>, <NUM> mmoL, <NUM> moL%), and sodium tert-butoxide (<NUM>, <NUM> mmoL, <NUM> eq. ), followed by adding toluene (<NUM>). The reaction was carried out at <NUM> in an oil bath and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of white solid in <NUM>% yield, which was used directly in subsequent reactions.

Synthesis of the ligand L-PtS2: to a reaction flask were added LNH-<NUM> (<NUM>, <NUM> mmoL, <NUM> eq. ), ammonium hexafluorophosphate (<NUM>, <NUM> mmoL, <NUM> eq. ), and triethyl orthoformate (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of white solid in <NUM>% yield, <NUM>H NMR (<NUM>, DMSO) δ <NUM> (s, <NUM>), <NUM> (s, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (dd, J = <NUM>, <NUM>, <NUM>), <NUM>-<NUM> (m, <NUM>), <NUM>-<NUM>(m, <NUM>), <NUM>-<NUM>(m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (s, <NUM>), <NUM>-<NUM>(m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (s, <NUM>).

Synthesis of PtS2: to a reaction flask were added L-PtS2 (<NUM>, <NUM> mmoL, <NUM> eq. ), (<NUM>,<NUM>-cyclooctadiene) platinum (II) dichloride (<NUM>, <NUM> mmoL, <NUM> eq. ), sodium acetate (<NUM>, <NUM> mmoL, <NUM> eq. ), and diethylene glycol dimethyl ether (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of light yellow solid in <NUM>% yield. <NUM>H NMR (<NUM>, DMSO) δ <NUM> (s, <NUM>), <NUM> (s, <NUM>), <NUM>-<NUM> (m, <NUM>), <NUM>-<NUM> (m, <NUM>), <NUM>-<NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (dd, J = <NUM>, <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>).

Synthesis of intermediate <NUM>-Cl: to a reaction flask were added <NUM>-OH (<NUM>, <NUM> mmoL, <NUM> eq. ), m-chlorobromobenzene (<NUM>, <NUM> mmoL, <NUM> eq. ), <NUM>-picolinic acid (<NUM>, <NUM> mmoL, <NUM> mmoL%), cuprous iodide (<NUM>, <NUM> mmoL, <NUM> mmoL%), potassium phosphate (<NUM>, <NUM> mmoL, <NUM> eq. ), and dimethyl sulfoxide (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of white solid in <NUM>% yield. <NUM>H NMR (<NUM>, DMSO) δ <NUM> (s, <NUM>), <NUM> -<NUM> (m, <NUM>), <NUM>-<NUM>(m, <NUM>), <NUM> (dd, J = <NUM>, <NUM>, <NUM>), <NUM> -<NUM>(m, <NUM>), <NUM>-<NUM>(m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM>-<NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> -<NUM>(m, <NUM>), <NUM> -<NUM> (m, <NUM>).

Synthesis of intermediate LNH-PtS1: to a reaction flask were added dPh-NH<NUM> (<NUM>, <NUM> mmoL, <NUM> eq. ), <NUM>-Cl (<NUM>, <NUM> mmoL, <NUM> eq. ), tris (dibenzylideneacetone) dipalladium (<NUM>, <NUM> mmoL, <NUM> moL%), <NUM>-(di-tert-butylphosphino) biphenyl (<NUM>, <NUM> mmoL, <NUM> moL%), and sodium tert-butoxide (<NUM>, <NUM> mmoL, <NUM> eq. ), followed by adding toluene (<NUM>). The reaction was carried out at <NUM> in an oil bath and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of white solid in <NUM>% yield, which was used directly in subsequent reactions.

Synthesis of ligand L-PtS1: to a reaction flask were added LNH-PtS1 (<NUM>, <NUM> mmoL, <NUM> eq. ), ammonium hexafluorophosphate (<NUM>, <NUM> mmoL, <NUM> eq. ), and triethyl orthoformate (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of white solid in <NUM>% yield, <NUM>H NMR (<NUM>, DMSO) δ <NUM> (s, <NUM>), <NUM> (t, J = <NUM>, <NUM>), <NUM> -<NUM>(m, <NUM>), <NUM> (dd, J = <NUM>, <NUM>, <NUM>), <NUM>-<NUM>(m, <NUM>), <NUM>-<NUM>(m, <NUM>), <NUM>-<NUM>(m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM>-<NUM>(m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM>-<NUM>(m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (s, <NUM>).

Synthesis of PtS1: to a reaction flask were added L-PtS1 (<NUM>, <NUM> mmoL, <NUM> eq. ), (<NUM>,<NUM>-cyclooctadiene) platinum (II) dichloride (<NUM>, <NUM> mmoL, <NUM> eq. ), sodium acetate (<NUM>, <NUM> mmoL, <NUM> eq. ), and diethylene glycol dimethyl ether (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of light yellow solid in <NUM>% yield. <NUM>H NMR (<NUM>, CDCl<NUM>) δ <NUM> (s, <NUM>), <NUM> (dd, J = <NUM>, <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> - <NUM>(m, <NUM>), <NUM> (d, J = <NUM>, <NUM>).

Synthesis of intermediate LNH-PtS5: to a reaction flask were added dPh-NH<NUM> (<NUM>, <NUM> mmoL, <NUM> eq. ), <NUM>-Cl (<NUM>, <NUM> mmoL, <NUM> eq. ), tris(dibenzylideneacetone)dipalladium (<NUM>, <NUM> mmoL, <NUM> moL%), <NUM>-dicyclohexylphosphino-<NUM>',<NUM>'-dimethoxy-biphenyl (<NUM>, <NUM> mmoL, <NUM> moL%), and sodium tert-butoxide (<NUM>, <NUM> mmoL, <NUM> eq. ), followed by adding toluene (<NUM>). The reaction was carried out at <NUM> in an oil bath and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of white solid in <NUM>% yield, which was used directly in subsequent reactions.

Synthesis of the ligand L-PtS5: to a reaction flask were added LNH-PtS5 (<NUM>, <NUM> mmoL, <NUM> eq. ), ammonium hexafluorophosphate (<NUM>, <NUM> mmoL, <NUM> eq. ), and triethyl orthoformate (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of white solid in <NUM>% yield. <NUM>H NMR (<NUM>, DMSO) δ <NUM> (s, <NUM>), <NUM> (s, <NUM>), <NUM> (t, J= <NUM>, <NUM>), <NUM> - <NUM><NUM> (m, <NUM>), <NUM> (dd, J = <NUM>, <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (s, <NUM>).

Synthesis ofPtS5: to a reaction flask were added L-PtS5 (<NUM>, <NUM> mmoL, <NUM> eq. ), (<NUM>,<NUM>-cyclooctadiene) platinum (II) dichloride (<NUM>, <NUM> mmoL, <NUM> eq. ), sodium acetate (<NUM>, <NUM> mmoL, <NUM> eq. ), and diethylene glycol dimethyl ether (<NUM>). The reaction was carried out at <NUM> and stopped after <NUM>. After cooling to room temperature, the reaction product was concentrated and subjected to silica gel column chromatography to give <NUM> of light yellow solid in <NUM>% yield. <NUM>H NMR (<NUM>, DMSO-d<NUM>) δ <NUM> (s, <NUM>), <NUM> (s, <NUM>), <NUM> (dd, J = <NUM>, <NUM>, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> (s, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>), <NUM> - <NUM> (m, <NUM>), <NUM> (d, J = <NUM>, <NUM>).

PtS27 was synthesized by referring to the synthesis procedure and reaction condition of compound PtS06 in Example <NUM>. The synthesis afforded the desired product LNH-PtS27, <NUM> of light green foamy solid in <NUM>% yield. The desired product L-PtS27, <NUM> of light green foamy solid, in <NUM>% yield. Molecular weight [M]+: <NUM>. The desired product PtS27, <NUM> of yellow solid in <NUM>% yield. Molecular weight [M+H]+: <NUM>.

PtS28 was synthesized by referring to the synthesis procedure and reaction condition of compound PtS06 in Example <NUM>. The synthesis afforded the desired product LNH-PtS28, <NUM> of light green foamy solid in <NUM>% yield. The desired product L-PtS28, <NUM> of light green foamy solid, in <NUM>% yield. Molecular weight [M]+: <NUM>. The desired product PtS28, <NUM> of yellow solid in <NUM>% yield. Molecular weight [M+H]+: <NUM>.

PtS13 was synthesized by referring to the synthesis procedure and reaction condition of compound PtS06 in Example <NUM>. The synthesis afforded the desired product LNH-PtS13, <NUM> of light green foamy solid in <NUM>% yield. The desired product L-PtS13, <NUM> of light green foamy solid, in <NUM>% yield. Molecular weight [M]+: <NUM>. The desired product PtS28, <NUM> of yellow solid in <NUM>% yield. Molecular weight [M+H]+: <NUM>.

PtS17 was synthesized by referring to the synthesis procedure and reaction condition of compound PtS06 in Example <NUM>. The synthesis afforded the desired product LNH-PtS17, <NUM> of light green foamy solid in <NUM>% yield. The desired product L-PtS17, <NUM> of light green foamy solid, in <NUM>% yield. Molecular weight [M]+: <NUM>. The desired product PtS17, <NUM> of yellow solid in <NUM>% yield. Molecular weight [M+H]+: <NUM>.

PtO52 was synthesized by referring to the synthesis procedure and reaction condition of compound PtO6 in Example <NUM>. The desired product was obtained as <NUM> of yellow solid in <NUM>% yield. Molecular weight [M+H]+: <NUM>.

PtO74 was synthesized by referring to the synthesis procedure and reaction condition of compound PtO6 in Example <NUM>. The desired product was obtained as <NUM> of yellow solid in <NUM>% yield. Molecular weight [M+H]+: <NUM>.

PtO88 was synthesized by referring to the synthesis procedure and reaction condition of compound PtO6 in Example <NUM>. The desired product was obtained as <NUM> of yellow solid in <NUM>% yield. Molecular weight [M+H]+: <NUM>.

PtO89 was synthesized by referring to the synthesis procedure and reaction condition of compound PtO6 in Example <NUM>. The desired product was obtained as <NUM> of yellow solid in <NUM>% yield. Molecular weight [M+H]+: <NUM>.

PtO140 was synthesized by referring to the synthesis procedure and reaction condition of compound PtO6 in Example <NUM>. The desired product was obtained as <NUM> of yellow solid in <NUM>% yield. Molecular weight [M+H]+: <NUM>.

PtO144 was synthesized by referring to the synthesis procedure and reaction condition of compound PtO6 in Example <NUM>. The desired product was obtained as <NUM> of yellow solid in <NUM>% yield. Molecular weight [M+H]+: <NUM>.

PtO150 was synthesized by referring to the synthesis procedure and reaction condition of compound PtO6 in Example <NUM>. The desired product was obtained as <NUM> of yellow solid in <NUM>% yield. Molecular weight [M+H]+: <NUM>.

PtO158 was synthesized by referring to the synthesis procedure and reaction condition of compound PtO6 in Example <NUM>. The desired product was obtained as <NUM> of yellow solid in <NUM>% yield. Molecular weight [M+H]+: <NUM>.

PtS47 was synthesized by referring to the synthesis procedure and reaction condition of compound PtS6 in Example <NUM>. The desired product was obtained as <NUM> of yellow solid in <NUM>% yield. Molecular weight [M+H]+: <NUM>.

PtS87 was synthesized by referring to the synthesis procedure and reaction condition of compound PtS6 in Example <NUM>. The desired product was obtained as <NUM> of yellow solid in <NUM>% yield. Molecular weight [M+H]+: <NUM>.

PtS93 was synthesized by referring to the synthesis procedure and reaction condition of compound PtS6 in Example <NUM>. The desired product was obtained as <NUM> of yellow solid in <NUM>% yield. Molecular weight [M+H]+: <NUM>.

PtS135 was synthesized by referring to the synthesis procedure and reaction condition of compound PtS6 in Example <NUM>. The desired product was obtained as <NUM> of yellow solid in <NUM>% yield. Molecular weight [M+H]+: <NUM>.

Theoretical calculations show that the geometry of the ground state (S<NUM>) molecule is optimized using density functional theory (DFT). DFT calculations were performed using B3LYP functional where the <NUM>-<NUM>(d) basis set was used for C, H, O and N atoms and the LANL2DZ basis set was used for Pt atoms.

From the calculation data in Table <NUM>, it can be seen that the introduction of the fused ring at different positions of carbazole enlarges the conjugated system and increases the distribution of the local excited state, so that the emission shoulder peak becomes lower, the Full Width at Half Maximum becomes narrower and the color purity is higher, which can meet the requirements of blue materials.

<FIG> show room temperature emission spectra of R1 and some of the compounds of the present invention, respectively, in a dichloromethane solution. From <FIG> and Table <NUM>, it can be seen that by the introduction of the fused ring at different positions of carbazole, the complexes provided in the present invention expand the conjugated system and increase the distribution of local excited states, so that the emission shoulder peak becomes significantly lower, the Full Width at Half Maximum becomes narrower and the color purity is higher.

As a reference preparation method for a device example, the method of the present invention includes: evaporating a p-doped material on the surface or an anode of an ITO glass with a light-emitting area of <NUM> x <NUM> or co-evaporating the p-doped material with a hole-injection material at a concentration of <NUM>%-<NUM>% to form a hole-injection layer (HIL) of <NUM>-<NUM>, a hole-transport layer (HTL) of <NUM>-<NUM>, then forming a light emitting layer (EML) of <NUM>-<NUM> (which may contain the compound described in the present invention) on the hole-transport layer, and forming an electron transport layer (ETL) of <NUM>-<NUM> and a cathode of <NUM>-<NUM>. If necessary, an electron-blocking layer (EBL) can be added between the HTL and EML layers, and an electron-injecting layer (EIL) can be added between the ETL and the cathode to fabricate an OLED device. The OLED can be tested by standard methods. The device materials referred to in the present invention may be obtained by known synthetic methods unless otherwise specified.

In a preferred example, the structure of Device Example <NUM> provided by the present invention was: ITO/P-<NUM> (<NUM>)/NPD (<NUM>)/HTH-<NUM> (<NUM>)/platinum (II) complex: the mass ratio of HTH-<NUM>: ETH-<NUM> (<NUM>)(PtO6: HTH-<NUM>: ETH-<NUM> was <NUM>: <NUM>: <NUM>)/ETH-<NUM> (<NUM>)/ET-<NUM> (<NUM>)/LiQ (<NUM>)/Al (<NUM>).

Device Examples <NUM>-<NUM> and Comparative Example <NUM> were prepared using a structure similar to Device Example <NUM>, except that PO6 in Device Example <NUM> was replaced with PtO2, PtO5, PtO27, PtO33, PtO34, PtO37, PtO38, PtO93, PtO107, PtO109, PtS6, PtS2, PtS1, PtS5, PtS27, PtS28, PtS13, PtS17, PtO52, PtO74, PtO88, PtO89, PO140, PtO144, PtO150, PtO158, PtS47, PtS87, PtS93, PtS135, R1, respectively. The comparative examples and each device example prepared above were tested for luminescence characteristics by standard methods, and the data are shown in Table <NUM>. The structural formula of the device involved was as follows: wherein P-<NUM> is HATCN, and ET-<NUM> is BPyTP. <CHM>
<CHM>
<CHM>.

As can be seen from Table <NUM>, Device Examples <NUM>-<NUM> prepared in the present application exhibited good device performance in terms of drive voltage, current efficiency, and device lifetime compared to Comparative Example <NUM>. In addition, the color purity of the device can be greatly improved. The improvement in performance of each device example is based on the fact that the specific compound materials of the present invention have a small emission shoulder peak while having a better electron transport capacity. As can be seen, it is prepared as a light emitting layer material into an electronic device with higher current efficiency, device lifetime, and color purity while reducing the driving voltage. It is shown that the compounds provided by the present invention have certain commercial applications. Furthermore, the devices produced by the present invention are all deep blue devices.

In a preferred embodiment, the structure of Device Example <NUM> provided by the present invention was: ITO/P-<NUM> (<NUM>)/NPD (<NUM>)/HTH-<NUM> (<NUM>)/platinum (II) complex: Boron-containing compounds: the mass ratio of HTH-<NUM>: ETH-<NUM> (<NUM>)(PtO6: BN1-<NUM>: HTH-<NUM>: ETH-<NUM> was <NUM>: <NUM>: <NUM>: <NUM>)/ETH-<NUM> (<NUM>)/ET-<NUM> (<NUM>)/LiQ (<NUM>)/Al (<NUM>).

Device Examples <NUM>-<NUM> were each prepared using a structure similar to Device Example <NUM>, except that the platinum (II) complex and the boron-containing compound in Device Example <NUM> were replaced with the compounds listed in Table <NUM>, respectively. The structural formulas of the devices involved are as follows, and the device structure and luminescence characteristic data are shown in Table <NUM>. <CHM>
<CHM>.

As can be seen from Table <NUM>, when the compound of the present invention is used as a sensitizing material together with a boron-containing compound as a light emitting material for devices, the performance of each device can also be significantly improved. It is further shown that the compounds provided by the present invention have certain commercial applications. The addition of boron-containing compounds can further reduce the CIEy value and improve the luminescence color purity of the device.

We also made a top-emitting device D1 for PtO37 and compared it with PtON-TBBI. The device structure used was, ITO/HT-<NUM>: P-<NUM> (<NUM>: <NUM>)/HT-<NUM> (<NUM>)/p-host (<NUM>)/p-host: ETH-<NUM>: PtO37 (<NUM>:<NUM>:<NUM>, <NUM>)/ mSiTRz (<NUM>)/ET-<NUM>:Liq (<NUM>:<NUM>, <NUM>)/Yb (<NUM>)/Ag (<NUM>)/CPL (<NUM>), the comparative device D-R1 replaced the PtO37 in the device D1 with PtON-TBBI. The data are shown in Table <NUM>. The structural formula of the device materials involved is as follows:
<CHM>
<CHM>
<CHM>.

As can be seen from Table <NUM>, the application of the compound of the present invention, PtO37, as a deep blue light emitting material, together with PtON-TBBI as a light emitting material on a device can obtain a significant improvement in emission spectrum Full Width at Half Maximum, color purity, external quantum efficiency, blue light index and lifetime; at the same time, the driving voltage at high brightness of <NUM> cd/m<NUM> can also be decreased significantly. The above data show that the deep blue light emitting materials of the present invention have great application prospects.

Claim 1:
A fused ring carbazole tetradentate metal platinum (II) complex having the general structure shown in formula (I):
<CHM>
where X is selected from O or S; R<NUM>-R<NUM> each independently represent mono- to maximum substitution, or no substitution; R<NUM>-R<NUM> are each independently selected from the group consisting of hydrogen, deuterium, halogen, CN, C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> haloalkyl, C<NUM>-C<NUM> deuterated alkyl, C<NUM>-C<NUM> aryl, C<NUM>-C<NUM> arylsilane, and combinations thereof.