Source: https://patents.google.com/patent/JP2019188208A/en
Timestamp: 2020-04-04 22:36:31
Document Index: 498658998

Matched Legal Cases: ['Application No. 61', 'art 12', 'art 12', 'art 12', 'art 12', 'art 206', 'art.\n6', 'art.\n16']

JP2019188208A - Double bipolar configuration for atrial fibrillation annotation - Google Patents
Double bipolar configuration for atrial fibrillation annotation Download PDF
JP2019188208A
JP2019188208A JP2019124274A JP2019124274A JP2019188208A JP 2019188208 A JP2019188208 A JP 2019188208A JP 2019124274 A JP2019124274 A JP 2019124274A JP 2019124274 A JP2019124274 A JP 2019124274A JP 2019188208 A JP2019188208 A JP 2019188208A
JP2019124274A
P M Houben Richard
リチャード・ピー．エム．・ホウベン
Ben Zriham Yaniv
ヤニブ・ベン・ズリハム
Pressman Assaf
アサフ・プレスマン
ロイ・ウルマン
Auerbach Shmuel
シュムエル・アウアーバッハ
2014-01-29 Priority to US201461932877P priority Critical
2014-01-29 Priority to US61/932,877 priority
2014-12-30 Priority to US14/585,828 priority
2014-12-30 Priority to US14/585,828 priority patent/US9554718B2/en
2019-07-03 Application filed by Biosense Webster (Israel) Ltd, バイオセンス・ウエブスター・（イスラエル）・リミテッドＢｉｏｓｅｎｓｅ Ｗｅｂｓｔｅｒ （Ｉｓｒａｅｌ）， Ｌｔｄ． filed Critical Biosense Webster (Israel) Ltd
2019-10-31 Publication of JP2019188208A publication Critical patent/JP2019188208A/en
206010061592 Cardiac fibrillation Diseases 0 claims description 19
230000002600 fibrillogenic Effects 0 claims description 19
210000003748 Coronary Sinus Anatomy 0 claims description 2
A method and apparatus for performing a cardiac catheterization procedure. The method includes inserting a probe having electrodes into the heart of a living subject, and recording a bipolar and monopolar electrogram from one of the electrodes at a location within the heart. Defining a window of interest in which the rate of change of the potential of the bipolar electrogram exceeds a predetermined value. Annotation is established in the monopolar electrogram, the annotation indicating the maximum rate of change of the potential of the monopolar electrogram within the window of interest. A quality value is assigned to the annotation, and a three-dimensional map containing the annotation and its quality value is generated for a portion of the heart. [Selection diagram] Fig. 1
This application claims the benefit of US Provisional Application No. 61/932877, filed January 29, 2014, which is incorporated herein by reference.
The present invention relates to cardiac physiology. In particular, the present invention relates to the assessment of electrical propagation in the heart.
Cardiac arrhythmias such as atrial fibrillation are a significant cause of morbidity and mortality. US Pat. No. 5,546,951 and US Pat. No. 6,690,963, both assigned to Ben Haim, and PCT application WO 96/05768, all of which are hereby incorporated by reference. Incorporated into the specification, a method for detecting electrical properties of cardiac tissue, such as local excitement arrival time, as a function of exact location within the heart is disclosed. Data is acquired using one or more catheters with electrical and position sensors at the distal tip and advanced into the heart. A method for generating a map of cardiac electrical activity based on these data is disclosed in commonly assigned US Pat. No. 6,226,542 and US Pat. No. 6,301,496 issued to Reisfeld. Which are incorporated herein by reference. As shown in these patents, position and electrical activity are typically first measured at about 10 to about 20 points to generate a preliminary reconstruction or map of the heart surface. . The preliminary map is often combined with data obtained at additional points to generate a more comprehensive map of the heart's electrical activity. In fact, in clinical situations, it is not uncommon to accumulate data at over 100 sites to produce a detailed comprehensive map of heart chamber electrical activity. The detailed map generated can then serve as a reference for determining therapeutic behavioral guidelines, such as tissue ablation, to alter the propagation of cardiac electrical activity and to restore normal heart rhythm.
A catheter containing a position sensor may be used to determine the trajectory of each point on the heart surface. These trajectories may be used to infer motion characteristics such as tissue contraction force. As disclosed in US Pat. No. 5,738,096 issued to Ben Haim, the entire contents of which are incorporated herein by reference, the trajectory at a sufficient number of points in the heart. Once the information is sampled, a map showing such movement characteristics can be constructed.
Electrical activity at points in the heart is usually measured by advancing a multi-electrode catheter, and electrical activity at multiple points in the heart chamber is measured simultaneously. A record obtained from a time-varying potential measured at one or more electrodes is known as an electrogram. The electrogram can be measured with monopolar or bipolar leads and is used, for example, to determine the onset of electrical propagation at a point, known as the local excitation arrival time.
However, the determination of the local excitement arrival time as an index of electrical propagation becomes a problem when there is a conduction abnormality. For example, an atrial electrogram during ongoing atrial fibrillation has three different patterns: single potential, double potential, and complex fragmented atrial electrogram (CFAE). Thus, compared to normal sinus rhythm signals, atrial fibrillation signals are not only more variable, but also extremely complex. Noise exists in both types of signals, complicating their analysis, but due to the complexity and variability of atrial fibrillation signals, the analysis is correspondingly more difficult. On the other hand, in order to overcome atrial fibrillation in medical procedures, it is helpful to establish a possible path for an active wave traveling through the heart representing atrial fibrillation. Once these pathways are identified, they can be blocked, for example, by appropriate resection of the heart region. Pathways can be measured by analysis of atrial fibrillation signals within the heart, and embodiments of the present invention facilitate that analysis.
For ease of explanation, the description herein is directed to the situation where atrial fibrillation is occurring, but those skilled in the art will make this description to other types of fibrillation with the necessary changes. It is possible to adapt.
Embodiments of the present invention simultaneously acquire cardiac potential signals using a catheter having multiple electrodes at the distal end, each electrode generating a respective monopolar signal. The signal may be considered a unipolar signal or may be considered a bipolar signal in combination with another electrode. A monopolar signal may be calculated for a Wilson central electrode (WCT) or for another intracardiac electrode.
In the first part of the signal analysis, the parts of the signal that have important features, usually large numerical gradients, are identified. Analysis is performed on monopolar signals (using bipolar signals to improve the analysis). The analysis identifies the electrical activations referred to herein as annotations and assigns a respective quality factor to each of the annotations.
In the second part of the analysis, the blocked area of the heart, i.e. the cells are temporarily saturated (refractory), so that the activation wave path and subsequent detection of the annotation cannot be maintained. The atrial fibrillation signal is further examined to identify areas of the heart that can only be or partially maintained. The analysis can identify cells that are permanently non-conductive, such as cells of scar tissue.
The results of the two parts of the analysis can be incorporated into a dynamic 3D map of the heart showing the progression of the activation wave through the heart, as well as the blocked area of the heart, i.e., the area where the activation wave does not pass.
In accordance with an embodiment of the present invention, a method is provided, the method comprising inserting a probe having an electrode into a living subject's heart, a bipolar potential diagram and a monopolar potential from one of the electrodes at a location within the heart. Recording a diagram and defining a time interval including a window of interest where the rate of change of potential of the bipolar electrogram exceeds a predetermined value. The method comprises establishing a monopolar electrogram annotation, wherein the annotation indicates a maximum rate of change of the monopolar electrogram potential within the window of interest, and assigning a quality value to the annotation; Generating a three-dimensional map of a portion of the heart including the annotation and its quality value.
According to another aspect of the method, recording the bipolar electrogram includes establishing a dual bipolar electrode arrangement of the electrodes. The dual bipolar electrode arrangement includes a first differential signal from the first monopolar electrode pair and a second differential signal from the second monopolar electrode pair, wherein the bipolar electrogram is the first difference signal Measured as the time-varying difference between the motion signal and the second differential signal.
According to yet another aspect of the method, establishing the annotation includes calculating a wavelet transform of the monopolar electrogram.
An additional aspect of the method includes generating a wavelet transform scalogram and determining a maximum rate of change in the scalogram.
Yet another aspect of the method includes identifying from the quality value that the annotation is a qualified annotation that meets a predetermined blocking criterion, and the map includes a qualified annotation on or near a blocked region of the heart. Indicating that there is.
According to yet another aspect of the method, establishing the annotation includes removing a ventricular far-field component from the monopolar electrogram.
According to one aspect of the method, the step of establishing the annotation determines whether the temporal cycle length of the monopolar electrogram in the annotation is within a predefined statistical boundary of the temporal cycle length of other annotations. Determining.
An additional aspect of the method includes adjusting the quality value of the annotation according to at least one of the quality value, the distance between annotations, and the timing of another annotation.
According to another aspect of the method, other annotations were generated from another monopolar electrogram read from another of the electrodes.
A further aspect of the method includes filtering the monopolar electrogram by an amount sufficient to reduce noise to a predetermined level, and assigning a quality value includes determining the amount.
In accordance with an embodiment of the present invention, there is further provided an apparatus comprising an in-vivo probe having a plurality of electrodes. The probe is configured to contact heart tissue. The apparatus includes a display and a processor, the processor receiving electrical signals from the electrodes and recording bipolar and monopolar electrograms from one of the electrodes at a location in the heart; Defining a time interval including a window of interest whose rate of change of potential exceeds a predetermined value and establishing an annotation of a monopolar electrogram, wherein the annotation is a potential of a monopolar electrogram within the window of interest Indicating a maximum rate of change of the method, assigning a quality value to the annotation, and generating a three-dimensional map of a portion of the heart on the display, the map including the annotation and its quality value; , Configured to perform.
According to a further aspect of the apparatus, the probe has a plurality of radial portions, each of the radial portions having at least one electrode.
According to one aspect of the apparatus, the probe is a basket catheter having a plurality of ribs, each rib having at least one electrode.
For a better understanding of the invention, reference will now be made, by way of example, to the detailed description of the invention, which should be read in conjunction with the following drawings, in which like elements have like reference numerals: It is.
1 is a diagram of a system for detecting an abnormal electrical activity region of a living heart according to an embodiment of the present invention. FIG. FIG. 3 is a group of bipolar potential diagrams according to an embodiment of the present invention. FIG. 3 is a view of a basket ventricular mapping catheter used in accordance with an embodiment of the present invention. FIG. 3 is a view of a spline catheter used in accordance with an embodiment of the present invention. 3 is a flowchart of a method for annotating an electroanatomical map of a heart according to an embodiment of the present invention. FIG. 4 is a block diagram of monopolar local excitation arrival time detection according to an embodiment of the present invention. It is a detailed block diagram of the aspect of monopolar local excitement arrival time detection shown in FIG. It is a detailed block diagram of the aspect of monopolar local excitement arrival time detection shown in FIG. FIG. 9 shows signals processed according to the diagram shown in FIG. FIG. 6 is a block diagram illustrating wavelet detection according to an embodiment of the present invention. FIG. 11 is a diagram illustrating signals generated by the configuration shown in FIG. 10 according to an embodiment of the present invention. FIG. 6 shows different arrhythmia wavelet transforms according to an embodiment of the present invention. FIG. 6 is a set of diagrams illustrating the removal of interfering signals from a monopolar fibrillation signal according to an embodiment of the present invention. It is a graph which shows the annotation of the electrogram by embodiment of this invention. FIG. 6 is a graph illustrating an annotation of electrical activity in the case of atrial fibrillation, according to an embodiment of the present invention. FIG. 6 is a graph showing an annotation of electrical activity according to an embodiment of the present invention.
In the following description, numerous specific details are set forth in order to facilitate a thorough understanding of the various principles of the present invention. However, those skilled in the art will appreciate that not all of these details are necessarily required for the practice of the present invention. In this case, details of well-known circuits, control logic, and computer program instructions relating to conventional algorithms and processes are not shown in detail in order not to unnecessarily obscure the general concepts.
“Annotation” or “annotation point” indicates a point or candidate on the electrogram that is considered to indicate an event of interest. In this disclosure, the event is the start of propagation of radio waves (local excitement arrival time) normally detected by the electrodes.
As used herein, electrogram “activity” is used to mean a distinct region of explosive or undulating changes in an electrogram signal. Such a region can be seen as prominent among regions of the baseline signal. In this disclosure, “activity” often refers to the electrogram expression of one or more electric propagating waves through the heart.
Turning now to the drawings and referring first to FIG. 1, which is a diagram of a system 10 for detecting an abnormal electrical activity region of a heart 12 of a living body 21, in accordance with an embodiment of the present invention. The system includes a probe, usually a catheter 14, which is inserted percutaneously by an operator 16, usually a physician, and enters the heart's ventricle or vasculature through the patient's vasculature. The operator 16 brings the catheter distal tip 18 into contact with the heart wall at the target site to be diagnosed. Monopolar and bipolar electrograms are recorded using mapping electrodes on the distal segment of the catheter. Then, according to the methods disclosed in the above-mentioned US Pat. Nos. 6,226,542 and 6,301,496, and US Pat. No. 6,892,091 by the same applicant, An activation map is created. The above disclosure is incorporated herein by reference.
System 10 may include a general purpose or embedded computer processor, which is programmed with suitable software for performing the functions described below. Thus, although the portion of system 10 shown in other figures herein is shown to include several individual functional blocks, these blocks are not necessarily separate physical entities, eg, a processor May represent different computational tasks or data objects stored in accessible memory. These tasks can be performed by software running on a single processor or multiple processors. The software can be provided to one or more processors in a tangible non-transitory medium such as a CD-ROM or non-volatile memory. Alternatively or additionally, system 10 may include a digital signal processor or hardwired logic.
The catheter 14 typically includes a handle 20 having suitable controls that allow the operator 16 to turn, position, and orient the distal end of the catheter as needed to perform ablation. To assist the operator 16, the distal portion of the catheter 14 houses a position sensor (not shown) that provides a signal to a positioning processor 22 distributed within the console 24. The catheter 14 can be made from the ablation catheter described in commonly assigned US Pat. No. 6,669,692, with the necessary modifications. The above disclosure is incorporated herein by reference. The console 24 typically includes an ECG processor 26 and a display 30.
The positioning processor 22 measures the position and orientation coordinates of the catheter 14. In one embodiment, the system 10 includes a magnetic position tracking system that determines the position and orientation of the catheter 14. The system 10 typically includes a set of external radiators, such as a magnetic field generating coil 28, which are located at certain known locations outside the patient's body. The coil 28 generates an electromagnetic field in the vicinity of the heart 12. These fields are detected by a magnetic field sensor provided on the catheter 14.
Although not shown in the figures for simplicity, the system 10 typically includes other elements. For example, the system 10 may include an electrocardiogram (ECG) monitor coupled to receive signals from one or more body surface electrodes to provide an ECG synchronization signal to the console 24. The system 10 typically includes an externally applied reference patch attached to the exterior of the subject's body, or a catheter inserted and placed within the heart 12 that is maintained in a fixed position relative to the heart 12. A reference position sensor is also included on either. Conventional pumps and lines may be provided to circulate the catheter 14 through the liquid for cooling the ablation site.
One system that embodies the above features of system 10 is Biosense Webster, Inc. CARTO® 3 System, available from (3333 Diamond Canyon Road, Diamond Bar, CA 91765). This system can be modified by one of ordinary skill in the art to embody the principles of the invention described herein. Multi-electrode baskets and spline catheters that are suitable for obtaining monopolar and bipolar electrograms are known. An example of such a spline catheter is the Pentalay® NAV catheter available from Biosense Webster.
To better illustrate the problems that can be solved by applying the principles of the present invention, reference is now made to FIG. 2, which is a group of bipolar electrograms according to embodiments of the present invention, which are simulated here. Bipolar electrodes are placed in eight directions. A bipolar electrogram is calculated from the difference between the squares 32, 34 shown in the characteristic hatching pattern of the monopolar electrogram, eg, the electroanatomical map 36, where one pole is fixedly placed on the square 32 and the other The pole rotates in 8 steps (4 vertical and 4 tilted positions) around the fixed pole position. In the map 36, the activation wave propagates slightly diagonally from right to left. The morphology observed from the eight bipolar complexes is different. This group shows complex activation resulting from the fusion of two waves, which leads to a large difference in the form and amplitude of the bipolar complex within the window of interest 38. FIG. 2 illustrates the ambiguity of detection of activation. The local excitement arrival time passing through a point where the activation wave passes is calculated by placing an event on an electrogram that satisfies the criteria described later, and subtracting the time of the reference from the time of the event. The time of the reference event can be defined using another intracardiac signal or body surface electrocardiogram.
The following two figures are schematic views of the distal end of a catheter used to obtain an electrical potential from the heart, according to one embodiment of the present invention.
Reference is now made to FIG. 3, which is an illustration of a basket ventricular mapping catheter 40 used in accordance with an embodiment of the present invention. Catheter 40 is similar in design to the basket catheter described in US Pat. No. 6,748,255 (Fuimaono et al.), Which is assigned to the assignee of the present invention and is hereby incorporated by reference. Embedded in the book. The catheter 40 has a plurality of ribs, and each rib has a plurality of electrodes. In one embodiment, the catheter 40 has 64 monopolar electrodes and can be configured with up to 7 bipolar pairs per spline. For example, the rib 42 has monopolar electrodes M1-M8 with bipolar configurations B1-B7. The distance between the electrodes is 4 mm.
Reference is now made to FIG. 4, which is an illustration of a spline catheter 44 used in accordance with an embodiment of the present invention. An example of such a spline catheter is the Pentalay® NAV catheter available from Biosense Webster. The catheter 44 has a plurality of splines, each spline having a number of electrodes. In one embodiment, the catheter 44 has 20 monopolar electrodes, which can be configured as two or three bipolar pairs per spline. For example, the spline 46 has a first pair of monopolar electrodes 48, 50 and a second pair (M1-M4) of monopolar electrodes 52, 54. The difference between each monopolar electrode pair is calculated in blocks 56 and 58. The outputs of blocks 56, 58 (B1, B2) may be related to each other to form a hybrid bipolar electrode configuration, an arrangement referred to herein as a “double bipolar configuration”. A dual bipolar configuration is used to establish the bipolar window of interest as described below. Possible interelectrode distances are 4-4-4 or 2-6-6 mm. A similar bipolar configuration can be established with catheter 40 (FIG. 3).
Both catheters 38, 44 are examples of distal ends having multiple electrodes and having multiple electrodes on their individual splines, spokes, or branches, and inserting the distal ends into the patient's heart can do. Embodiments of the present invention use catheters such as catheters 38, 44 to simultaneously acquire time-varying potentials from different regions of the heart. If atrial fibrillation is occurring in the heart, the acquired potential is analyzed to characterize those transitions in the heart.
Reference is now made to FIG. 5, which is a flowchart of a method for annotating an electroanatomical map of the heart, according to an embodiment of the present invention. The processing steps are shown in a specific linear order for clarity. However, it will be apparent that many of these processing steps may be performed in parallel, asynchronously, or in a different order. One skilled in the art will appreciate that the process may alternatively be expressed as a number of interrelated states or events, for example, in a state diagram. Moreover, not all illustrated processing steps may be required to implement the method.
The method includes analyzing a potential obtained by the plurality of catheter electrodes while the subject is experiencing a conduction disturbance (eg, atrial fibrillation). Initially, the potential signal is obtained as a bipolar potential plotted over time, usually by finding the differential signal between adjacent electrode pairs. However, the electrode pairs need not be adjacent, and in some embodiments, bipolar signals from non-adjacent electrodes are used. For bipolar signals, information about the three-dimensional position of the electrodes can be used. Alternatively or additionally, information regarding the electrode placement of the catheter can be used.
In the first step 60, a relatively large change in potential, i.e.
The bipolar signal is analyzed to determine the initial period or window where there is a maximum value of.
Reference is now made to FIG. 6, which is a block diagram of a method of monopolar local excitation arrival time (LAT) detection, according to an embodiment of the present invention. Unipolar electrogram (EGM) input 62 is processed to eliminate the ventricular far-field effect of block 64. Far-field reduction can be achieved using the teaching of application number 14 / 166,982 by the same applicant whose title is Hybrid Bipolar / Unipolar Detection of Activation Wavefront. The above content is incorporated herein by reference. At block 66, pre-filtering is performed, which can be accomplished using high pass and low pass filters (eg, FIR and IIR filters). The output of block 66 is then processed by wavelet detection block 68, the details of which will be described later.
The output of block 66 forms the input 70 of double bipolar electrogram calculation block 72. Another input 74 of block 72 conveys the identity of the electrodes used to calculate the bipolar signal, which is output signal 76. Each member of the bipolar pair is constructed as described with respect to catheter 44 (FIG. 4). For example, the inputs 70, 74 of the block 72 may be monopolar electrodes 48, 50 (FIG. 4) of the catheter 44. Block 56 in FIG. 4 corresponds to block 72 in FIG. The start and end of bipolar EGM is established at block 78. This can be accomplished by the teaching of US Patent Application Publication No. 2013/0281870 by the same applicant. The above contents are incorporated herein by reference. A window of interest for the bipolar electrogram is established at block 80 using the outputs of block 68 and block 78.
Reference is now made to FIG. 7, which is a detailed block diagram illustrating the operation of block 72 (FIG. 6) according to an embodiment of the present invention. The two EGM inputs 82, 84 are prefiltered far field components that are removed at blocks 86, 88. Inputs 82 and 84 are typically generated from adjacent electrode pairs, and each member of the electrode pair itself constitutes a bipolar source as shown in FIGS. For example, the input 82 may come from the monopolar electrode 50 (FIG. 4). The outputs of blocks 86 and 88 are subtracted at block 92 to produce a dual bipolar output signal 94. The signal 94 is subjected to another pre-filtering step at block 96 and the notch is removed at block 98 and the output signal 100 is submitted to block 102 where the bipolar window of interest is determined. Block 102 generates an output signal 104.
Reference is now made to FIG. 8, which is a detailed block diagram illustrating a portion of the operation of block 102 (FIG. 7) according to an embodiment of the present invention. Signals 106 and 108 represent successive provisional window decisions (signal 104 (FIG. 7)) and are evaluated at window detection blocks 110 and 112, which detect output signals 114 and 116, respectively. Is generated. The maximum value between the two minimums is detected. Signals 114 and 116 are processed at block 118 to determine the overlap of the detected windows. If there is more than 20% overlap, at block 120, the windows found at blocks 110, 112 are merged. Block 120 outputs a signal 122 representing the window of interest.
Reference is now made to FIG. 9, which is a diagram illustrating signals processed according to the configuration of FIG. 8, in accordance with an embodiment of the present invention. Graphs 124, 126 represent the output of blocks 110, 112, showing the electrogram form and the respective detected windows. For example, the windows 128, 130 overlap extensively and are therefore fused, as shown in the graph 132. Graph 132 shows the superposition of the electrograms of graphs 124, 126 and the fusion of windows 128, 130 to form a larger window 134. The window 134 starts from a point 136 that is the minimum start time of the windows 128 and 130 and ends at a point 138 that is the maximum end time of the windows 128 and 130.
Reference is now made to FIG. 10, which is a detailed block diagram illustrating the operation of the wavelet detection block 68 (FIG. 6) according to an embodiment of the present invention. The wavelet transform provides a decomposition of the signal as a set of (orthogonal) basis functions that are derived from the mother wavelet by magnification and translation. If the wavelet is a derivative of the smoothing function, the wavelet coefficient represents the slope of the input signal. The wavelet parameters used in the configuration of FIG. 10 are (1) continuous wavelet transform (CWT), (2) first derivative of Gaussian wavelet, and (3) block 141 followed by ratings and peak detection in blocks 145, 147, 143 of 15 resolutions on 15 linear scales.
Reference is now made to FIG. 11, which is a diagram illustrating signals generated by the configuration shown in FIG. 10, in accordance with an embodiment of the present invention. In the wavelet transform block 142, a scalogram 140 is generated from the electrogram 144 by forming an ordered set of curves with chain maxima and minima, ie, iterative filtering. Although time intervals, for example, time intervals 146, 148, indicate maximum and minimum values that are readily discernable in the scalogram 140, these are not so obvious in the electrogram 144.
Reference is now made to FIG. 12, which illustrates the operation of the different arrhythmia wavelet transform block 68 (FIG. 6), according to an embodiment of the present invention. The local electroanatomical map 150 shows various types of atrial arrhythmia abnormalities associated with atrial fibrillation. The map 150 is shown by a corresponding electrogram 152 and a scalogram 154. Scalogram 154 has a different form for each electrogram 152. In general, the peaks of the electrogram 152 are more clearly separated in the scalogram 154, especially when activation is less clear, as in the case 156, 158 on the right of the figure.
Returning to FIG. 5, in the signal conditioning step 160, the interfering signal is removed from the unipolar fibrillation signal to expose the fibrillation signal. Interfering signals include ventricular far-field signals or components emitted from the ventricles. In one method of removing these components, a signal radiating from the ventricle is detected and the average QRS signal is subtracted from the fibrillation signal when the ventricular signal is generated.
Reference is now made to FIG. 13, which is a set of diagrams illustrating the removal of interfering signals from a unipolar fibrillation signal, according to an embodiment of the present invention. As shown in the first portion 162, the fibrillation signal initially includes a ventricular far-field portion. The average QRS signal is typically generated from a set of QRS signals, as shown in the second portion 164, and the fibrillation signal subtracts the average QRS signal, as shown in the third and fourth portions 166. It is corrected by.
Alternatively or additionally, templates based on template matching to predefined ventricular signals and / or estimation from fibrillation signals can predict a ventricular far-field signal of a unipolar fibrillation signal if the signal is only ventricular. Can be used for. Usually, the time at which a ventricular signal is expected to occur can be determined from a body ECG signal, a ventricular intracardiac signal, or a coronary sinus signal. Using the template, the ventricular far field signal or component can be calculated and subtracted from the fibrillation signal.
Those skilled in the art will be able to adapt the above description to other methods of removing ventricular far-field signals, making the necessary changes. Furthermore, disturbing signals other than ventricular far-field signals can be removed by methods similar to those described above for ventricular signals.
Other adjustments that can be performed in the signal conditioning step by any method known in the art include noise reduction (including induced noise due to 50/60 Hz signals), electromagnetic interference (EMI) reduction, and baseline variation. Including correction.
Returning to the flowchart of FIG. 5, in a further analysis step 168 performed on the adjusted unipolar fibrillation signal, the maximum
The time at which is detected is determined. Biggest
The process of determining the value is applied to the adjusted signal in the window found in the initial analysis initial step 60 and further includes a noise reduction process. In one embodiment, noise reduction applied to the corrected fibrillation signal includes forming a composite of different wavelet transforms using the corrected fibrillation signal. Different wavelet transforms effectively produce filters with different bandwidths, and the synthesis of these filters with the corrected fibrillation signal reduces the noise of the signal.
Additionally or alternatively, other methods of noise reduction can be applied to the corrected fibrillation signal within the above window, for example by applying one or more different bandwidth filters to the signal. .
In the quality assessment step 170, each maximum is determined according to the amount and type of filtering required to determine the annotation in step 168.
An annotation can be assigned a parameter that measures the goodness of the annotation. For example, annotations assigned by high parameter values can be returned for both low and high levels of filtering, while annotations assigned by low parameter values can be returned only for low or high filter levels, but both Not about.
The annotation is further characterized to evaluate the final quality of the annotation. Characterization is based on the position of the electrodes that generate those signals, the position at which the signal is acquired in the heart, the timing of the annotation, the goodness parameters of the annotation (determined in the previous step), and / or the annotation Whether or not the signal adjustment described above in the step is performed or close is determined. Each of these parameters can be assigned a numerical value. For example, from the position of the first electrode, if it is considered physiologically unlikely that the signal acquired by the electrode contains an annotation, the final quality of the annotation can be reduced. For the second electrode, the final quality of the annotation can be increased if the signal is likely to contain the annotation.
In addition to the above variables for assessing the quality of a given annotation, you can check the quality of adjacent space annotations, the distance between annotations, and timing, and adjust the quality of a given annotation accordingly . For example, if a given electrode is surrounded by electrodes that produce annotation with high quality, the quality of the given electrode annotation may increase in some cases (as described below with respect to step 28). In this case, there can be a blocking effect). Alternatively, the quality of a given electrode annotation may be reduced if the given electrode is surrounded by electrodes that produce annotation with low quality. Furthermore, the quality of a given electrode can be further reduced if the given electrode is surrounded by electrodes that generate quality annotations significantly outside the physiological range.
As a further check to determine the quality of the annotation, the annotation is evaluated against statistics describing other annotations. For example, a histogram of the temporal cycle length of each annotation can be generated. Only those annotations that are within the predefined boundaries of the histogram can be considered valid, and annotations that are outside the boundaries are considered to be incorrect.
In a blocking identification step 172, the region of the heart that appears to have been “blocked” for myocardial activation is considered, taking into account annotations that meet the criteria assigned in step 170. Such blocking occurs when the activation wave collides or separates, temporarily saturating the cardiomyocytes at the location of the collision, so that the cardiomyocytes cannot be reactivated. These are known as “refractory cells”. Blocked regions can be identified by considering the signals of a given electrode as well as surrounding electrodes. Typically, a given electrode is a blocked region of the heart if the annotation signal of the given electrode is significantly smaller than the surrounding electrode annotation signal, has a different morphology, and / or has a lower quality. Or it can be considered that it is located in the vicinity. The block may be temporary (functional block) or permanent (eg, scar).
In display step 174, the results of the two previous steps, ie, high quality annotations and regions identified as being blocked, are displayed in a dynamic 3D map of the heart or ventricle. Usually, a dynamic map shows the relative timing and quality of cardiac annotations and the calculated “flow” of annotations, ie the time interval between successive annotations. The dynamic map also shows the regions of the heart that are considered blocked. A dynamic map can also indicate the region of the heart or ventricle for which no information was acquired.
Reference is now made to FIG. 14, which is a graph illustrating the annotation of electrogram 176 according to an embodiment of the present invention. The lower part of the figure details the process applied to the representative complex 178. Hybrid bipolar windows 180, 182 are obtained from the two monopolar electrodes as described above. Traces 184, 186 represent the first derivative of the signal from the two monopolar electrodes. Scalogram 188 was created from a wavelet transform calculated based on electrogram 176. A series of annotations 190 is shown in the scalogram 188.
Reference is now made to FIG. 15, which is a graphical diagram illustrating annotation of electrical activity in the case of atrial fibrillation, according to an embodiment of the present invention. Trace 194 is the superimposed body surface electrode signal. Annotations are shown for some complexes in the scalogram 196 at the bottom of the figure, further indicated by the number of triangles at the bottom of the figure. For example, the annotation indicated by arrow 198 is associated with only two triangles 200 and is of relatively low quality compared to the annotation indicated by arrow 202 associated with a greater number of triangles 204. In the middle part 206, the quality of the annotation is further illustrated graphically. The technology has successfully annotated the complex subdivision portion 208 of activity 192.
Reference is now made to FIG. 16, which is a graphical diagram illustrating annotations of electrical activity according to an embodiment of the present invention. This representation is similar to FIG. The quality of the annotation is further indicated by dots 210. Dot 210 represents a chain starting from the finest scale and going to the coarser scale. By inspecting the chain indicated by the dot 210 along with the chain indicated by the triangle traveling in the opposite direction, the operator can distinguish between the various activation patterns indicated by the scalogram 154 (FIG. 12).
Those skilled in the art will appreciate that the present invention is not limited to what has been particularly shown and described hereinabove. Rather, the scope of the present invention includes various combinations and partial combinations of the features described above, as well as variations and modifications of features not found in the prior art that would occur to those skilled in the art upon reading the above description. Is also included.
Inserting a probe with electrodes into the heart of a living subject;
Recording a bipolar electrogram and a monopolar electrogram from one of the electrodes at a location in the heart;
Defining a time interval including a window of interest in which the rate of change of potential of the bipolar electrogram exceeds a predetermined value;
Establishing an annotation of the monopolar electrogram, wherein the annotation indicates a maximum rate of change of the potential of the monopolar electrogram within the window of interest; and
Assigning a quality value to the annotation;
Generating a three-dimensional map of the portion of the heart, the map comprising the annotation and its quality value.
(2) recording the bipolar electrogram includes establishing a double bipolar electrode arrangement of electrodes, the double bipolar electrode arrangement comprising: a first differential signal from a first monopolar electrode pair; Including a second differential signal from a second monopolar electrode pair, wherein the bipolar electrogram is a time-varying difference between the first differential signal and the second differential signal. The method of embodiment 1, wherein the method is measured.
(3) The method according to embodiment 1, wherein establishing the annotation comprises calculating a wavelet transform of the monopolar electrogram.
4. The method of embodiment 3, further comprising the step of generating a scaleogram of the wavelet transform and determining the maximum rate of change in the scaleogram.
(5) identifying from the quality value that the annotation is a qualified annotation that satisfies a predetermined blocking criterion;
The method of claim 1, further comprising: indicating on the map that the eligible annotation is at or near a blocked area of the heart.
6. The method of embodiment 1, wherein establishing an annotation comprises removing ventricular far field components from the monopolar electrogram.
(7) establishing an annotation comprises determining whether the temporal cycle length of the monopolar electrogram in the annotation is within a predefined statistical boundary of the temporal cycle length of other annotations; The method of embodiment 1, comprising.
8. The method of embodiment 1, further comprising the step of adjusting the quality value of the annotation according to at least one of a quality value, an inter-annotation distance, and another annotation timing.
9. The method of embodiment 8, wherein the other annotation is generated from another unipolar electrogram read from another of the electrodes.
10. The embodiment of claim 1, further comprising filtering the monopolar electrogram by an amount sufficient to reduce noise to a predetermined level, and assigning a quality value comprises determining the amount. the method of.
(11) A device,
An intracorporeal probe having a plurality of electrodes and configured to contact heart tissue;
A processor for receiving an electrical signal from the electrode;
Generating a three-dimensional map of a portion of the heart on the display, the map including the annotation and the quality value thereof, a processor configured to perform Including equipment.
(12) recording the bipolar electrogram includes establishing a double bipolar electrode arrangement of electrodes, the double bipolar electrode arrangement comprising: a first differential signal from a first monopolar electrode pair; Including a second differential signal from a second monopolar electrode pair, wherein the bipolar electrogram is a time-varying difference between the first differential signal and the second differential signal. The apparatus of embodiment 11 to be measured.
(13) The apparatus of embodiment 11, wherein establishing the annotation comprises calculating a wavelet transform of the monopolar electrogram.
14. The apparatus of embodiment 13, further comprising: generating a scaleogram of the wavelet transform and determining the maximum rate of change in the scaleogram.
(15) identifying from the quality value that the annotation is a qualified annotation that satisfies a predetermined blocking criterion;
12. The apparatus of embodiment 11, further comprising: indicating on the map that the eligible annotation is at or near a blocked area of the heart.
16. The apparatus of embodiment 11, wherein establishing the annotation comprises removing a ventricular far field component from the monopolar electrogram.
(17) establishing the annotation comprises determining whether the temporal cycle length of the monopolar electrogram in the annotation is within a predefined statistical boundary of the temporal cycle length of other annotations; The apparatus of embodiment 11 comprising.
18. The apparatus according to embodiment 11, wherein the probe has a plurality of rays and each of the radial parts has at least one electrode.
19. The apparatus of embodiment 11, wherein the probe is a basket catheter having a plurality of ribs, each rib having at least one electrode.
A method of removing an interfering signal from a unipolar fibrillation signal,
Receiving a first monopolar electrogram and a second monopolar electrogram;
Generating an average QRS template;
Subtracting the average QRS template from the first monopolar electrogram to obtain a first generated monopolar electrogram;
Subtracting the average QRS template from the second monopolar potential diagram to obtain a second generated monopolar potential diagram;
Subtracting the first generated monopolar potential diagram from the second generated monopolar potential diagram to generate a bipolar potential diagram.
Generating the average QRS template;
Identifying the occurrence of a plurality of series of QRS signals in the first unipolar electrogram;
Identifying an average of the series of QRS signals;
The method of claim 1, further comprising: generating the average QRS template from an average of the plurality of series of QRS signals.
The method of claim 1, further comprising generating the average QRS template from a pre-defined ventricular signal.
The method of claim 1, further comprising: predicting a ventricular far field signal of the unipolar fibrillation signal if the fibrillation signal is ventricular only.
2. The method of claim 1, further comprising identifying a plurality of series of QRS signal occurrences in each of the first monopolar electrograms from one or more of a body ECG signal, a ventricular intracardiac signal, or a coronary sinus signal. The method described in 1.
Each of the subtracting processes
Identifying each time of occurrence of a plurality of series of QRS signals in each of the unipolar electrograms;
Subtracting the average QRS template from the first or second monopolar electrogram at a time specified in each of the generation of the series of QRS signals in the first or second monopolar electrogram. ,
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JP2019124274A Pending JP2019188208A (en) 2014-01-29 2019-07-03 Double bipolar configuration for atrial fibrillation annotation
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