Abstract:
A data set processing method for Raman spectroscopy systems using tunable lasers and multielement spectrometers compiles the spectral data set into an array and then estimates the background component, which is usually dominated by sample and optical train fluorescence, detector array dark current signal, fixed-pattern signal, and stray-light signals either modulated or non-modulated by in-path optics. This estimate is used as a baseline correction to the spectral data set to thereby isolate the sample&#39;s Raman response.

Description:
RELATED APPLICATIONS  
       [0001]     This application claims the benefit under 35 USC 119(e) of U.S. Provisional Application No. 60/654,855, filed on Feb. 18, 2005, which is incorporated herein by reference in its entirety. 
     
    
     BACKGROUND OF THE INVENTION  
       [0002]     Raman spectroscopy is similar to infrared (IR), including near infrared (NIR), spectroscopy but has several advantages. The Raman effect is highly sensitive to slight differences in chemical composition and crystallographic structure. These characteristics make it very useful for substance identification such as the investigation of illegal drugs and other unknown substances as it enables distinguishing between legal and illicit compounds, even when the compounds have a similar elemental composition. In other applications, taggants, with known Raman signatures, are used as markers for goods.  
         [0003]     Raman spectroscopy has additional advantages. When using IR spectroscopy on aqueous samples, a large proportion of the vibrational spectrum can be masked by the intense water signal or absorbed by the water. This typically necessitates sample preparation. In contrast, with Raman spectroscopy, aqueous samples can be more readily analyzed since the Raman signature from water is relatively weak. Also, because of the poor water signature, Raman spectroscopy is often useful when analyzing biological and inorganic systems, and in studies dealing with water pollution problems.  
         [0004]     Raman scattering may be regarded as an inelastic collision of an incident photon with a molecule. The photon may be scattered elastically, that is without any change in its wavelength, and this is known as Rayleigh scattering. Conversely the photon may be scattered inelastically resulting in the Raman effect.  
         [0005]     There are two types of Raman transitions. Upon collision with a molecule, a photon may lose some of its energy. This is known as Stokes radiation. Or, the photon may gain some energy—this is known as anti-Stokes radiation. This happens when the incident photon is scattered by a vibrationally excited molecule—there is gain in energy and the scattered photon has a higher frequency.  
         [0006]     When viewed with a spectrometer, both the Stokes and anti-Stokes radiation are composed of lines that correspond to molecular vibrations of the substance under investigation. Each compound has its own unique Raman spectrum, which can be used as a fingerprint for identification.  
         [0007]     The Raman process is non linear. When incident photons have a low intensity, only spontaneous Raman scattering will occur. As the intensity of the incident light wave is increased, an enhancement of the scattered Raman field can occur in which initially scattered Stokes photons can promote further scattering of additional incident photons. With this process, the Stokes field grows exponentially and is known as stimulated Raman scattering (SRS).  
         [0008]     One disadvantage associated with Raman spectroscopy, however, is fluorescence Fluorescence arising from molecular relaxation radiation has been the major obstacle for Raman spectroscopy. In many cases, the fluorescence response of a sample can overwhelm the typically much weaker Raman signature. This can make detection of small peaks in the Raman signature difficult. Some data processing techniques to the fluorescence baseline corrections are not effective since they usually do not provide sufficient discrimination between the fluorescent baseline and the Raman spectra.  
         [0009]     Often, fluorescence can be mitigated by moving to a longer wavelength excitation. This can create other problems, however. Another solution to the fluorescence response is using excitation signals at multiple wavelengths. This is sometimes referred to as Shifted Excitation Raman Difference Spectroscopy (SERDS). Specifically, in the past others have suggested to use excitation signals that comprise two excitation wavelengths, generated by two different single frequency lasers. Then, by looking at the spectra generated by each of the wavelengths, the fluorescence signal can be identified since the fluorescence signal changes very little with excitation wavelength, whereas the Raman signal changes as a direct function of the excitation wavelength. In the simplest example, the spectrum at the two wavelengths is subtracted to remove the highly stationary fluorescence response. Recently, this solution has been further enhanced by using a continuously tunable semiconductor diode laser system. In these systems, the spectral response of the sample is monitored as the excitation signals wavelength is scanned over a scan range. By looking at how the spectral response changes with the tuning of the excitation signal and how it does not change, the Raman response can be separated from the fluorescence response of the sample.  
       SUMMARY OF THE INVENTION  
       [0010]     Using a continuously tunable or a small step-wise tunable laser source in combination with a multi element detector system such as a grating-based spectrometer with a linear detector array, yields a large spectral data set compromised of each detector elements sampled response at each wavelength in the tunable laser&#39;s scan range. This spectral data set must be processed to remove noise, such as the fluorescence response and thereby isolate the Raman response.  
         [0011]     The present invention concerns a data set processing method for Raman spectroscopy systems using tunable lasers and multielement spectrometers. One example of such a spectrometer is the conventional grating-based dispersive spectrometer in which a grating is used to disperse the spectrum onto a linear detector array. Other examples are the tunable multiorder multichannel Raman spectrometers described in U.S. patent application Ser. No. 10/967,075, filed Oct. 15, 2004, by Xiaomei Wang, entitled Multi Channel Raman Spectrometer System and Method, which application is incorporated herein in its entirety by this reference.  
         [0012]     The invention comprises compiling the spectral data set into an array and then estimating the background component, which is usually dominated by sample and optical train fluorescence, detector array dark current signal, fixed-pattern signal, and stray-light signals either modulated or non-modulated by in-path optics. This estimate is used as a baseline correction to the spectral data set to thereby isolate the sample&#39;s Raman response.  
         [0013]     In principle, the invention is applicable in any tunable laser based Raman spectrometers, where fluorescence is present. By effectively removing the fluorescence and any other non-Raman background, the processed spectrum reflects the true substance properties. This produces much higher identification fidelity when identifying the substances against libraries.  
         [0014]     The theory behind this invention is that the spectra of fluorescence and some other baseline background, such as sample heat radiation, are described in absolute wavelength (frequency) domain, and fully characterized by the detection wavelength only. They usually have much broader peaks than Raman spectral peaks. The Raman spectra, on the other hand, depend on the Raman shift, which is related to both excitation and detection wavelength.  
         [0015]     In general, according to one aspect, the invention features a method of processing spectral data from a Raman spectroscopy system. This spectroscopy system comprises a source for illuminating a sample at a plurality of wavelengths within a scan band. In one example, the source is a tunable laser. A spectrometer is also provided. It includes an array of detection elements. One example is a linear detector array such as a CCD or InGaAs type detector arrays. The array detects the spectral response of the sample as the source is illuminated at the plurality of wavelengths. The method comprises compiling a spectral data set including the responses of the detection elements for each of the plurality of wavelengths. The responses are then characterized based on levels of change in the response with changes in the wavelength of the illumination. Then, a baseline is determined from the responses, and the spectral data set is corrected using the determined baseline.  
         [0016]     In specific embodiments, the spectrometer comprises a dispersive element such as a grating for dispersing the spectral response over the array of detection elements. In further examples, the step of compiling the spectral data set comprises placing the spectral data set in an array of responses for each of the detection elements for each of the plurality of wavelengths. The step of characterizing responses comprising analyzing responses of each of the detection elements with changes in the wavelength of illumination. One method of characterizing these changes is to calculate a standard deviation in the responses with changes and wavelength.  
         [0017]     The baseline is then determined typically by excluding the responses of the detection elements that exhibit a large change in standard deviation. A best fit polynomial is used in one example to characterize the baseline. This baseline is then subtracted from the spectral data set.  
         [0018]     In general, according to another aspect, the invention features a Raman spectroscopy system. This system comprises a source for illuminating a sample at a plurality of wavelengths within a scan band. A spectrometer includes an array of detection elements for detecting a spectral response of the sample in response to illumination by the source at the plurality of wavelengths. A system controller controls the source and receives the responses from the detection elements of the spectrometer. The system controller processes the spectral data to determine a Raman response of the sample. This is accomplished by compiling a spectral data set including the responses of the detection elements for each of the plurality of wavelengths and characterizing the responses of the detection elements based on levels of change in the response with changes in the wavelength of the illumination. Based on this analysis, a baseline is determined for the responses, and the spectral data set is then corrected based on the response to the determined baseline.  
         [0019]     The above and other features of the invention including various novel details of construction and combinations of parts, and other advantages, will now be more particularly described with reference to the accompanying drawings and pointed out in the claims. It will be understood that the particular method and device embodying the invention are shown by way of illustration and not as a limitation of the invention. The principles and features of this invention may be employed in various and numerous embodiments without departing from the scope of the invention.  
     
    
     BRIEF DESCRIPTION OF THE DRAWINGS  
       [0020]     In the accompanying drawings, reference characters refer to the same parts throughout the different views. The drawings are not necessarily to scale; emphasis has instead been placed upon illustrating the principles of the invention. Of the drawings:  
         [0021]      FIG. 1  is a schematic diagram illustrating a Raman spectroscopy system to which the present invention is applicable;  
         [0022]      FIG. 2  is a flow diagram illustrating a method for processing a spectral data from a Raman spectroscopy system;  
         [0023]      FIG. 3  is plot of normalized response as a function of shift in wavenumbers (cm −1) for a Raman spectrum of potassium cyanide (KCN) with a Gaussian-like fluorescence baseline; and  
         [0024]      FIG. 4  is plot of normalized response as a function of shift in wavenumbers (cm −1) for a Raman spectrum of acetaminophen. 
     
    
     DETAILED DESCRIPTION OF THE PREFERRED EMBODIMENTS  
       [0025]      FIG. 1  illustrates a spectroscopy system to which the present invention is applicable. Specifically, it comprises a source  110  for generating a tunable wavelength illuminating beam  112  for irradiating the sample  10  at a plurality of wavelengths λ 1 , λ 2 , λ m . Typically, the source  100  is a tunable laser.  
         [0026]     The illumination of the sample  110  by the laser beam  112  generates a response  114 . Typically this response is a combination of the fluorescence response and the Raman response of the sample  10 .  
         [0027]     In order to resolve the spectral response of the sample  10 , a spectrometer  120  is used. As a general example, the spectrometer comprises collection optics  122  that collect light from the sample  10  and direct it to a dispersive element  124 . In the typical example, the dispersive element  124  is a grating such as a standard line grating or a holographic grating.  
         [0028]     The dispersive element  124  disperses the spectrum of the light  114  from the sample  10  in order to determine the spectral response of the sample  10 . In the specific example, grating optics  126  is used to form the spectral image on the linear detector array  128 . In the preferred embodiment, this is a linear detector array  128  comprises elements i=1, 2, . . . n. Often n is greater than 10 and typically greater than 32.  
         [0029]     A system controller  150  is used to control the tunable laser  110  and specifically control its wavelength λ. The system controller  150  also receives the responses of the detection elements i=1, 2, . . . n from the detector array  128 .  
         [0030]     According to the present invention, the system controller analyzes the spectral data from the detector array  128  in combination with the wavelength of the tunable laser  110  in order to determine the Raman spectral response of the sample  10 .  
         [0031]      FIG. 2  shows the baseline estimation method according to the principles of the present invention.  
         [0032]     The detected signal at the detector array  128  can be written as: Iij=Ii(fluorescence)+Ii(dark current)+Ii(sample heating)+Iij(Raman signal), where i=1,2, . . . , n, represents each detector and j=1, 2, . . . , m, each step wise tuning point of the laser  110  or data acquisition point in a continuously tuning mode of the laser.  
         [0033]     In one example, the scan band of the laser  110  is between 1 and 15 nanometers. In a preferred embodiment, the scan band is between 2 and 5 nanometers. The spectral responses of the detector array  128  are collected at more than 5 different wavelengths (m&gt;5) within the scan band. In the preferred embodiment, spectral responses of the detector array  128  are collected at more than 12, preferably more than 20, different wavelengths within the scan band.  
         [0034]     The responses of the detection elements at each of the wavelengths λ 1  . . . λ m  are compiled into a spectral data set  210 . Specifically, the spectral data set  210  is formed into an array of responses that holds each of the detection elements response for each of the plurality of wavelengths.  
         [0035]     Then, in step  212 , the original spectral data set  210  is sorted so that the detected responses are in ascending order for each detector individually. It produces a sorted array  214 .  
         [0036]     From the sorted array, the mean and standard deviation are calculated for each of the detectors i=1 to n in step  216 . In the current embodiment, this is performed for a selected number m 1  of data points or a number of data points determined by a user selected criterion for each detector. This criterion can be either fixed or dynamically variable based on the data set. This process produces an array of calculated mean and standard deviation values  218 .  
         [0037]     In step  220 , the standard deviation and mean array  218  is sorted and only a fixed number n 1  or a number of detectors with the standard deviation less than a threshold times the lowest standard deviation, among the detectors, are selected to produce array  222 . In short, the responses of the detector elements that exhibited the smaller changes, have lower standard deviation as a function of changes in wavelength, are identified. The responses of these detector elements that exhibited the lowest change are then used to calculate a polynomial fit as a function of detector wavelengths in step  224 . This produces a polynomial array  226 .  
         [0038]     In one embodiment, the fitting results are analyzed and any outliers are removed. The polynomials are refit and the baseline is then re-calculated. This produces the polynomial array  226 . This baseline is then subtracted in step  228 . This produces the corrected Raman spectral response array  330 .  
         [0039]     Simulations of the method&#39;s performance were performed with four different slow varying baselines: linear, parabolic, slow and fast Gaussian. Due to the nature of the multiorder multichannel detection of the tunable multiorder multichannel Raman spectrometers as described in U.S. patent application Ser. No. 10/967,075, a typical expected detected signal with fluorescent baseline is illustrated in  FIG. 3 , where the Raman spectrum is from Potassium Cyanide and the baseline  310  is assumed to be in a fast Gaussian form. A stair-like baseline presents the discrimination between Raman signal and fluorescence background.  
         [0040]     In the simulation, we used the following parameters:  
         [0041]     1. Number of detectors: n=64  
         [0042]     2. Number of tuning steps: m=41  
         [0043]     3. Number of data points used for standard deviation and calculation: m 1 =10  
         [0044]     4. Number of detectors used for baseline estimation: n 1 =30  
         [0045]     Reference  312  illustrated the baseline corrected response of KCN with a single peak.  
         [0046]      FIG. 4  shows the raw response  310  and the baseline corrected Raman response  312  for over-the-counter acetaminophen.  
         [0047]     While this invention has been particularly shown and described with references to preferred embodiments thereof, it will be understood by those skilled in the art that various changes in form and details may be made therein without departing from the scope of the invention encompassed by the appended claims.