Patent Grant
9159539
The present disclosure relates to the chemical and/or molecular analysis of materials. More particularly, for example, the present disclosure relates to the mass spectrometry analysis of materials (e.g., analysis of one or more surface layers of materials, including solids and biomaterials).
The chemical and molecular analysis of the surface and thin surface layers of solid materials is usually based on the energetic stimulation of the sample surface and the mass spectrometry analysis of fragments ejected from the surface. There are two commonly used types of instruments used for this type of analysis.
The first of the two common types of instruments is based on the use of “primary” ion beams to excite the sample and to eject charged atomic and molecular species (referred to as “secondary” ions) that are analyzed by a mass spectrometer. This type of instrumental technique is normally called Secondary Ion Mass Spectrometry (SIMS). The SIMS instrument may also have an additional mode of ionizing neutral fragments that are emitted at the same time as the secondary ions and this mode of operation is normally called Post Ionization SIMS. To obtain the highest collection efficiency, sensitivity, and separation of the different species based on the mass-to-charge (m/z) ratio of these species, a Time-of-Flight (TOF) mass spectrometer may be used in this SIMS instrument. The technique is therefore commonly referred to as TOF-SIMS. The TOF-SIMS instrument may be used in various other operating modes. For example, with the use of a scanned, micro-focused primary ion beam, mass resolved images of the sample can also be obtained with the TOF-SIMS instrument; this is generally known as the microprobe mode of operation. Further, a microscope mode of operation of the TOF mass spectrometer can also be used to obtain mass resolved images of the sample with the TOF-SIMS instrument. Exemplary embodiments thereof, for example, are described in U.S. Pat. No. 5,128,543, herein incorporated by reference.
The second type of instrument uses a photon source to excite the sample material to cause the ejection of fragments from the surface. The analysis of the fragments emitted as charged particles (i.e., ions) from the surface by a mass spectrometer is commonly known as Laser Desorption Mass Spectrometry. To increase the efficiency of the emission of charged particles (i.e., ions), specially selected organic matrix materials can be added to the surface of the sample. This refinement is commonly known as Matrix Assisted Laser Desorption Ionization (MALDI). To obtain the highest collection efficiency, sensitivity and separation of the different emitted species based on the mass-to-charge ratio, a Time-of-Flight mass spectrometer is normally used in this MALDI instrument although other types of mass spectrometers have also been used in MALDI instruments. With the use of a scanning stage and a micro-focused laser photon source, mass resolved images of the sample can also be obtained with MALDI; this is generally known as the microprobe mode of operation. A microscope mode of operation of the TOF mass spectrometer can also be used to obtain mass resolved images of the sample with MALDI analysis. Exemplary embodiments thereof, for example, are described in the article, S. L. Luxembourg, et al., “High Spatial Resolution Mass Spectrometric Imaging of Peptide and Protein Distributions on a Surface Imaging Mass Spectrometry”, Anal. Chem. 2004 76(18) 5339-5344 as well as in the article, L. A. McDonnell et al., “Imaging Mass Spectrometry”, Mass Spectrometry Reviews, 2007, 26, 606-643, both herein incorporated by reference.
The unique identification of the charged species emitted with either the TOF-SIMS or the MALDI techniques was historically based on the high mass resolution and mass accuracy of the TOF mass spectrometer. However, for mass-to-charge species (m/z species) with a mass above approximately 500 dalton (Da), the mass resolution and mass accuracy of the TOF mass spectrometer may not provide a unique molecular fragment identification of the emitted species. Historically, for the mass spectrometry analysis of higher mass liquid and gas phase molecules, a technique of Mass Spectrometry/Mass Spectrometry (MS/MS) has been used to provide a unique molecular fragment identification of many high mass species. This technique is based on the selection of a high mass ion in a first stage mass spectrometer (referred to as a “precursor” ion), followed by an energetic activation resulting in fragmentation of the precursor ion, followed by a second mass spectrometry analysis of the resulting fragment ions. Exemplary embodiments thereof, for example, are described by Boesl et al. in U.S. Pat. No. 5,032,722, herein incorporated by reference. The use of MALDI MS/MS is discussed in Andersson, et al., “Imaging Mass Spectrometry of Proteins and Peptides: 3D Volume Reconstruction”, Nature Methods 2008 5, 101-108 as well as L. A. McDonnell et al, “Imaging Mass Spectrometry”, Mass Spectrometry Reviews 2007, 26, 606-643, both herein incorporated by reference.
Exemplary methods and apparatus to obtain MS/MS data with the mass spectrometry spectral data containing both the precursor ion data and the fragment ion data, along with exemplary embodiments thereof, are described by Alderdice, et al. in U.S. Pat. No. 5,206,508, herein incorporated by reference. The apparatus described in U.S. Pat. No. 5,206,508 provides a tandem mass spectrometry system, capable of obtaining tandem mass spectra for each parent ion without separate spectra of precursor ions of differing mass from fragment ions of different mass. The data shown in FIG. 4 of U.S. Pat. No. 5,206,508 illustrate the overlap in the spectral display of the precursor ions and the fragment ions. This spectral overlap of precursor and fragment ions is a result of the single detector after the second mass analyzer. The overlapping of the data in the spectra makes this method and apparatus unworkable for polymer and biological samples that are typical for imaging MALDI and imaging TOF-SIMS analyses.
There are, for example, three apparatus concepts that may provide imaging TOF-SIMS data with MS/MS data based on a sequential mode of operation (e.g., imaging precursor ion mass spectrometry analysis followed by fragment ion mass spectrometry analysis). These three apparatus concepts require that a choice be made between the acquisition of secondary ion (e.g., precursor ion) mass spectrometry data or fragment ion mass spectrometry data. This defines the sequential nature of the instrument operation in such apparatus concepts. This sequential mode of operation prevents analytical TOF-SIMS data and MS/MS data from being acquired from the same analytical sample volume.
The first apparatus concept is based on a reflectron analyzer which allows the rejection of the precursor ions before the ion mirror and allows the fragment ions that result from precursor ion uni-molecular ion decay in the flight path between the sample and the reflectron to be mass analyzed (see, e.g., D. Touboul, et al., Rapid Commun. Mass Spectrom. 2006; 20: 703-709, herein incorporated by reference). This apparatus concept depends on the creation of fragment ions by the in-flight decay of metastable ions and is referred to as post-source decay (PSD). This described apparatus concept does not include an activation device between the reflectron used for precursor ion TOF-SIMS and a second mass spectrometer for acquisition of a MS/MS fragment ion spectra.
The second apparatus concept is a hybrid triple quadrupole TOF mass spectrometer equipped with an ion gun to produce TOF-SIMS ions. The apparatus concept uses a series of three quadrupole mass spectrometers followed by an orthogonal TOF mass spectrometer to acquire precursor ion TOP-SIMS data. In a second mode of operation, the second quadrupole mass spectrometer may also be used to select a precursor ion from the TOF-SIMS imaging experiment. The third quadrupole can then be operated at high gas pressure (e.g., in an activation cell) to produce fragment ions that can be measured in the orthogonal TOF mass spectrometer (see, e.g., A. Carado, et al., Appl. Surf. Sci. 2008; 255: 1610-1613, herein incorporated by reference). This described apparatus concept does not simultaneously and in parallel measure the precursor ion TOF-SIMS imaging data and the fragment ion MS/MS data.
The third apparatus concept is a reflectron analyzer with an integral gas collision cell in the reflectron flight path. This apparatus concept requires a choice between the acquisition of the precursor ions for imaging TOF-SIMS or the use of a high pressure gas in the collision cell to activate the precursor ions to produce fragment ions which can be mass analyzed in the rest of the reflectron flight path (see, J. S. Fletcher, et al., Anal. Chem. 2008; 80 9058-9064, herein incorporated by reference). This product concept cannot simultaneously and in parallel measure the precursor ion TOF-SIMS imaging data and the fragment ion MS/MS data.
The present disclosure provides apparatus, methods, and systems that may, for example, add the capability of Mass Spectrometry/Mass Spectrometry (MS/MS) to a primary mass spectrometer instrument (e.g., to a Time-of-Flight Secondary Ion Mass Spectrometry (TOF-SIMS) instrument) in a way that improves the function and analytical benefits of materials analysis. In one or more embodiments of the apparatus, methods, and/or systems, MS/MS data is acquired in parallel with imaging data of a primary mass spectrometer (e.g., imaging TOF-SIMS data). For example, at least in one embodiment, this allows TOF-SIMS data to be acquired from the same analytical sample volume as the MS/MS data. Acquired in such a manner, the MS/MS data may therefore be used to provide confident molecular fragment, and, therefore, precursor ion, identification from the same analytical sample volume as the TOF-SIMS data.
In the examples of MS/MS combined with SIMS described in the Background section hereof, the instruments can operate in either the conventional SIMS mode or the MS/MS mode, but they cannot operate in the two modes simultaneously and in parallel. For example, with respect to the first apparatus concept described in the Background section hereof, this described apparatus concept does not include an activation device between the reflectron used for precursor ion TOF-SIMS and a second mass spectrometer for acquisition of a MS/MS fragment ion spectra, and as such, cannot operate in the two modes simultaneously and in parallel. With respect to the second apparatus concept described in the Background section herein, the hybrid triple quadrupole TOF mass spectrometer equipped with an ion gun to produce TOF-SIMS ions does not simultaneously and in parallel measure the precursor ion TOF-SIMS imaging data and the fragment ion MS/MS data. Further, with respect to the third apparatus concept described in the Background section herein, this reflectron analyzer requires a choice between the acquisition of the precursor ions for imaging TOF-SIMS or the use of a high pressure gas in the collision cell to activate the precursor ions to produce fragment ions which can be mass analyzed in the rest of the reflectron flight path, and as such, cannot simultaneously and in parallel measure the precursor ion TOF-SIMS imaging data and the fragment ion MS/MS data.
In one or more embodiments of the apparatus, methods, and systems described herein, either the microprobe mode or microscope mode of imaging may be used to provide parallel acquisition from the same analytical volume of both primary mass spectrometer data (e.g., TOF-SIMS data) and separate precursor ion mass spectrometry data with fragment ion MS/MS data. In one or more embodiments, such apparatus, methods, and systems may provide for the parallel acquisition of both MALDI data in the microscope mode (e.g., stigmatic direct ion imaging) and separate precursor ion mass spectrometry data with fragment ion MS/MS data. Further, unlike the undesirable overlapping of data described in U.S. Pat. No. 5,206,508 with respect to precursor ions and fragment ions, one or more embodiments of the apparatus, methods, and systems described herein may be used to obtain separate precursor ion spectra and fragment ion spectra from mass selected precursor ions in two separate data streams from the same analytical volume.
In one embodiment of an exemplary method for the acquisition of mass spectrometry data (e.g., TOF data and/or MS/MS data), the method may include applying an excitation pulse to a sample resulting in a stream of charged particles, using a primary mass spectrometer (e.g., a time-of-flight mass spectrometer) to separate charged particles of the stream of charged particles based on their mass-to-charge ratio and detecting the charged particles in a mass-to-charge spectrum, and diverting from the stream of charged particles a stream of one or more precursor ions having a selected mass range for fragmentation to provide fragment ions. The fragment ions may be provided to a second mass spectrometer for analysis of the fragment ions during the same time as the primary mass spectrometer is separating and detecting charged particles of the stream of charged particles based on their mass-to-charge ratio.
In one embodiment of the method, diverting from the stream of charged particles a stream of precursor ions may include activating the diverted stream of precursor ions for the production of the fragment ions and providing a mass spectrometry analysis of the mass-to-charge spectrum of a plurality of masses of the fragment ions.
In another embodiment of an exemplary method for the acquisition of mass spectrometry data, the method may include applying an excitation pulse to a sample resulting in a stream of charged particles from an analytical volume, using a primary mass spectrometer (e.g., a time-of-flight mass spectrometer) to separate charged particles of the stream of charged particles from the analytical volume based on their mass-to-charge ratio and detecting the charged particles in a mass-to-charge spectrum, and providing fragment ions to a second mass spectrometer for analysis of the fragment ions (e.g., the fragment ions may be provided by fragmentation of selected particles from the resulting stream of charge particles from the analytical volume).
In one embodiment of an exemplary apparatus for acquiring mass spectrometry data (e.g., TOF data and/or MS/MS data), the apparatus may include a primary mass spectrometer (e.g., a time-of-flight mass spectrometer) configured to separate charged particles of a stream of charged particles based on their mass-to-charge ratio and detecting the charged particles in a mass-to-charge spectrum, a selection apparatus configured to select a mass range of precursor ions from the stream of charged particles, an activation apparatus configured to activate and fragment the selected precursor ions during the same time as the primary mass spectrometer separates and detects charged particles based on their mass-to-charge ratio, and a second mass spectrometer configured for mass-to-charge analysis of a plurality of masses of the fragment ions provided from the activation apparatus.
One or more embodiments of the methods and/or apparatus may include one or more of the following features: the primary mass spectrometer may include a time-of-flight mass spectrometer; the primary mass spectrometer may acquire at least one of spatially resolved mass spectrometry spectra, spatially resolved mass spectrometry images, and spatially resolved depth profiles with the spatial resolution defined by the dimensions of an incident energetic probe on the sample surface; the primary mass spectrometer may acquire at least one of spatially resolved mass spectrometry spectra, spatially resolved mass spectrometry images, and spatially resolved depth profiles with the spatial resolution defined by parallel microscope imaging of a first spectrometer ion optics; an excitation probe configured to provide the stream of charged particles may include an ion beam or a laser beam (e.g., a focused ion beam or a focused laser beam); the selection apparatus may include a three aperture structure with an electrically activatable center aperture (e.g., wherein the selection apparatus may be pulse activatable to extract selected mass-to-charge precursor ions from the stream of charged particles provided by the primary mass spectrometer and inject the selected precursor ions into the activation apparatus and the subsequent second mass spectrometer for mass spectrometry/mass spectrometry analysis); the activation apparatus may be configured to provide activation and fragmentation of the precursor ions by either collision induced dissociation (CID) in a chamber containing a gas, electron beam induced dissociation, photon beam induced dissociation, or surface induced dissociation; the stream of charged particles may include portions thereof corresponding to each of one or more pulses of an excitation probe; a selection apparatus may be operable to select a mass range of precursor ions from portions of the stream of charged particles corresponding to a selected percentage of the one or more pulses under computer control for parallel mass spectrometry/mass spectrometry analysis; the time-of-flight mass spectrometer may include a TRIFT (Triple Ion Focusing Time-of-Flight Mass Analyzer) spectrometer; the second mass spectrometer may include a linear TOF spectrometer, a reflectron TOF spectrometer, or an orthogonal TOF spectrometer; an excitation probe may include an ion beam, wherein the ion beam may include at least one of monatomic ion species, polyatomic cluster ion species, molecular ion species, and poly-molecular cluster ion species (e.g., at least one of Ga+, In+, SF5+, C60+, C602+, C70+, C702+, C12H24+, Au+, Au3+, Au32+, and Binq+ where n=1, 2, 3, 5, or 7 and q=1 or 2); and/or an excitation probe may include a gas cluster ion beam (e.g., a gas cluster ion beam that includes Arn+, where n is an integer between 1 and 5,000).
The above summary is not intended to describe each embodiment or every implementation of the present disclosure. A more complete understanding will become apparent and appreciated by referring to the following detailed description and claims taken in conjunction with the accompanying drawings.
In the following detailed description of illustrative embodiments, reference is made to the accompanying figures of the drawing which form a part hereof, and in which are shown, by way of illustration, specific embodiments which may be practiced. It is to be understood that other embodiments may be utilized and structural/process changes may be made without departing from the scope of the present disclosure. Unless stated otherwise herein, the figures of the drawing are rendered primarily for clarity and thus may not be drawn to scale.
Methods herein are described in a particular illustrated order. However, orders other than the ones illustrated are feasible. It is furthermore feasible that additional process steps not listed in the method may be carried out. It is additionally possible for individual method steps or groups of method steps to be carried out repeatedly or to be carried out such that they overlap at least partially in terms of time.
One or more embodiments of apparatus, methods, and/or systems used for the acquisition of mass spectrometry data (e.g., MS/MS data acquired in parallel with imaging TOF-SIMS data) are described with reference to
The exemplary system 10 as shown in the block diagram of
One exemplary embodiment of an apparatus for acquiring mass spectrometry data (e.g., configured to carry out one or more methods described herein) may include a TOF mass spectrometer (e.g., such as a TOF mass spectrometer including an ion extractor 14, mass spectrometer optics 30 and associated MS1 detector 32) configured to separate charged particles from a stream of charged particles 22 based on their mass-to-charge ratio and detecting the charged particles in a mass-to-charge spectrum, a selection apparatus (e.g., a precursor ion selection apparatus 40) configured to select a mass range of precursor ions from the stream of charged particles 22 (e.g., such as the selection apparatus shown in
In one or more embodiments, the ion extractor 14, the first or primary mass spectrometer 30 (MS1) and associated MS1 detector 32 may be components of a TOF analyzer used within currently available TOF-SIMS and/or MALDI systems. In one or more embodiments of such systems, the precursor ion selection apparatus 40 may be placed within an ion stream of such TOF-SIMS and/or MALDI systems. Still further, for example, the precursor activation device 36, extraction (e.g., with ion bunching) into second mass spectrometer 50 and the MS2 detector 52 may be provided as part of a MS/MS TOF-SIMS system or a MS/MS MALDI system that includes parallel acquisition of MS and MS/MS data from the same analytical volume as described herein.
The generalized exemplary flow diagram of one embodiment of the operation of an exemplary system 10 (e.g., a MS/MS TOF-SIMS system or a MS/MS MALDI system) with parallel acquisition of primary mass spectrometry data and MS/MS data from the same analytical volume as shown in
After, for example, mass separation (e.g., desired and/or sufficient separation) of the stream of precursor ions 22 (block 110) in the first mass spectrometer analyzer (e.g., a TOF mass spectrometer analyzer) including, e.g., the ion extractor 14, the first mass spectrometer 30 (MS1) and associated MS1 detector 32), and before the stream of precursor ions are detected by the first mass spectrometer MS 1 detector 32 (block 122), a user defined specific mass region of the stream of precursor ions 22 may be deflected in a mass specific precursor deflection process (block 120) (e.g., by a precursor ion selection apparatus 40) (e.g., resulting in a diverted mass selected precursor ion stream 42 and the remainder of the stream of precursor ions 41 being provided to the MS1 detector). Because the precursor ion stream 22 is a series of pulsed ions, the mass specific precursor deflection (block 120) can be controlled to deflect all of a narrow mass range of precursor ions from all of the series of pulsed ions in the stream 22 or a user defined fraction of the series of mass specific precursor ions in the stream 22. This, for example, allows the entire mass spectrum of the precursor ions in the stream 22 to be recorded at the MS1 detector 32. Based on a user defined percentage of cycles that are deflected in the mass specific precursor deflection process (block 120), the intensity of ions recorded at the MS1 detector 32 within the mass region deflected in the mass specific precursor defection process (block 120) may be normalized to reflect the percentage of deflected cycles. This allows the spectrum recorded at the MS1 detector 32 to represent an accurate intensity distribution of precursor ions within the complete mass range of precursor ions. At least in one embodiment, the stream of charged particles from the excitation of the sample (e.g., precursor ions) may include portions thereof corresponding to each of one or more pulses of an excitation probe. The selection apparatus 40 may be operable to select a mass range of precursor ions from portions of the stream of charged particles corresponding to a selected percentage of the one or more pulses (e.g., the selection apparatus 40 may be activated under computer control to divert a mass range of precursor ions from portions of the stream of charged particles that correspond to a user defined percentage of the pulses such that the diverted precursor ion stream may be fragmented).
The deflected mass specific precursor ions 42 may be fragmented in a precursor ion fragmentation process (block 130) resulting in fragment ion stream 38 (e.g., using the precursor activation device 36). The resulting fragment ions 38 may then undergo fragment mass separation (block 134) (e.g., using the second mass spectrometer 50) and detection at the MS2 detector 52. For example, in one or more embodiments, the fragmentation process (block 130) of one cycle of precursor ions, the fragment ion mass separation (block 134), and the fragment ion detection by MS2 detector 52 occurs within the cycle time duration of one cycle of precursor ion mass separation (block 110). This may allow the concept to obtain with parallel acquisition both precursor ion MS data and fragment ion MS/MS data from the same analytical volume (e.g., from the same stream of precursor ions 22 provided during a period of time from the sample 20 using the pulsed excitation source 12).
For example, one embodiment of such a method for the acquisition of mass spectrometry data as shown generally in
Further, for example, another embodiment of a method for the acquisition of mass spectrometry may include applying an excitation pulse 13 to a sample 20 resulting in a stream of charged particles 22 from an analytical volume, using a primary mass spectrometer (e.g., such as a TOF mass spectrometer including an ion extractor 14, mass spectrometer optics 30 and associated MS1 detector 32) to separate charged particles of the stream of charged particles from the analytical volume based on their mass-to-charge ratio and detecting these charged particles in a mass-to-charge spectrum (see, for example, block 110 and block 32 of
As used herein, an analytical volume refers to a volume of the sample, bounded by the sample surface, from which precursor ions, and fragment ions derived from the activation and fragmentation of selected precursor ions, are provided to other components of a system for analysis thereof.
The primary mass spectrometer (i.e., mass spectrometer MS1) used to provide the functionality described herein may be any suitable mass spectrometer (e.g., a TOF mass spectrometer, a TRIFT mass spectrometer, etc.). In one or more embodiments of the apparatus or methods described herein, the primary mass spectrometer (e.g., a TOF mass spectrometer) may acquire at least one of mass spectrometry spectra (e.g., spatially resolved mass spectrometry data), mass spectrometry images (e.g., spatially resolved mass spectrometry images), and/or depth profiles (e.g., spatially resolved depth profiles with the spatial resolution defined by the dimensions of an incident energetic probe on the sample surface) (otherwise referred to as microprobe mode of operation). Further, in one or more embodiments of the apparatus or methods described herein, the TOF mass spectrometer may acquire mass spectrometry spectra (e.g., spatially resolved mass spectrometry data), mass spectrometry images (e.g., spatially resolved mass spectrometry images), and/or depth profiles (e.g., spatially resolved depth profiles with the spatial resolution defined by parallel microscope imaging of a first spectrometer ion optics) (otherwise referred to as microscope mode of operation). In one or more embodiments of the apparatus or methods described herein, an excitation probe configured to provide the stream of charged particles may include an ion beam or a laser beam.
The excitation source 12 (e.g., a pulsed excitation source) may be any excitation source suitable for use in providing a stream of precursor ions 22 (e.g., charged particles) for analysis. For example, in one or more embodiments, the excitation source may include an ion beam or a laser beam. Further, in one or more embodiments of the apparatus or methods described herein, the excitation probe configured to provide the stream of charged particles may include a focused ion beam or a focused laser beam. For example, in one or more embodiments, the excitation probe may include an ion beam (e.g., a focused ion beam) with the ion beam including at least one of monatomic ion species, polyatomic cluster ion species, molecular ion species, and poly-molecular cluster ion species. For example, the ion beam may include at least one of, for example, Ga+, In+, SF5+, C60+, C602+, C70+, C702+, C12H24+, Au+, Au2+, Au3+, Au32+, or Binq+ where n=1, 2, 3, 5, or 7 and q=1 or 2. Further, for example, the ion beam may include glycerol, C3H8O3n+, where n is greater than or equal to 1. Still further, in one or more embodiments of the apparatus or methods described herein, an excitation probe may include a gas cluster ion beam. For example, such a gas cluster ion beam may include Arn+ where n is an integer between 1 and 5,000.
The precursor ion selection apparatus 40 may be any suitable apparatus configured to extract selected mass-to-charge precursor ions 22 from the stream of charged particles 22 provided by the TOF mass spectrometer. For example, in one or more embodiments, the selection apparatus may include a three aperture structure with an electrically activatable center aperture (e.g., wherein the selection apparatus may be pulse activatable to extract selected mass-to-charge precursor ions from the stream of charged particles provided by the time-of-flight mass spectrometer) and inject the selected precursor ions into the 36 activation apparatus and the subsequent second mass spectrometer 50 for MS/MS analysis. One or more embodiments of exemplary selection apparatus are further described herein.
The precursor ion activation apparatus 36 may be any suitable apparatus configured to provide activation and fragmentation of the precursor ions. As used herein, activation refers to any process of adding internal energy to any precursor ion, and further fragmentation refers to the separation of the activated ion into neutral and ionized fragments. In one or more embodiments, for example, the activation apparatus may be a device configured to provide activation and fragmentation by one of collision induced dissociation (CID) in a chamber containing a gas, electron beam induced dissociation, photon beam induced dissociation, or surface induced dissociation.
In one or more embodiments of the apparatus or methods described herein, a percentage, between, for example, 100% and 0%, of the pulsed precursor ion beams may be chosen by the control computer for parallel MS/MS analysis. The control computer may select a specific m/z precursor ion species from the entire mass range of precursor ions for parallel MS/MS analysis. This allows parallel acquisition from the same analysis volume of the entire precursor mass spectrum and the MS/MS mass spectrum of the selected precursor ion species.
The second mass spectrometer (e.g., mass spectrometer MS2, including extraction and mass spectrometer optics 50 and associated MS2 detector) used to provide the functionality described herein may be any suitable mass spectrometer configured for use in generating MS/MS data. In one or more embodiments of the apparatus or methods described herein, the second mass spectrometer may include a linear TOF spectrometer, a reflectron TOF spectrometer, or an orthogonal TOF spectrometer. Further, for example, the second mass spectrometer may be a mass spectrometer that meets the analytical requirements of parallel acquisition of all fragment ion species from the activation and fragmentation of a single m/z precursor ion species, as well high mass resolution (e.g. >2000 M/Δm at 2000 m/z) and high mass accuracy from 0 to 2000 m/z).
A combined system (e.g., such as shown and described generally in
One example of an existing TOF-SIMS apparatus that, for example, may be modified to provide the functionality described herein, is a PHI TRIFT V nanoTOF instrument (see,
For example, such a system may include processing apparatus and data storage. Data storage may allow for access to processing programs or routines and one or more other types of data that may be employed to carry out the illustrative methods or control the various processes described herein. For example, processing programs or routines may include programs or routines for performing computational mathematics, matrix mathematics, decomposition algorithms, compression algorithms (e.g., data compression algorithms), calibration algorithms, image construction algorithms, signal processing algorithms, standardization algorithms, comparison algorithms, vector mathematics, or any other processing required to implement one or more embodiments as described herein. Data may include, for example, sampled data, measurement data, signal data, electronic module status data from one or more system components, processing programs or routines employed according to the present disclosure, or any other data that may be necessary for carrying out the one or more processes described herein.
In one or more embodiments, the systems and/or methods may be implemented using one or more computer programs executed on programmable computers, such as computers that include, for example, processing capabilities, data storage (e.g., volatile or non-volatile memory and/or storage elements), input devices, and output devices. Program code and/or logic described herein may be applied to input data to perform functionality described herein and to generate desired output information. The output information may be applied as input to one or more other devices and/or processes as described herein or as would be applied in a known fashion.
The one or more programs used to implement the processes described herein may be provided using any programmable language, e.g., a high level procedural and/or object orientated programming language that is suitable for communicating with a computer system. Any such programs may, for example, be stored on any suitable device, e.g., a storage media, readable by a general or special purpose program, computer or a processor apparatus for configuring and operating the computer when the suitable device is read for performing the procedures described herein. In other words, at least in one embodiment, the system may be implemented using a non-transitory computer readable storage medium, configured with a computer program, where the non-transitory storage medium so configured causes the computer to operate in a specific and predefined manner to perform functions described herein.
The processing apparatus may be, for example, any fixed or mobile computer system (e.g., a personal computer or minicomputer). The exact configuration of the computing apparatus is not limiting and essentially any device capable of providing suitable computing capabilities and control capabilities may be used. Further, various peripheral devices, such as a computer display, mouse, keyboard, memory, printer, scanner, are contemplated to be used in combination with processing apparatus and data storage.
In
One feature of such a TOF spectrometer (e.g., the TRIFT TOF mass spectrometer) is a triple-focusing property thereof. The analyzer instrument shown in
As described herein, for example, in one or more embodiments, one or more components (e.g., a precursor ion selection apparatus, such as shown generally in
For example, to perform the parallel functionality described herein requires a device (e.g., a precursor ion selection apparatus) for diverting a user definable percentage of the series of precursor ions of a selected mass (e.g., diverting a portion of the ions produced by the series of pulses of a primary ion source from the stream of precursor or secondary ions) provided by the first mass spectrometer (MS1) (e.g., from a stream of precursor ions provided by the TRIFT TOF mass spectrometer) for further analysis in a second mass spectrometer (MS2) (generally designated as reference numeral 190 in
For example, one exemplary selection apparatus 220 (see
When precursor or secondary ions of a selected mass (e.g., a user selected mass) have entered the gap (e.g., with an initial momentum p=(2 meV0)1/2) between the outer electrode plate 219 and the middle electrode plate 226 (e.g., entered through the opening 261 in the outer electrode plate 219 and into the space between the outer electrode plate 219 and the middle or center electrode plate 226), the middle electrode plate 226 may be pulsed with the secondary or precursor ions receiving a momentum impulse equal to the electric field times the pulse width; the momentum impulse (eV1t/d=p sin(Θ)). With such a momentum impulse being applied, precursor ions of the selected mass 42 are deflected and exit the selection apparatus 220 parallel to the plates 219 and 221 through the space therebetween (e.g., the space defined between the first outer electrode plate 219 and the middle electrode plate 226) while the remainder of the secondary or precursor ions of other masses 41 which arrive earlier or later continue unaffected through the selection apparatus 220 (e.g., through the openings 262, 263 of the plates 221, 226, respectively) for analysis by the first mass spectrometer (MS1) (e.g., the TRIFT spectrometer including the detector 810).
For example, as shown in
Precursor ions 42 diverted by the selection apparatus 220 include those to be identified by fragmentation and further mass analysis in a second mass spectrometer (MS2) 190 (see, e.g.,
In one embodiment, the second mass spectrometer MS2 190 may be a linear TOF mass spectrometer as shown in FIGS. 5 and 9-10. For example, such a linear design has been described by W. E. Stephens, “A Pulsed Mass Spectrometer with Time Dispersion,” Physical Review, 1946 69, 691, which is incorporated herein by reference. For example, secondary ions in the precursor ion stream 22 of a selected mass may be deflected (e.g., by 45 degrees) by the selection apparatus 220 as shown in
Thereafter, for example, bunching and acceleration apparatus 263 may be used to provide the necessary narrowing of the energy spread of the fragment ions and the necessary high kinetic energy to provide high mass resolution, high mass accuracy and high detection efficiency in the MS2. Any suitable bunching and acceleration apparatus may be used.
In one or more embodiments, bunching and acceleration apparatus 263 may include two parallel grids forming a buncher as shown in
Further, the bunching and acceleration apparatus 263 may include acceleration optics such as shown in
Experimental Results
A prototype MS2 spectrometer was constructed and tested to demonstrate the feasibility of the MS2 design concept (see,
In summary, the experimental results validate the design concept.
The complete disclosure of the patents, patent documents, and publications cited in the Background, the Summary, the Detailed Description of Exemplary Embodiments, and elsewhere herein are incorporated by reference in their entirety as if each were individually incorporated. Exemplary embodiments of the present invention are described above. Those skilled in the art will recognize that many embodiments are possible within the scope of the invention. Other variations, modifications, and combinations of the various components and methods described herein can certainly be made and still fall within the scope of the invention. Thus, the invention is limited only by the following claims and equivalents thereto.
This application is the §371 U.S. National Stage of International Application No. PCT/US2013/030751, filed 13 Mar. 2013, which claims the benefit of U.S. Provisional Application Ser. No. 61/616,540, filed 28 Mar. 2012, entitled “Method And Apparatus To Provide Parallel Acquisition Of Mass Spectrometry/Mass Spectrometry Data,” which are incorporated herein by reference in their entireties.
| Filing Document | Filing Date | Country | Kind |
|---|---|---|---|
| PCT/US2013/030751 | 3/13/2013 | WO | 00 |
| Publishing Document | Publishing Date | Country | Kind |
|---|---|---|---|
| WO2013/148181 | 10/3/2013 | WO | A |
| Number | Name | Date | Kind |
|---|---|---|---|
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| 20150090874 A1 | Apr 2015 | US |
| Number | Date | Country | |
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| 61616540 | Mar 2012 | US |
