Patent Grant
8288719
The present disclosure relates to analytical instruments, instrumentation, instrument assemblies, and analytical methods. More specific embodiments include mass analysis instrumentation as well as mass analysis methods.
Analytical instrumentation and particularly mass analysis instrumentation can be utilized to determine both the identity and amount of unknown compounds and mixtures. It is desirable to determine the identity and amount of unknown compounds and mixtures at their point of origin rather than obtaining a sample and transporting that sample to a laboratory for analysis, at least in that sampling and transportation of samples can contaminate the sample obtained and/or because sampling is not practical. Furthermore, it may be important to quickly ascertain the identity and amount of unknown compounds and sampling and transportation of the sample does not facilitate quick analysis. The capability that mass spectrometry provides is sought after for many uses including field applications where the instrument would ideally be brought to the sample rather than the more traditional transportation of the sample to the laboratory.
At least some embodiments of the analytical instrumentation and methods are portable and can be transported to where the chemistry happens, outside the laboratory.
Embodiments of the disclosure are described below with reference to the following accompanying drawings.
Analytical instruments configured to perform atmospheric pressure ionization are provided that are less than 50 kgs in total weight and/or less than 1 m3 in total volume.
Mass analysis instruments are provided that can include an interface vacuum structure operatively coupled between an ionization source and a vacuum region housing a detector.
Mass analysis instruments are also provided that can include an ionization source coupled to an analysis region via an interface vacuum structure, with at least two independent vacuum components.
Analytical instruments are provided that can include a housing encompassing an operational number of analytical components, and an ionization source being at least one of the analytical components, the ionization source being configured to be operational under atmospheric pressure; an analysis region being at least another of the analytical components, the analysis region comprising an interface region and a vacuum region, the interface region being coupled to both the ionization region and the vacuum region; and at least two vacuum sources within the housing, one of the vacuum sources being coupled to the interface region and another vacuum source being coupled to the vacuum region.
Instrumental analytical methods are provided that can include ionizing at least a portion of sample under atmospheric pressure to form a plurality of analytes, and guiding at least some of the analytes to a vacuum region for analysis using a interface region at a first pressure less than atmospheric pressure, the vacuum region being a second pressure less than the first pressure.
This disclosure is submitted in furtherance of the constitutional purposes of the U.S. Patent Laws “to promote the progress of science and useful arts” (Article 1, Section 8).
At least some embodiments provide analytical instruments, assemblies, and/or methods. Exemplary configurations of these instruments, assemblies, and/or methods are described with reference to
Referring first to
In an example embodiment, structure 12 can support, surround, and/or partially surround components 14. Components 14 can include an operational number of components, for example, all components necessary to acquire mass spectral characteristics of a sample. According to some embodiments, structure 12 can be referred to as a frame, base, case, cabinet, and/or any structure that can define a space occupied by components 14. An example material of structure 12 includes aluminum. In some configurations the space defined by structure 12 is no greater than or equal to about 1 m3 in volume. In other configurations the space defined by structure 12 is between 0.01 m3 and 0.15 m3 in volume.
According to example implementations, instrument 10 including housing 12 encompassing components 14 can have a weight no greater than or equal to about 50 kg. According to other implementations, instrument 10 can have a total weight of between 4 and 50 kgs. Exemplary configurations of instrument 10 are person-portable. Person-portable instruments include those instruments that can be transported by an individual outside the traditional laboratory. These instruments can be self-contained including a power source, or they can be configured to utilize power sources available in the field.
With reference to
As depicted in
Sample inlet component 16 can be configured to introduce an amount of sample 26 into instrument 10 (
Component 18 can be configured to convert portions or an entirety of sample 26 into analyte ions in one example. This conversion can include the bombardment of sample 26 with electrons, ions, molecules, and/or photons. This conversion can also be performed by thermal or electrical energy.
Ion source component 18 may utilize, for example, chemical ionization, and/or electrospray ionization (ESI). Also, when utilizing ESI, sample 26 can be energized under atmospheric pressure. Ion source component 18 can be configured to perform atmospheric pressure ionization, for example.
Ion source component 18 can also be configured to fragment analytes without ionizing the analytes. In exemplary implementations, the analytes may be fragmented after ionization. An exemplary fragmentation technique includes collisionally activated disassociation.
The analyte ions can proceed from ion source component 18 to mass separator component 20, for example. Mass separator component 18 can include one or more of linear quadrupoles, triple quadrupoles, quadrupole ion traps (Paul), cylindrical ion traps, linear ion traps, rectilinear ion traps, ion cyclotron resonance, quadrupole ion trap/time-of-flight mass spectrometers, or other structures. Mass separator component 18 can also include focusing lenses as well as tandem mass separator components such as tandem ion traps or ion traps and quadrupoles in tandem. In one implementation, at least one of multiple tandem mass separator components can be an ion trap. Tandem mass separator components can be placed in series or parallel. In an exemplary implementation, tandem mass separator components can receive ions from the same ion source component. In an exemplary aspect, the tandem mass separator components may have the same or different geometric parameters. The tandem mass separator components may also receive analyte ions from the same or multiple ion source components.
Analytes may proceed to detector component 22 from mass separator component 20. Example detector components include electron multipliers, Faraday cup collectors, photographic and scintillation-type detectors.
Acquisition and generation of data can be facilitated with processing and control device component 24. Exemplary embodiments provide that the progression of mass spectrometry analysis from sample inlet component 16 to detector component 22 can be controlled and monitored by a processing and control device component 24. Processing and control device component 24 can be a computer or mini-computer or other appropriate circuitry that is capable of controlling components 14. This control can include, for example, the specific application of voltages to ion source component 18 and mass separator component 20, as well as the introduction of sample 26 via sample inlet component 16, and may further include determining, storing and ultimately displaying mass spectra recorded from detector component 22. Processing and control device component 24 can contain data acquisition and searching software. In one aspect, such data acquisition and searching software can be configured to perform data acquisition and searching that includes the programmed acquisition of total analyte count. In another aspect, data acquisition and searching parameters can include methods for correlating the amount of analytes generated to predetermine programs for acquiring data.
As the space defined by structure 12 (e.g.,
Referring to
Instrument components 14 can be configured to provide mass spectral data, for example. Instrument components 14 can further include a power supply coupled to processing and control components 24 and, as necessary, inlet components 16 and analysis components 24. Exemplary power supplies can include portable batteries such as sealed lead-acid and/or lithium ion or polymer batteries. In other embodiments, the power supply may be located outside the space defined by structure 12.
Referring to
Interface region 34 can be configured to couple source 32 to vacuum region 35. Vacuum region 35 can be configured to house separator components 20 and/or detector components 22, for example. Vacuum region 35 can also house vacuum subregions 36 and 38. While
Region 34 can be configured to transfer ions from source 32 into region 35. Transfer of ions from source 32 to region 35 can be accomplished through, including but not limited to, the use of a capillary tube transfer element combined with a skimmer element to transfer ions to region 35. As such region 34 can be configured as capillary tube transfer element combined with a skimmer element. Region 34 can be maintained at a pressure less than that of source 32.
Subregion 36 can be configured to facilitate the transfer of the ions from interface 34 to subregion 38. Subregion 36 may consist of multiple vacuum regions between the pressure of the region 34 and that of the subregion 38. Transfer of ions from subregion 36 to subregion 38 may be accomplished via DC lenses, RF lenses such as octapoles, for example. Subregion 38 can include the mass analyzer, such as but not limited to quadrupole ion traps, linear ion traps, cylindrical ion traps, linear quadrupoles, time-of-flight analyzers, magnetic sector analyzers, or magnetic/electric sector combination analyzers. An example mass separator component 20 useful in accordance with one embodiment is a cylindrical ion trap (CIT). CITs typically include three components: a trapping volume and two endcaps. Typically an RF voltage is applied to the trapping volume at a predefined rate (e.g., controlled by 50) to eject trapped analytes which are subsequently detected. RF voltage ramps may include variables such as power and/or frequency. Combinations of these variables in predefined amounts are typically referred to as waveforms. Generally, waveforms can be optimized to increase detection of specific analytes of interest. Waveforms can also be optimized to allow for multiple stages of mass analysis.
In an example embodiment, mass separator component 20 within region 35 can be a cylindrical ion trap and the mass separator parameter of the cylindrical ion trap can be a parameter that influences the mass-to-charge ratio of ionized analytes received by detector component 22. An example cylindrical ion trap parameter value that influences the mass-to-charge ratio of ionized analytes received by detector component 22 is a mass-to-charge ratio range that can be specified as waveform values.
Housing 12 of instrument 10 can be configured to fully contain the vacuum system utilized by components 18, 20 and 22, as well as regions 34 and 35 and/or subregions 36 and 38. In accordance with an example configuration there are no external pumps or other components related to the vacuum system outside housing 12 of analytical instrument 10.
Referring to
Region 34 can be operatively coupled to a vacuum structure 46. Structure 46 can include an independent vacuum source, such as a drag pump 48. In the shown embodiment, structure 46 includes two vacuum sources serially aligned within structure 46, a drag pump 48 and a diaphragm pump 42. However, it is contemplated that specific implementations of interface region 34 can be maintained at adequate pressure with a single vacuum source. According to the depicted embodiment, drag pump 48 can be an Alcatel MDP5011 or TPD021 drag pump (obtained from Midwest Vacuum, Inc., 201 E. Ogden Avenue, Suite 15, Hinsdale, Ill. 60521, 630-323-5399 or US Headquarters, Pfeiffer Vacuum, 24 Trafalgar Square Nashua, N.H. 03063, 603-578-6500, respectively) and diaphragm pump 42 can be a KNF Neuberger N920 diaphragm pump (KNF NEUBERGER, INC., Two Black Forest Road, Trenton, N.J. 08691-1810 USA, 609-890-8600).
Subregion 36 can be operatively aligned between region 34 and subregion 38 within vacuum region 35. As an example, subregion 36 can define a vacuum structure 47 distinct from that of region 34 and/or subregion 38. Structure 47 can be coupled to at least a portion of vacuum structure 49 defined by subregion 38. Subegion 38 can define a vacuum structure 49 such as a housing coupled to turbo pump 44 which can be serially aligned with diaphragm pump 45. According to an example embodiment, structure 47 can be in fluid connection with structure 49 and thereby reliant on the vacuum sources of structure 49 such as pumps 44 and 45 which can be Pfeiffer TMH071-003 split flow turbo pump (US Headquarters, Pfeiffer Vacuum, 24 Trafalgar Square Nashua, N.H. 03063, 603-578-6500) and KNF Neuberger 813.4 diaphragm pumps, respectively.
The specific pumps referenced in relation to regions 34, 36 and 38 are but examples that can, according to some embodiments, facilitate housing instrument 10 within the defined space. Other pumps configured the same or differently may be utilized.
Referring to
Referring to
According to another example embodiment and referring to
Analytes prepared using components 16, 18, and/or 20 can be detected in detection component 22, for example. Exemplary detection components include electron multipliers, Faraday cup collectors, photographic, and scintillation-type detectors as described above.
Processing and control components 24 can be coupled to components 16, 18, 20, and/or 22, for example. All the components described above can be controlled, monitored, and/or have data acquired from by processing and control components 24. In exemplary embodiments, all, or at least more than one of, the components described above can be coupled to processing and control components 24.
Referring again to
According to one embodiment, the user interface can be coupled to structure 12 and provide user access to process circuitry. The user interface can take the form of a touch screen aligned with the exterior of structure 12 in exemplary embodiments, and the user interface can be within the volume defined by structure 12 Access to the user interface can be had through access panels, doors or openings in structure 12. In other embodiments, the user interface can be a computer interface that is configured to provide access to another process and control component, for example a stand alone computer. In exemplary embodiments, the computer interface can be a wireless interface and in other embodiments, the computer interface can take the form of a TCP/IP or a standard LAN connection. In exemplary embodiments, instrument 10 can be configured to accumulate and store sample data unattended. In other embodiments, instrument 10 can be configured to allow access to data and further provide for the manipulation of the data acquired. According to another embodiment, instrument 10 can be configured to send data to a remote computer upon acquisition.
In one embodiment, the progression of analysis from sample inlet component 16 to analysis component 22 can be controlled and/or monitored by the processing circuitry. The processing circuitry may be implemented as a processor or other structure configured to execute executable instructions including, for example, software and/or firmware instructions. Other exemplary embodiments of processing circuitry include hardware logic, PGA, FPGA, ASIC, and/or other structures. These examples of the processing circuitry are for illustration, and other configurations are possible.
The processing circuitry can be configured to control the values of analytical component parameters defined by the user of instrument 10 and/or monitor the components described above. Control of the analytical component parameter values by processing circuitry can include, for example, dictating a predefined application of ionization energy by modification component 20, such as components within regions 34, 36, and/or 38, for example. Exemplary monitoring includes the recording of data received from detector component 22. By varying analytical component parameter values, sample characteristics and/or data can be obtained. Exemplary sample characteristics and data can include mass spectra.
In one aspect, processing circuitry may execute data acquisition and searching programming and be configured to perform data acquisition and searching that includes the acquisition of sample characteristics such as total ion current or mass spectra. In another aspect, processing circuitry can be configured to associate detected sample characteristics such as total ion current responsive to one or more analytical parameters such as an ionization parameter including electron impact ion source energy.
The processing circuitry can be configured to store and access data from storage circuitry. The storage circuitry can be configured to store electronic data and/or programming such as executable instructions (e.g., software and/or firmware), data, or other digital information, and may include processor-usable media. Processor-usable media includes any article of manufacture which can contain, store or maintain programming, data and/or digital information for use by or in connection with an instruction execution system including processing circuitry, in the exemplary embodiment. For example, exemplary processor-usable media may include any one of physical media such as electronic, magnetic, optical, electromagnetic, and infrared or semiconductor media. Some more specific examples of processor-usable media include, but are not limited to, a portable magnetic computer diskette, such as a floppy diskette, zip disk, hard drive, random access memory, read only memory, flash memory, cache memory, and/or other configurations capable of storing programming, data, or other digital information. Embodiments also include configurations where processing and control components 24 can be configured to acquire sample data and analyze acquired data unattended. For example, sample inlet component 16 can be configured as an auto-sampler and, in exemplary embodiments, air samples can be acquired at predefined intervals as dictated by processing and control component 24. Processing and control component 24 can be configured according to predefined user parameters to acquire sample data. In other embodiments, processing and control component 24 can be configured to forward data and/or instrument status to remote locations via wireless and/or wired communication.
Referring to
In compliance with the statute, embodiments of the invention have been described in language more or less specific as to structural and methodical features. It is to be understood, however, that the entire invention is not limited to the specific features and/or embodiments shown and/or described, since the disclosed embodiments comprise forms of putting the invention into effect. The invention is, therefore, claimed in any of its forms or modifications within the proper scope of the appended claims appropriately interpreted in accordance with the doctrine of equivalents.
This application claims priority to U.S. provisional patent application 60/877,965 which was filed Dec. 29, 2006, entitled “Analytical Instruments, Assemblies, and Methods”, the entirety of which is incorporated by reference herein.
This invention was made with Government support under SBIR Phase-II Grant 0450512 awarded by the National Science Foundation. The Government has certain rights in the invention.
| Number | Name | Date | Kind |
|---|---|---|---|
| 4531056 | Labowsky et al. | Jul 1985 | A |
| 4542293 | Fenn et al. | Sep 1985 | A |
| 4804839 | Broadbent et al. | Feb 1989 | A |
| 4948962 | Mitsui et al. | Aug 1990 | A |
| 4977320 | Chowdhury et al. | Dec 1990 | A |
| 4999493 | Allen et al. | Mar 1991 | A |
| 5155357 | Hemond | Oct 1992 | A |
| 5157260 | Mylchreest et al. | Oct 1992 | A |
| 5245186 | Chait et al. | Sep 1993 | A |
| 5313061 | Drew et al. | May 1994 | A |
| 5525799 | Andresen et al. | Jun 1996 | A |
| 5539204 | Coutts et al. | Jul 1996 | A |
| 5672868 | Mordehai et al. | Sep 1997 | A |
| 5728584 | Sausa et al. | Mar 1998 | A |
| 5744798 | Kato | Apr 1998 | A |
| 5818041 | Mordehai et al. | Oct 1998 | A |
| 5852295 | Da Silveira et al. | Dec 1998 | A |
| 6093929 | Javahery et al. | Jul 2000 | A |
| 6107627 | Nakagawa et al. | Aug 2000 | A |
| 6265717 | Sakata et al. | Jul 2001 | B1 |
| 6351983 | Haas et al. | Mar 2002 | B1 |
| 6462336 | Bajic | Oct 2002 | B1 |
| 6627877 | Davis et al. | Sep 2003 | B1 |
| 6646257 | Fischer et al. | Nov 2003 | B1 |
| 6683300 | Doroshenko et al. | Jan 2004 | B2 |
| 6744045 | Fries et al. | Jun 2004 | B2 |
| 6797947 | Russ et al. | Sep 2004 | B2 |
| 6800848 | Shiokawa et al. | Oct 2004 | B2 |
| 6809312 | Park et al. | Oct 2004 | B1 |
| 6841773 | McLoughlin et al. | Jan 2005 | B2 |
| 6924478 | Zubarev et al. | Aug 2005 | B1 |
| 6949741 | Cody et al. | Sep 2005 | B2 |
| 7015466 | Takats et al. | Mar 2006 | B2 |
| 7091477 | Jolliffe et al. | Aug 2006 | B2 |
| 7402799 | Freidhoff | Jul 2008 | B2 |
| 20010048074 | Shiokawa et al. | Dec 2001 | A1 |
| 20020036263 | Shiokawa et al. | Mar 2002 | A1 |
| 20020079442 | Fries et al. | Jun 2002 | A1 |
| 20030020011 | Anderson et al. | Jan 2003 | A1 |
| 20030141449 | Wells et al. | Jul 2003 | A1 |
| 20040222372 | McLoughlin et al. | Nov 2004 | A1 |
| 20050035287 | Jolliffe et al. | Feb 2005 | A1 |
| 20050173627 | Cotter et al. | Aug 2005 | A1 |
| 20050230635 | Takats et al. | Oct 2005 | A1 |
| 20050258364 | Whitehouse et al. | Nov 2005 | A1 |
| 20060068081 | Izawa et al. | Mar 2006 | A1 |
| 20060079002 | Gologan et al. | Apr 2006 | A1 |
| 20070114392 | Mukaibatake | May 2007 | A1 |
| 20080138219 | Stones et al. | Jun 2008 | A1 |
| 20080166219 | Stuart et al. | Jul 2008 | A1 |
| Number | Date | Country | |
|---|---|---|---|
| 60877965 | Dec 2006 | US |
