Alan G. Marshall

FOURIER TRANSFORM ION CYCLOTRON RESONANCE MASS SPECTROMETRY: A PRIMER

This review offers an introduction to the principles and generic applications of FT-ICR mass spectrometry, directed to readers with no prior experience with the technique. We are able to explain the fundamental FT-ICR phenomena from a simplified theoretical treatment of ion behavior in idealized magnetic and electric fields. The effects of trapping voltage, trap size and shape, and other nonidealities are manifested mainly as perturbations that preserve the idealized ion behavior modified by appropriate numerical correction factors. Topics include: effect of ion mass, charge, magnetic field, and trapping voltage on ion cyclotron frequency; excitation and detection of ICR signals; mass calibration; mass resolving power and mass accuracy; upper mass limit(s); dynamic range; detection limit, strategies for mass and energy selection for MSn; ion axialization, cooling, and remeasurement; and means for guiding externally formed ions into the ion trap. The relation of FT-ICR MS to other types of Fourier transform spectroscopy and to the Paul (quadrupole) ion trap is described. The article concludes with selected applications, an appendix listing accurate fundamental constants needed for ultrahigh-precision analysis, and an annotated list of selected reviews and primary source publications that describe in further detail various FT-ICR MS techniques and applications.

Fourier Transform Ion Cyclotron Resonance Spectroscopy

In recent years several spectroscopic techniques have been revolutionized by the introduction of Fourier multiplex methods. The principal advantage of the Fourier method is that the whole spectrum may be obtained in a very short period of time, namely the amount of time which a conventional spectrometer would require to observe just a single point in the spectrum. The most important applications of Fourier methods have been to nuclear magnetic resonance spectroscopy and to infra-red spectroscopy, but the methods have also been found useful in optical spectroscopy, microwave spectroscopy and even electrochemistry. The advantages of the Fourier method would clearly be desirable in the field of mass spectrometry and in principle can be realized by the development of the Fourier transform ion cyclotron resonance (FT-ICR)1–5 mass spectrometer.

A universal algorithm for fast and automated charge state deconvolution of electrospray mass-to-charge ratio spectra

This article describes a new algorithm for charge state determination and deconvolution of electrospray ionization (ESI) mass-to-charge ratio spectra. The algorithm (Zscore) is based on a charge scoring scheme that incorporates all above-threshold members of a family of charge states or isotopic components, and deconvolves both low- and high-resolution mass-to-charge ratio spectra, with or without a peak list (stick plot). A scoring weight factor, log (I/I0), in which I is the signal magnitude at a calculated mass-to-charge ratio, and I0 is the signal threshold near that mass-to-charge ratio, was used in most cases. For high-resolution mass-to-charge ratio spectra in which all isotopic peaks are resolved, the algorithm can deconvolve overlapped isotopic multiplets of the same or different charge state. Compared to other deconvolution techniques, the algorithm is robust, rapid, and fully automated (i. e., no user input during the deconvolution process). It eliminates artifact peaks without introducing peak distortions. Its performance is demonstrated for experimental ESI Fourier transform ion cyclotron resonance mass-to-charge ratio spectra (both low and high resolution). Charge state deconvolution to yield a “zero-charge” mass spectrum should prove particularly useful for interpreting spectra of complex mixtures, identifying contaminants, noncovalent adducts, fragments (N-terminal, C-terminal, internal), and chemical modifications of electrosprayed biomacromolecules.

Asphaltenes, Heavy Oils, and Petroleomics

The first € price and the £ and

External Accumulation of Ions for Enhanced Electrospray Ionization Fourier Transform Ion Cyclotron Resonance Mass Spectrometry

price are net prices, subject to local VAT. Prices indicated with * include VAT for books; the €(D) includes 7% for Germany, the €(A) includes 10% for Austria. Prices indicated with ** include VAT for electronic products; 19% for Germany, 20% for Austria. All prices exclusive of carriage charges. Prices and other details are subject to change without notice. All errors and omissions excepted. O.C. Mullins, E.Y. Sheu, A. Hammami, A.G. Marshall Asphaltenes, Heavy Oils, and Petroleomics

Frequency-sweep fourier transform ion cyclotron resonance spectroscopy

Electrospray ionization (ESI) in combination with Fourier transform ion cyclotron resonance (FTICR) mass spectrometry provides for mass analysis of biological molecules with unrivaled mass accuracy, resolving power and sensitivity. However, ESI FTICR MS performance with on-line separation techniques such as liquid chromatography (LC) and capillary electrophoresis has to date been limited primarily by pulsed gas assisted accumulation and the incompatibility of the associated pump-down time with the frequent ion beam sampling requirement of on-line chromatographic separation. Here we describe numerous analytical advantages that accrue by trapping ions at high pressure in the first rf-only octupole of a dual octupole ion injection system before ion transfer to the ion trap in the center of the magnet for high performance mass analysis at low pressure. The new configuration improves the duty cycle for analysis of continuously generated ions, and is thus ideally suited for on-line chromatographic applications. LC/ESI FTICR MS is demonstrated on a mixture of 500 fmol of each of three peptides. Additional improvements include a fivefold increase in signal-to-noise ratio and resolving power compared to prior methods on our instrument.

Petroleomics: Chemistry of the underworld

Abstract A single ion cyclotron resonance (ICR) absorption spectrum showing both CH + 3 and CH + 4 signals has been obtained by exciting both ion cyclotron resonances with a frequency-swept rf irradiation, followed by broad-band detection, digitization of the (time-domain) response, and finally discrete Fourier transformation to produce the (frequency-domain) spectrum. Pulsed-excitation Fourier transform ICR has demonstrated the use of broad-band detection in rapid generation of ICR spectra by Fourier transform methods; this paper demonstrates that frequency-sweep excitation can provide the broad-band irradiation required to excite ion cyclotron resonances throughout any desired mass range. It will thus be possible to obtain an ICR absorption spectrum of given mass range, signal-to-noise ratio, and resolution in an observation period which is two orders of magnitude shorter than that needed to obtain the same spectrum by conventional slow-sweep detection.

Milestones in fourier transform ion cyclotron resonance mass spectrometry technique development

Each different molecular elemental composition—e.g., CcHhNnOoSs—has a different exact mass. With sufficiently high mass resolving power (m/Δm50% ≈ 400,000, in which m is molecular mass and Δm50% is the mass spectral peak width at half-maximum peak height) and mass accuracy (<300 ppb) up to ≈800 Da, now routinely available from high-field (≥9.4 T) Fourier transform ion cyclotron resonance mass spectrometry, it is possible to resolve and identify uniquely and simultaneously each of the thousands of elemental compositions from the most complex natural organic mixtures, including petroleum crude oil. It is thus possible to separate and sort petroleum components according to their heteroatom class (NnOoSs), double bond equivalents (DBE = number of rings plus double bonds involving carbon, because each ring or double bond results in a loss of two hydrogen atoms), and carbon number. “Petroleomics” is the characterization of petroleum at the molecular level. From sufficiently complete characterization of the organic composition of petroleum and its products, it should be possible to correlate (and ultimately predict) their properties and behavior. Examples include molecular mass distribution, distillation profile, characterization of specific fractions without prior extraction or wet chemical separation from the original bulk material, biodegradation, maturity, water solubility (and oil:water emulsion behavior), deposits in oil wells and refineries, efficiency and specificity of catalytic hydroprocessing, “heavy ends” (asphaltenes) analysis, corrosion, etc.

KIT kinase mutants show unique mechanisms of drug resistance to imatinib and sunitinib in gastrointestinal stromal tumor patients.

Abstract The present range and power of Fourier transform ion cyclotron resonance mass spectrometry rest on a number of prior technique developments. In this article, selected developments in neutral/ion introduction, ionization methods, excitation/detection, ion trap configuration/operating modes, ion dissociation and MS/MS, ion cooling techniques, theory and data reduction are briefly explained and chronicled. Evidence for the value of these techniques is provided by a compilation of current world records for mass resolution, mass resolving power and mass accuracy. With these capabilities, it becomes possible to resolve and identify up to thousands of components of a complex mixture, often without prior wet chemical separation, thereby potentially changing the whole approach to dealing with chemical and biological complexity.

A High‐performance Modular Data System for Fourier Transform Ion Cyclotron Resonance Mass Spectrometry

Most gastrointestinal stromal tumors (GISTs) exhibit aberrant activation of the receptor tyrosine kinase (RTK) KIT. The efficacy of the inhibitors imatinib mesylate and sunitinib malate in GIST patients has been linked to their inhibition of these mutant KIT proteins. However, patients on imatinib can acquire secondary KIT mutations that render the protein insensitive to the inhibitor. Sunitinib has shown efficacy against certain imatinib-resistant mutants, although a subset that resides in the activation loop, including D816H/V, remains resistant. Biochemical and structural studies were undertaken to determine the molecular basis of sunitinib resistance. Our results show that sunitinib targets the autoinhibited conformation of WT KIT and that the D816H mutant undergoes a shift in conformational equilibrium toward the active state. These findings provide a structural and enzymologic explanation for the resistance profile observed with the KIT inhibitors. Prospectively, they have implications for understanding oncogenic kinase mutants and for circumventing drug resistance.