Instrumentation development, improvement, simplification, and miniaturization: The multifunctional plate source for use in mass spectrometry

Author:

Trimpin Sarah12ORCID,Inutan Ellen3,Coffinberger Hope24,Hoang Khoa24,Yenchick Frank1,Wager-Miller James5,Pophristic Milan24,Mackie Ken5ORCID,McEwen Charles N.24

Affiliation:

1. Wayne State University, Detroit, MI, USA

2. Research and Development, MSTM, LLC, Philadelphia, PA, USA

3. Department of Chemistry, Mindanao State University-Illigan Institute of Technology, Illigan City, Philippines

4. Department of Chemistry & Biochemistry, Saint Joseph's University, Philadelphia, PA, USA

5. Psychological and Brain Sciences Campus, Indiana University, Bloomington, IN, USA

Abstract

In remembrance of Prof. Dr Przybylski, we are presenting a vision towards his beloved mass spectrometry (MS) and its far-reaching promises outside of the academic laboratory. Sub-atmospheric pressure (AP) ionization MS is well positioned to make a step-change in direct ionization, a concept that allows sublimation/evaporation ionization and mass analyses of volatile and nonvolatile molecules from clean or dirty samples, directly, accurately, sensitively, and in a straightforward manner that has the potential to expand the field of MS into unchartered application areas. Contrary to ambient ionization MS, ionization commences in the sub-AP region of the mass spectrometer, important for practical and safety reasons, and offers inter alia, simplicity, speed, sensitivity, and robustness directly from real-world samples without cleanup. The plate source concept, presented here, provides an easy to use, rapid, and direct sample introduction from AP into the sub-AP of a mass spectrometer. Utilizing sub-AP ionization MS based on the plate source concept, small to large molecules from various environments that would be deemed too dirty for some direct MS methods are demonstrated. The new source concept can be expanded to include multiple ionization methods using the same plate source “front end” without the need to vent the mass spectrometer between the different methods, thus allowing ionization of more compounds on the same mass spectrometer for which any one ionization method may be insufficient. Examples such as fentanyl, gamma-hydroxybutyric acid, clozapine, 1-propionyllysergic acid, hydrocodone angiotensin I and II, myoglobin, and carbonic anhydrase are included.

Funder

National Institutes of Health

National Science Foundation

Publisher

SAGE Publications

Subject

Spectroscopy,Atomic and Molecular Physics, and Optics,General Medicine

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