The Charge-State and Structural Stability of Peptides Conferred by Microsolvating Environments in Differential Mobility Spectrometry

Christian Ieritano; Daniel Rickert; Joshua Featherstone; John F Honek; J Larry Campbell; J C Yves Le Blanc; Bradley B Schneider; W Scott Hopkins

doi:10.1021/jasms.0c00469

The Charge-State and Structural Stability of Peptides Conferred by Microsolvating Environments in Differential Mobility Spectrometry

J Am Soc Mass Spectrom. 2021 Apr 7;32(4):956-968. doi: 10.1021/jasms.0c00469. Epub 2021 Mar 18.

Authors

Christian Ieritano¹, Daniel Rickert¹, Joshua Featherstone¹, John F Honek¹, J Larry Campbell^{1

2

3}, J C Yves Le Blanc⁴, Bradley B Schneider⁴, W Scott Hopkins^{1

2

5

6}

Affiliations

¹ Department of Chemistry, University of Waterloo, 200 University Avenue West, Waterloo N2L 3G1, Ontario, Canada.
² Watermine Innovation, Waterloo N0B 2T0, Ontario, Canada.
³ Bedrock Scientific, Milton L6T 6J9, Ontario, Canada.
⁴ SCIEX, 71 Four Valley Drive, Concord L4K 4 V8, Ontario, Canada.
⁵ Waterloo Institute for Nanotechnology, University of Waterloo, 200 University Avenue West, Waterloo N2L 3G1, Ontario, Canada.
⁶ Centre for Eye and Vision Research, Hong Kong Science Park, New Territories 999077, Hong Kong.

PMID: 33733774
DOI: 10.1021/jasms.0c00469

Abstract

The presence of solvent vapor in a differential mobility spectrometry (DMS) cell creates a microsolvating environment that can mitigate complications associated with field-induced heating. In the case of peptides, the microsolvation of protonation sites results in a stabilization of charge density through localized solvent clustering, sheltering the ion from collisional activation. Seeding the DMS carrier gas (N₂) with a solvent vapor prevented nearly all field-induced fragmentation of the protonated peptides GGG, AAA, and the Lys-rich Polybia-MP1 (IDWKKLLDAAKQIL-NH₂). Modeling the microsolvation propensity of protonated n-propylamine [PrNH₃]⁺, a mimic of the Lys side chain and N-terminus, with common gas-phase modifiers (H₂O, MeOH, EtOH, iPrOH, acetone, and MeCN) confirms that all solvent molecules form stable clusters at the site of protonation. Moreover, modeling populations of microsolvated clusters indicates that species containing protonated amine moieties exist as microsolvated species with one to six solvent ligands at all effective ion temperatures (T_eff) accessible during a DMS experiment (ca. 375-600 K). Calculated T_eff of protonated GGG, AAA, and Polybia-MPI using a modified two-temperature theory approach were up to 86 K cooler in DMS environments seeded with solvent vapor compared to pure N₂ environments. Stabilizing effects were largely driven by an increase in the ion's apparent collision cross section and by evaporative cooling processes induced by the dynamic evaporation/condensation cycles incurred in the presence of an oscillating electric separation field. When the microsolvating partner was a protic solvent, abstraction of a proton from [MP1 + 3H]³⁺ to yield [MP1 + 2H]²⁺ was observed. This result was attributed to the proclivity of protic solvents to form hydrogen-bond networks with enhanced gas-phase basicity. Collectively, microsolvation provides analytes with a solvent "air bag," whereby charge reduction and microsolvation-induced stabilization were shown to shelter peptides from the fragmentation induced by field heating and may play a role in preserving native-like ion configurations.

Keywords: charge transfer; clustering; differential mobility spectrometry; ion mobility; ion−solvent interaction; microsolvation.

MeSH terms

Amino Acid Sequence
Ion Mobility Spectrometry / methods*
Ions
Molecular Dynamics Simulation
Peptides / chemistry*
Solutions
Solvents / chemistry
Static Electricity
Temperature

Substances

Ions
Peptides
Solutions
Solvents