ライフサイエンスコーパス: drift time

1 or segments of the 2D mobiligram (m/z versus drift time).

2 th- and mobility-dependent variations in ion drift time.

3 orrelated to fwhm) becomes a function of the drift time.

4 precursor fragmentation with their mobility drift time.

5 ution which results in a modification of IMS drift time.

6 d in the acyl chain causes a 5% reduction in drift time.

7 ysis by differences of up to 30% in mobility drift time.

8 400 micros) followed by a comparatively long drift time (25-100 ms), which translates into a loss of

9 imensions: high-resolution LC separation, IM drift time, accurate mass precursor, and fragment ion me

10 es, which can be further characterized using drift-time alignment of product and precursor ions disti

11 Such short drift times allow for a significantly increased repetiti

12 LWC was used to compress the IMS data in the drift time and data acquisition dimensions on IMS data o

13 argue that the incorporation of ion mobility drift time and product ion information are worthy pursui

14 We also show that the inclusion of drift time and product ion information results in higher

15 ntation spectra, exhibit very distinctive IM drift times and collision cross sections (CCS).

16 Comparison of both the fragment drift times and IR spectra with those of suitable refere

17 r nitrogen has a dramatic effect on measured drift times and must not be ignored when comparing and i

18 nomers and fragment ions with characteristic drift times and peak intensities, associated with ion ma

19 pects of the data, particularly ion mobility drift times and product ion information.

20 To further reduce drift times and thus increase the repetition rate, heliu

21 o fragment 50% of a selected precursor ion), drift time, and collision induced dissociation (CID) spe

22 ith mass to charge ratio (m/z), ion mobility drift time, and intensity information for each individua

23 from low to high while monitoring a specific drift time, and the resulting data were processed to cre

24 nderstand potential deviations from expected drift time behaviors.

25 ced mobility of just 0.94 cm(2)/(V s) have a drift time below 1.6 ms.

26 Ions with a drift time between 9 and 18 ms in the first drift region

27 base of 8675 peptide sequences with measured drift times, both techniques statistically significantly

28 onosaccharide regioisomers which differed in drift time by only 0.8%.

29 These instruments often rely on drift-time calibrants to perform qualitative identificat

30 sors and overlapping in m/z but separated in drift time can be examined individually.

31 erest is based on the fact that the measured drift times can be converted into collision cross sectio

32 ative parameters including m/z distribution, drift time, carbon number range, and associated double b

33 periments showed a dramatic shift to shorter drift times caused by conformational changes upon metal

34 es are here shown to be highly reproducible (drift time coefficients of variation < 1.0% and isotopic

35 From experimentally measured drift times, collision cross-sections can be deduced.

36 downward saccades with the PE in abduction, drift time constants averaged 35 ms; (3) peak dynamic bl

37 Interestingly, drift time data enabled the recognition of multiply char

38 In contrast, considerable differences in drift times detected were found with increasing humidity

39 his paper introduces a strategy for accurate drift time determination using traveling wave ion mobili

40 f peptides to accurately predict a peptide's drift time directly from its amino acid sequence.

41 Extracted ion drift time distributions (XIDTDs) of deuterated peptic p

42 al isotopic composition and nearly identical drift time distributions, these isomers could not be dis

43 Ion mobility drift times, flight times, relative signal intensities,

44 ure to convert measured physical quantities (drift time for TWIMS and elution voltage for TIMS) into

45 Specific combinations of drift times for fragments and precursor ions provide add

46 accharides, which provided us with reference drift times for fragments of known conformation.

47 Plots of drift times for pairs of protonated monomer and fragment

48 T-wave drift-times for the protonated diastereomers betamethaso

49 Drift times from TWIMS were calibrated to CCSs using eit

50 ave incorporated ion mobility and subsequent drift time gating into the UVPD method allowing the sepa

51 precisely preserves the peak location (i.e., drift time), height, and shape.

52 Existing drift time IMS cells utilize a static voltage typically

53 pproach to increase the resolving power of a drift time IMS without employing higher drift voltages a

54 lude m/z value, drift time in He buffer gas, drift time in He and D2O buffer gases, deuterium incorpo

55 ique information for ions include m/z value, drift time in He buffer gas, drift time in He and D2O bu

56 ly derived relationship between mobility and drift time in TWIMS stacked ring ion guide (SRIG) and co

57 imilar mass-to-charge ratios with dissimilar drift times in complex biological samples removes some s

58 uctural isomers exhibited different mobility drift times in either system, depending on differences i

59 structural isomers have remarkably different drift times in ion mobility separation, corresponding to

60 ndent acquisition (DDA) by considering their drift times in traveling wave ion mobility spectrometry

61 separation (based on the retention time and drift time information) and identification of an analyte

62 of the separation while preserving retention/drift time information.

63 The possibility of false positives by drift time interferences and false negatives by competit

64 has been studied using mass spectrometry and drift time ion mobility mass spectrometry (DT IM-MS) in

65 e mass spectrometry and variable-temperature drift time ion mobility mass spectrometry (VT-DT-IM-MS).

66 ycotoxins were considered and analyzed using drift time ion mobility mass spectrometry.

67 If an optimal drift time is calculated for each voltage and scanned si

68 The drift time is reduced at a rate of approximately 1% for

69 Corresponding ions, masses, drift times, K(o) values, and arbitrary signal intensiti

70 our previously reported observation that the drift time-m/z relationship for singly charged phosphory

71 ding to appropriate rules that depend on the drift times measured by ion mobility spectrometry for re

72 "wrap-around" can be mitigated by comparing drift times measured during single- and multipass experi

73 or 113 peptide ions determined directly from drift times measured in a low-pressure, ambient temperat

74 e ions and the errors concomitant with using drift times measured in N(2) gas to estimate Omega(He).

75 ently cannot be determined directly from the drift times measured.

76 Overall analysis times and drift time measurement precision were found to be unaffe

77 ce of numerous isomers could be ruled out by drift time measurements and molecular modeling together

78 This has implications for drift time measurements, made on traveling wave ion mobi

79 f the IMS system, while maintaining accurate drift time measurements.

80 RI, ECOM(50), and drift-time models are used for filtering compounds downl

81 field created by a large peak influences the drift time of a neighboring small peak.

82 re, we analyze the effect of nitrogen on the drift time of a series of cationic 1,10-phenanthroline c

83 ak full width at half-maximum (fwhm) and the drift time of model compounds for wide range of settings

84 arkers by LAESI can be enhanced by using the drift times of individual ions as an additional paramete

85 In general, drift time patterns (relative drift times of isomers) matched between the two instrume

86 of cross sections, mobilities and associated drift times of peptides, thereby enhancing downstream da

87 The impact of water vapor on the drift times of small ions at different temperatures was

88 rization of the attached glycan based on the drift times of the monosaccharide product ions generated

89 such as resolution, theoretical plates, and drift times of the parabens were also evaluated based on

90 By compressing both the drift time order and the spectrum acquisition order, gre

91 In general, drift time patterns (relative drift times of isomers) ma

92 o IMMS data, which allows one to compare m/z-drift time plots to highlight differences between sample

93 Charge state distributions, drift time profiles, and collision cross sections were d

94 negative ion mobility spectrum, each with a drift time range of 13 ms (minimum reduced ion mobility

95 s-phase IR spectra of simultaneously m/z and drift-time-resolved species of benzocaine.

96 successfully separated and identified using drift time separation.

97 ture property relationship-based modeling of drift times showed a better correlation with experimenta

98 some caution when calibrating sample protein drift times simply with single numeric CCS values.

99 Experimental research consisted of recording drift time spectra for 2-pentanone and n-heptanone, at v

100 beam, it is possible to successfully obtain drift time spectra for an assortment of simple peptide a

101 orm ion mobility mass spectrometry (FT-IMMS) drift time spectra, we demonstrate significant time savi

102 r the lack of ion charge conservation in the drift time spectrum are ion recombination, mutual repuls

103 A single peak in the drift time spectrum is usually generated by a mixture of

104 s contained in the area of peaks forming the drift time spectrum.

105 r correlation with experimentally determined drift times than did Mobcal cross-sectional areas.

106 by filtering the chromatogram to retain the drift time that corresponds to the unique gas-phase conf

107 s that are formed in the collision cell have drift times that are coincident with their antecedent pa

108 CS and HS disaccharide isomers have similar drift times, they can be uniquely distinguished by their

109 h the theoretical optimum potential at every drift time, this work solves the General Elution Problem

110 a frequency that is resonant with the ion's drift time through each region.

111 ge state are separated based on their unique drift times through the TWIM region.

112 to travel multiple passes, increasing their drift times to the detector and relative separation.

113 DI-ESI-TWIM-MS was able, via distinct drift times, to set apart different classes of metabolit

114 sing TWIMS in N2 drift gas, and the observed drift time trends compared.

115 eters: The apex of the peak (A) and the mean drift time value (mu).

116 Drift time values of low charged multiply protonated mol

117 ar dynamics simulation predicted theoretical drift time values, which were in good agreement with exp

118 arge state, LC elution time and ion mobility drift time values.

119 oach is limited by observed variation in ion drift time/velocity in these measurements.

120 Comparative analysis of drift time versus mass-to-charge ratio plots was perform

121 Slope for plots of ion abundance against drift time was fitted by successive approximation betwee

122 Drift times were correlated with collisional cross secti

123 Short drift times while maintaining high resolving power are r

124 Calibration of these drift-times yields T-wave Omega(N(2)) values of 189.4 an