Literature DB >> 19835365

MALDI mass spectrometric imaging using the stretched sample method to reveal neuropeptide distributions in aplysia nervous tissue.

Tyler A Zimmerman1, Stanislav S Rubakhin, Elena V Romanova, Kevin R Tucker, Jonathan V Sweedler.   

Abstract

Neuropeptides are a diverse set of complex cell-cell signaling molecules that modulate behavior, learning, and memory. Their spatially heterogeneous distributions, large number of post-translational modifications, and wide range of physiologically active concentrations make their characterization challenging. Matrix-assisted laser desorption/ionization (MALDI) mass spectrometric imaging is well-suited to characterizing and mapping neuropeptides in the central nervous system. Because matrix application can cause peptide migration within tissue samples, application parameters for MALDI typically represent a compromise between attaining the highest signal quality and preserving native spatial distributions. The stretched sample approach minimizes this trade-off by fragmenting the tissue section into thousands of spatially isolated islands, each approximately 40 mum in size. This inhibits analyte migration between the pieces and, at the same time, reduces analyte-salt adduct formation. Here, we present methodological improvements that enable the imaging of stretched tissues and reveal neuropeptide distributions in nervous tissue from Aplysia californica. The distributions of known neuropeptides are shown to correspond with previous immunohistochemical results, demonstrating that the stretched imaging method is well-suited for working with easily redistributed molecules and heterogeneous tissues and reduces adducts from physiological salts.

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Year:  2009        PMID: 19835365      PMCID: PMC2837479          DOI: 10.1021/ac901820v

Source DB:  PubMed          Journal:  Anal Chem        ISSN: 0003-2700            Impact factor:   6.986


  50 in total

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4.  Automated acoustic matrix deposition for MALDI sample preparation.

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5.  Autonomic control network active in Aplysia during locomotion includes neurons that express splice variants of R15-neuropeptides.

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6.  Massively parallel sample preparation for the MALDI MS analyses of tissues.

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  18 in total

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Review 2.  Small-volume analysis of cell-cell signaling molecules in the brain.

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3.  Stretched tissue mounting for MALDI mass spectrometry imaging.

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4.  Genetically Encoded Fluorescent Proteins Enable High-Throughput Assignment of Cell Cohorts Directly from MALDI-MS Images.

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Review 6.  Challenges and recent advances in mass spectrometric imaging of neurotransmitters.

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7.  Neuropeptidomics: mass spectrometry-based qualitative and quantitative analysis.

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8.  Comparison of NIMS and MALDI platforms for neuropeptide and lipid mass spectrometric imaging in C. borealis brain tissue.

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9.  The modified-bead stretched sample method: development and application to MALDI-MS imaging of protein localization in the spinal cord.

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Review 10.  Neuropeptidomics: Improvements in Mass Spectrometry Imaging Analysis and Recent Advancements.

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