Bioengineering (Mar 2023)

Proteomic Profiling of Fallopian Tube-Derived Extracellular Vesicles Using a Microfluidic Tissue-on-Chip System

  • Didi Zha,
  • Sagar Rayamajhi,
  • Jared Sipes,
  • Angela Russo,
  • Harsh B. Pathak,
  • Kailiang Li,
  • Mihaela E. Sardiu,
  • Leonidas E. Bantis,
  • Amrita Mitra,
  • Rajni V. Puri,
  • Camille V. Trinidad,
  • Brian P. Cain,
  • Brett C. Isenberg,
  • Jonathan Coppeta,
  • Shannon MacLaughlan,
  • Andrew K. Godwin,
  • Joanna E. Burdette

DOI
https://doi.org/10.3390/bioengineering10040423
Journal volume & issue
Vol. 10, no. 4
p. 423

Abstract

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The human fallopian tube epithelium (hFTE) is the site of fertilization, early embryo development, and the origin of most high-grade serous ovarian cancers (HGSOCs). Little is known about the content and functions of hFTE-derived small extracellular vesicles (sEVs) due to the limitations of biomaterials and proper culture methods. We have established a microfluidic platform to culture hFTE for EV collection with adequate yield for mass spectrometry-based proteomic profiling, and reported 295 common hFTE sEV proteins for the first time. These proteins are associated with exocytosis, neutrophil degranulation, and wound healing, and some are crucial for fertilization processes. In addition, by correlating sEV protein profiles with hFTE tissue transcripts characterized using GeoMx® Cancer Transcriptome Atlas, spatial transcriptomics analysis revealed cell-type-specific transcripts of hFTE that encode sEVs proteins, among which, FLNA, TUBB, JUP, and FLNC were differentially expressed in secretory cells, the precursor cells for HGSOC. Our study provides insights into the establishment of the baseline proteomic profile of sEVs derived from hFTE tissue, and its correlation with hFTE lineage-specific transcripts, which can be used to evaluate whether the fallopian tube shifts its sEV cargo during ovarian cancer carcinogenesis and the role of sEV proteins in fallopian tube reproductive functions.

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