4.6 Article

Transcriptome analysis of cervical cancer exosomes and detection of HPVE6*I transcripts in exosomal RNA

Journal

BMC CANCER
Volume 22, Issue 1, Pages -

Publisher

BMC
DOI: 10.1186/s12885-022-09262-4

Keywords

Cervical cancer; Exosome; Human papillomavirus; Next generation sequencing; Transcript profiling; Reverse transcriptase polymerase chain reaction; Oncoprotein E6

Categories

Funding

  1. Science and Engineering Research Board Department of Science and Technology, Government of India (DST-SERB) [EMR/2017/004018/BBM]
  2. ICMR [5/13/38/2014-NCD-III, 2017-2834/CMB/BMS]
  3. Senior Research Fellowship [09/045(1629)/2019-EMR-I, 09/045(1622)/2019-EMR-I]
  4. Council of Scientific and Industrial Research (CSIR)
  5. Department of Science and Technology, India [EMR/2017/004018/BBM]
  6. University Grants Commission (UGC) [2061430699 22/06/2014(i) EU-V, 573(CSIR-UGC NET JUNE 2017)]
  7. Indian Council of Medical Research [5/13/38/2014 NCDIII-Eoffice73143, 3/2/2/278/2014-NCDIII]

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The study found diverse transcripts in exosomes from cervical cancer cells, some of which are related to Hh signaling pathways and tumor innervation. Additionally, the E6*I splice variant is a potential exosomal biomarker.
Background Exosomes play a key role in cell-to-cell communication and are integral component of the tumor microenvironment. Recent observations suggest transfer of RNA through tumor-derived exosomes that can potentially translate into regulatory proteins in the recipient cells. Role of cervical cancer-derived exosomes and their transcript cargo is poorly understood. Materials and methods The total RNA of exosomes from HPV-positive (SiHa and HeLa) and HPV-negative (C33a) cervical cancer cell lines were extracted and the transcripts were estimated using Illumina HiSeq X. Further, validation of HPV transcripts were performed using RT-PCR. Results 3099 transcripts were found to be differentially-exported in HPV-positive vs. HPV-negative exosomes (p value <0.05). Analysis of top 10 GO terms and KEGG pathways showed enrichment of transcripts belonging to axon guidance and tumor innervation in HPV-positive exosomes. Among top 20 overexpressed transcripts, EVC2, LUZP1 and ANKS1B were the most notable due to their involvement in Hh signaling, cellular migration and invasion, respectively. Further, low levels of HPV-specific reads were detected. RT-PCR validation revealed presence of E6*I splice variant of HPV18 in exosomal RNA of HeLa cells. The E6*I transcripts were consistently retained in exosomes obtained from HeLa cells undergoing 5-FU and cisplatin-induced oxidative stress. Conclusion Our data suggests the enrichment of poly-A RNA transcripts in the exosomal cargo of cervical cancer cells, which includes pro-tumorigenic cellular RNA and viral transcripts such as HPV E6, which may have clinical utility as potential exosomal biomarkers of cervical cancer.

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