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      Targeting of stromal versican by miR-144/199 inhibits multiple myeloma by downregulating FAK/STAT3 signalling

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          ABSTRACT

          The abnormal growth of malignant plasma cells in Multiple Myeloma (MM) requires bone marrow (BM) niche consisting of proteoglycans, cytokines, etc. Versican (VCAN), a chondroitin sulphate proteoglycan promotes progression in solid tumours but there is dearth of literature in MM. Hence, we studied the involvement of VCAN in MM and its regulation by microRNAs as a therapeutic approach. Thirty MM patients and 20 controls were recruited and BM stromal cells (BMSCs) were isolated by primary culture. Molecular levels of VCAN, miR-144, miR-199 & miR-203 were determined in study subjects and cell lines. The involvement of VCAN in myeloma pathogenesis was studied using BMSCs-conditioned medium (BMSCs-CM) and VCAN-neutralizing antibody or microRNA mimics. Elevated expression of VCAN was observed in patients especially in BM stroma while microRNA expression was significantly lower and showed negative correlation with VCAN. Moreover, BMSCs-CM showed the presence of VCAN which upon supplementing to MM cells alter parameters in favour of myeloma progression, however, this effect was neutralized by VCAN antibody or miR (miR-144 and miR-199) mimics. The downstream signalling of VCAN was found to activate FAK and STAT3 which subsides by using VCAN antibody or miR mimics. The neutralization of oncogenic effect of BMSCs-CM by VCAN blockage affirms its plausible role in progression of MM. VCAN was observed as a paracrine mediator in the cross-talk of BMSCs and myeloma cells in BM microenvironment. Therefore, these findings suggest exploring VCAN as novel therapeutic target and utilization of microRNAs as a therapy to regulate VCAN for better management of MM.

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          Author and article information

          Journal
          RNA Biol
          RNA Biol
          KRNB
          krnb20
          RNA Biology
          Taylor & Francis
          1547-6286
          1555-8584
          2020
          29 September 2019
          : 17
          : 1
          : 98-111
          Affiliations
          [a ] Department of Biochemistry, All India Institute of Medical Sciences (AIIMS) , New Delhi, India
          [b ] Department of Hematology, All India Institute of Medical Sciences (AIIMS) , New Delhi, India
          [c ] Department of Orthopedics, All India Institute of Medical Sciences (AIIMS) , New Delhi, India
          Author notes
          CONTACT Alpana Sharma dralpanasharma@ 123456gmail.com Department of Biochemistry, All India Institute of Medical Sciences , New Delhi 110029, India
          Article
          PMC6948970 PMC6948970 6948970 1669405
          10.1080/15476286.2019.1669405
          6948970
          31532704
          a213d5cc-264f-4d48-930b-d19a7bcc9aa2
          © 2019 Informa UK Limited, trading as Taylor & Francis Group
          History
          : 22 June 2019
          : 9 September 2019
          : 14 September 2019
          Page count
          Figures: 7, Tables: 2, References: 48, Pages: 14
          Funding
          Funded by: All-India Institute of Medical Sciences 10.13039/501100007338
          Award ID: A-489
          Funded by: Council of Scientific and Industrial Research 10.13039/501100001412
          Award ID: 09/006(0451)/2015-EMR-I
          This work was supported by the All India Institute of Medical Sciences [A-489]; Council of Scientific and Industrial Research [09/006(0451)/2015-EMR-I].
          Categories
          Research Paper

          versican,therapeutics,bone marrow microenvironment,microRNAs,Multiple myeloma

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