4.5 Article

Tumor activated platelets induce vascular mimicry in mesenchymal stem cells and aid metastasis

期刊

CYTOKINE
卷 158, 期 -, 页码 -

出版社

ACADEMIC PRESS LTD- ELSEVIER SCIENCE LTD
DOI: 10.1016/j.cyto.2022.155998

关键词

Mesenchymal-stem-cells; Platelets; Vascular -mimicry; Metastasis; E-cadherin; Vimentin

资金

  1. Department of Science and Technology, New Delhi, Government of India [SB/YS/LS-289/2013, SR/WOS-A/LS-152/2017]
  2. Council of Scientific and Industrial Research, New Delhi, Government of India [09/030 (0067) 2011- EMR-I, 09/030 (0086) /2019-EMR-I]
  3. University Grant Commission, New Delhi [21/06/2015, 19/06/2016, 191620061322]
  4. Indian Council of Medical Research, New Delhi, India [61/1/2019-BMS]

向作者/读者索取更多资源

The extent of cancer metastasis affects platelet activation in the tumor microenvironment. Activated platelets enhance the migration of mesenchymal stem cells (MSCs) in secondary metastatic sites, leading to the formation of vascular mimicry (VM). This VM phenomenon has been observed in various types of cancer and is associated with poor prognosis.
Extent of metastasis influences activation of platelets in tumor-microenvironment. Activated platelets potentiate mesenchymal-stem-cells (MSCs) to migrate in secondary metastatic sites without participation in process of invasion. Presence of higher percentage of MSCs along with activated-platelets induces formation of vascular -mimicry (VM). The pathophysiology, VM, has already been reported in multiple types of cancer including lung, ovary, melanoma etc. and related to poor-prognosis. Interaction of MSCs with platelets in cell-to-cell contact dependent manner is essential for their migration, thereby, VM. Evidences are obtained suggesting that under influence of tumor-associated-activated-platelets, expressions of vimentin, ve-cadherin are increased, along with decrease in e-cadherin on CD105+ MSCs in both mRNA and protein levels that may help in formation of vessel like structure in VM. Adoptive transfer of MSCs along with tumor-activated-platelets causes greater B16 melanoma metastasis at lungs in comparison to MSCs with non-activated platelets. Presence of CD105+Vimentin+ MSCs in vessel like structure in the metastatic lung confirms the involvement of platelet-activated-MSCs in VM, thereby, in metastasis.

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