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MEST Regulates the Stemness of Human Periodontal Ligament Stem Cells.
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- المؤلفون: Hasegawa, Daigaku1 (AUTHOR); Hasegawa, Kana2 (AUTHOR); Kaneko, Hiroshi3 (AUTHOR); Yoshida, Shinichiro1 (AUTHOR); Mitarai, Hiromi4 (AUTHOR); Arima, Mai3 (AUTHOR); Tomokiyo, Atsushi1 (AUTHOR); Hamano, Sayuri3,5 (AUTHOR); Sugii, Hideki1 (AUTHOR); Wada, Naohisa4 (AUTHOR); Kiyoshima, Tamotsu2 (AUTHOR); Maeda, Hidefumi1,3 (AUTHOR)
- المصدر:
Stem Cells International. 7/8/2020, p1-15. 15p.
- الموضوع:
- معلومة اضافية
- نبذة مختصرة :
Periodontal ligament (PDL) stem cells (PDLSCs) have been reported as a useful cell source for periodontal tissue regeneration. However, one of the issues is the difficulty of obtaining a sufficient number of PDLSCs for clinical application because very few PDLSCs can be isolated from PDL tissue of donors. Therefore, we aimed to identify a specific factor that converts human PDL cells into stem-like cells. In this study, microarray analysis comparing the gene profiles of human PDLSC lines (2-14 and 2-23) with those of a cell line with a low differentiation potential (2-52) identified the imprinted gene mesoderm-specific transcript (MEST). MEST was expressed in the cytoplasm of 2-23 cells. Knockdown of MEST by siRNA in 2-23 cells inhibited the expression of stem cell markers, such as CD105, CD146, p75NTR, N-cadherin, and NANOG; the proliferative potential; and multidifferentiation capacity for osteoblasts, adipocytes, and chondrocytes. On the other hand, overexpression of MEST in 2-52 cells enhanced the expression of stem cell markers and PDL-related markers and the multidifferentiation capacity. In addition, MEST-overexpressing 2-52 cells exhibited a change in morphology from a spindle shape to a stem cell-like round shape that was similar to 2-14 and 2-23 cell morphologies. These results suggest that MEST plays a critical role in the maintenance of stemness in PDLSCs and converts PDL cells into PDLSC-like cells. Therefore, this study indicates that MEST may be a therapeutic factor for periodontal tissue regeneration by inducing PDLSCs. [ABSTRACT FROM AUTHOR]
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