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      KCI등재 SCIE SCOPUS

      Effects of Trichostatin A on the Chondrogenesis from Human Mesenchymal Stem Cells

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      https://www.riss.kr/link?id=A105916317

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      다국어 초록 (Multilingual Abstract)

      Histone deacetylase inhibitors (HDACi) are a class of compounds that suppress the function of histone deacetylases (HDACs). This study was performed to examine the effects of Trichostatin A (TSA), a typical HDACi, on chondrogenesis of human bone marro...

      Histone deacetylase inhibitors (HDACi) are a class of compounds that suppress the function of histone deacetylases (HDACs). This study was performed to examine the effects of Trichostatin A (TSA), a typical HDACi, on chondrogenesis of human bone marrow mesenchymal stem cells (hBMMSCs) and related molecular pathways. After evaluating the concentration for cytotoxicity and HDAC activity, hBMMSCs underwent chondrogenic differentiation in pellet culture with or without TSA for 21 days. The weight of TSA-treated pellets was 25% lower than that of untreated pellets. DNA level was not significantly different, but glycosaminoglycan content per DNA level was lower in TSA-treated pellets than that of untreated pellets. Gene expression of the chondrogenic markers (SOX9, Aggrecan, and Col2A1) decreased by by 12.9-fold, 8.9-fold, and 7.6-fold respectively in TSA-treated pellets compared with that in TSA-untreated pellets. TSA-treated pellets had lower cell density and lower proteoglycan staining content compared with those of TSA-untreated pellets. A microarray analysis from TSA-treated pellets showed that 1,467 chondrogenic-related genes were downregulated and 1,524 were upregulated by more than 2-fold compared with TSA-untreated pellets. Col10A1, TGF-b3, and SOX9 decreased significantly by 10-fold, 2.1-fold, and 3.2-fold respectively in TSA-treated pellets compared with those in untreated pellets, whereas expression of BMP4 and FGFR3 increased significantly by 2.1-fold and 5.4-fold respectively. It is concluded that TSAinhibits chondrogenesis and does not seem to be useful for cartilage tissue engineering of hBMMSCs.

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      참고문헌 (Reference)

      1 Vigushin DM, "Trichostatin A is a histone deacetylase inhibitor with potent antitumor activity against breast cancer in vivo" 7 : 971-976, 2001

      2 Wang JP, "Trichostatin A inhibits TGF-beta1 induced in vitro chondrogenesis of hMSCs through Sp1 suppression" 81 : 119-126, 2011

      3 Katsura T, "The effects of trichostatin A on the oncolytic ability of herpes simplex virus for oral squamous cell carcinoma cells" 16 : 237-245, 2009

      4 Chen TH, "Sodium butyrate activates ERK to regulate differentiation of mesenchymal stem cells" 355 : 913-918, 2007

      5 Sengupta N, "Regulation of histone deacetylase activities" 93 : 57-67, 2004

      6 Herzog EL, "Plasticity of marrow-derived stem cells" 102 : 3483-3493, 2003

      7 Ja¨hn K, "Pellet culture model for human primary osteoblasts" 20 : 149-161, 2010

      8 Young DA, "Histone deacetylase inhibitors modulate metalloproteinase gene expression in chondrocytes and block cartilage resorption" 7 : R503-R512, 2005

      9 Karantzali E, "Histone deacetylase inhibition accelerates the early events of stem cell differentiation: transcriptomic and epigenetic analysis" 9 : R65-, 2008

      10 El-Serafi AT, "Epigenetic modifiers influence lineage commitment of human bone marrow stromal cells : differential effects of 5-aza-deoxycytidine and trichostatin A" 81 : 35-41, 2011

      1 Vigushin DM, "Trichostatin A is a histone deacetylase inhibitor with potent antitumor activity against breast cancer in vivo" 7 : 971-976, 2001

      2 Wang JP, "Trichostatin A inhibits TGF-beta1 induced in vitro chondrogenesis of hMSCs through Sp1 suppression" 81 : 119-126, 2011

      3 Katsura T, "The effects of trichostatin A on the oncolytic ability of herpes simplex virus for oral squamous cell carcinoma cells" 16 : 237-245, 2009

      4 Chen TH, "Sodium butyrate activates ERK to regulate differentiation of mesenchymal stem cells" 355 : 913-918, 2007

      5 Sengupta N, "Regulation of histone deacetylase activities" 93 : 57-67, 2004

      6 Herzog EL, "Plasticity of marrow-derived stem cells" 102 : 3483-3493, 2003

      7 Ja¨hn K, "Pellet culture model for human primary osteoblasts" 20 : 149-161, 2010

      8 Young DA, "Histone deacetylase inhibitors modulate metalloproteinase gene expression in chondrocytes and block cartilage resorption" 7 : R503-R512, 2005

      9 Karantzali E, "Histone deacetylase inhibition accelerates the early events of stem cell differentiation: transcriptomic and epigenetic analysis" 9 : R65-, 2008

      10 El-Serafi AT, "Epigenetic modifiers influence lineage commitment of human bone marrow stromal cells : differential effects of 5-aza-deoxycytidine and trichostatin A" 81 : 35-41, 2011

      11 Zhang S, "Effect of trichostatin a on viability and microRNA expression in human pancreatic cancer cell line BxPC-3" 30 : 265-268, 2008

      12 Aoyama T, "Cell-specific epigenetic regulation of ChM-I gene expression : crosstalk between DNA methylation and histone acetylation" 365 : 124-130, 2008

      13 Tuan RS, "Adult mesenchymal stem cells and cell-based tissue engineering" 5 : 32-45, 2003

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      학술지 이력

      학술지 이력
      연월일 이력구분 이력상세 등재구분
      학술지등록 한글명 : 조직공학과 재생의학
      외국어명 : Tissue Engineering and Regenerative Medicine
      2023 평가예정 해외DB학술지평가 신청대상 (해외등재 학술지 평가)
      2020-01-01 평가 등재학술지 유지 (해외등재 학술지 평가) KCI등재
      2013-10-01 평가 등재학술지 선정 (기타) KCI등재
      2012-01-01 평가 등재후보 1차 FAIL (기타) KCI등재후보
      2011-01-01 평가 등재후보 1차 PASS (등재후보1차) KCI등재후보
      2010-01-01 평가 등재후보 1차 FAIL (등재후보1차) KCI등재후보
      2008-01-01 평가 SCIE 등재 (신규평가) KCI등재후보
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      학술지 인용정보

      학술지 인용정보
      기준연도 WOS-KCI 통합IF(2년) KCIF(2년) KCIF(3년)
      2016 1.08 0.42 0.81
      KCIF(4년) KCIF(5년) 중심성지수(3년) 즉시성지수
      0.69 0.51 0.367 0.03
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