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Piezo1 expression in chondrocytes controls endochondral ossification and osteoarthritis development
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作者 Laura J.Brylka Assil-Ramin Alimy +18 位作者 Miriam E.A.Tschaffon-Müller Shan Jiang Tobias Malte Ballhause Anke Baranowsky Simon von Kroge Julian Delsmann Eva Pawlus Kian Eghbalian Klaus Püschel Astrid Schoppa Melanie Haffner-Luntzer david j.beech Frank Timo Beil Michael Amling Johannes Keller Anita Ignatius Timur A.Yorgan Tim Rolvien Thorsten Schinke 《Bone Research》 SCIE CAS CSCD 2024年第1期199-214,共16页
Piezo proteins are mechanically activated ion channels,which are required for mechanosensing functions in a variety of cell types.While we and others have previously demonstrated that the expression of Piezo1 in osteo... Piezo proteins are mechanically activated ion channels,which are required for mechanosensing functions in a variety of cell types.While we and others have previously demonstrated that the expression of Piezo1 in osteoblast lineage cells is essential for boneanabolic processes,there was only suggestive evidence indicating a role of Piezo1 and/or Piezo2 in cartilage.Here we addressed the question if and how chondrocyte expression of the mechanosensitive proteins Piezo1 or Piezo2 controls physiological endochondral ossification and pathological osteoarthritis(OA)development.Mice with chondrocyte-specific inactivation of Piezo1(Piezo1^(Col2a1Cre)),but not of Piezo2,developed a near absence of trabecular bone below the chondrogenic growth plate postnatally.Moreover,all Piezo1^(Col2a1Cre) animals displayed multiple fractures of rib bones at 7 days of age,which were located close to the growth plates.While skeletal growth was only mildly affected in these mice,OA pathologies were markedly less pronounced compared to littermate controls at 60 weeks of age.Likewise,when OA was induced by anterior cruciate ligament transection,only the chondrocyte inactivation of Piezo1,not of Piezo2,resulted in attenuated articular cartilage degeneration.Importantly,osteophyte formation and maturation were also reduced in Piezo1^(Col2a1Cre) mice.We further observed increased Piezo1 protein abundance in cartilaginous zones of human osteophytes.Finally,we identified Ptgs2 and Ccn2 as potentially relevant Piezo1 downstream genes in chondrocytes.Collectively,our data do not only demonstrate that Piezo1 is a critical regulator of physiological and pathological endochondral ossification processes,but also suggest that Piezo1 antagonists may be established as a novel approach to limit osteophyte formation in OA. 展开更多
关键词 Piezo1 markedly OSSIFICATION
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人血管内皮细胞特异性表达TMEM 16B 被引量:1
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作者 付兆君 刘红巾 +2 位作者 程军 徐先荣 david j.beech 《空军医学杂志》 2015年第3期151-153,157,共4页
目的探讨人血管内皮细胞上TMEM16A、TMEM16B蛋白的表达情况,并初步探讨后者的功能。方法采用实时PCR方法检测人脐带静脉内皮细胞(human umbilical vein endothelial cells,HUVECs)中TMEM16A、TMEM16B的基因表达情况。采用Western-Blot... 目的探讨人血管内皮细胞上TMEM16A、TMEM16B蛋白的表达情况,并初步探讨后者的功能。方法采用实时PCR方法检测人脐带静脉内皮细胞(human umbilical vein endothelial cells,HUVECs)中TMEM16A、TMEM16B的基因表达情况。采用Western-Blot及免疫荧光染色方法进一步证实HUVECs中TMEM16B的表达情况。Fura-2am标记HUVECs后采用Flex-station检测细胞内钙变化情况。结果 HUVECs细胞表达TMEM16B,而未表达TMEM16A。Western-Blot及免疫荧光方法从蛋白水平证明HUVECs表达TMEM16B。在使用TMEM16B的si RNA干预HUVECs后,无论是有钙及无钙溶液,在50 n M血管内皮细胞生长因子(vascular endothelial growth factor,VEGF)刺激下,钙浓度峰值均增大,而且峰值出现时间提前。结论人血管内皮细胞特异性表达TMEM16B,生理情况下TMEM16B对VEGF刺激引起的Ca2+的释放过程可能起着负向调节作用。 展开更多
关键词 血管内皮细胞 TMEM16B 离子通道 细胞内钙调节
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