Jay Patrick Y, Harris Brett S, Maguire Colin T, Buerger Antje, Wakimoto Hiroko, Tanaka Makoto, Kupershmidt Sabina, Roden Dan M, Schultheiss Thomas M, O'Brien Terrence X, Gourdie Robert G, Berul Charles I, Izumo Seigo
Department of Cardiology, Children's Hospital, Boston, Massachusetts 02115, USA.
J Clin Invest. 2004 Apr;113(8):1130-7. doi: 10.1172/JCI19846.
Heterozygous mutations of the cardiac transcription factor Nkx2-5 cause atrioventricular conduction defects in humans by unknown mechanisms. We show in KO mice that the number of cells in the cardiac conduction system is directly related to Nkx2-5 gene dosage. Null mutant embryos appear to lack the primordium of the atrioventricular node. In Nkx2-5 haploinsufficiency, the conduction system has half the normal number of cells. In addition, an entire population of connexin40(-)/connexin45(+) cells is missing in the atrioventricular node of Nkx2-5 heterozygous KO mice. Specific functional defects associated with Nkx2-5 loss of function can be attributed to hypoplastic development of the relevant structures in the conduction system. Surprisingly, the cellular expression of connexin40, the major gap junction isoform of Purkinje fibers and a putative Nkx2-5 target, is unaffected, consistent with normal conduction times through the His-Purkinje system measured in vivo. Postnatal conduction defects in Nkx2-5 mutation may result at least in part from a defect in the genetic program that governs the recruitment or retention of embryonic cardiac myocytes in the conduction system.
心脏转录因子Nkx2 - 5的杂合突变通过未知机制导致人类房室传导缺陷。我们在基因敲除小鼠中发现,心脏传导系统中的细胞数量与Nkx2 - 5基因剂量直接相关。纯合突变胚胎似乎缺乏房室结原基。在Nkx2 - 5单倍体不足的情况下,传导系统中的细胞数量只有正常数量的一半。此外,Nkx2 - 5杂合基因敲除小鼠的房室结中整个连接蛋白40(-)/连接蛋白45(+)细胞群缺失。与Nkx2 - 5功能丧失相关的特定功能缺陷可归因于传导系统中相关结构的发育不全。令人惊讶的是,连接蛋白40(浦肯野纤维的主要缝隙连接亚型且可能是Nkx2 - 5的靶点)的细胞表达未受影响,这与体内测量的通过希氏 - 浦肯野系统的正常传导时间一致。Nkx2 - 5突变导致的出生后传导缺陷可能至少部分是由于控制胚胎心肌细胞在传导系统中募集或保留的遗传程序缺陷所致。
