Culiat C T, Stubbs L, Nicholls R D, Montgomery C S, Russell L B, Johnson D K, Rinchik E M
Biology Division, Oak Ridge National Laboratory, TN 37831-8077.
Proc Natl Acad Sci U S A. 1993 Jun 1;90(11):5105-9. doi: 10.1073/pnas.90.11.5105.
Genetic and molecular analyses of a number of radiation-induced deletion mutations of the pink-eyed dilution (p) locus in mouse chromosome 7 have identified a specific interval on the genetic map associated with a neonatally lethal mutation that results in cleft palate. This interval, closely linked and distal to p, and bracketed by the genes encoding the alpha 5 and beta 3 subunits of the type A gamma-aminobutyric acid receptor (Gabra5 and Gabrb3, respectively), contains a gene(s) (cp1; cleft palate 1) necessary for normal palate development. The cp1 interval extends from the distal breakpoint of the prenatally lethal p83FBFo deletion to the Gabrb3 locus. Among 20 p deletions tested, there was complete concordance between alterations at the Gabrb3 transcription unit and inability to complement the cleft-palate defect. These mapping data, along with previously described in vivo and in vitro teratological effects of gamma-aminobutyric acid or its agonists on palate development, suggest the possibility that a particular type A gamma-aminobutyric acid receptor that includes the beta 3 subunit may be necessary for normal palate development. The placement of the cp1 gene within a defined segment of the larger D15S12h (p)-D15S9h-1 interval in the mouse suggests that the highly homologous region of the human genome, 15q11-q13, be evaluated for a role(s) in human fetal facial development.
对小鼠7号染色体上多个辐射诱导的粉红眼稀释(p)位点缺失突变进行的遗传和分子分析,在遗传图谱上确定了一个特定区间,该区间与一个导致腭裂的新生致死突变相关。这个区间与p紧密连锁且位于其远端,以分别编码A型γ-氨基丁酸受体α5和β3亚基的基因(Gabra5和Gabrb3)为边界,包含一个正常腭发育所必需的基因(cp1;腭裂1)。cp1区间从产前致死性p83FBFo缺失的远端断点延伸至Gabrb3基因座。在测试的20个p缺失中,Gabrb3转录单位的改变与无法弥补腭裂缺陷之间完全一致。这些定位数据,连同先前描述的γ-氨基丁酸或其激动剂对腭发育的体内和体外致畸作用,提示包含β3亚基的特定A型γ-氨基丁酸受体可能是正常腭发育所必需的。cp1基因在小鼠较大的D15S12h(p)-D15S9h-1区间的一个确定片段内的定位表明,人类基因组的高度同源区域15q11-q13应评估其在人类胎儿面部发育中的作用。
