Blaschke R J, Monaghan A P, Schiller S, Schechinger B, Rao E, Padilla-Nash H, Ried T, Rappold G A
Institute of Human Genetics, Heidelberg University, Im Neuenheimer Feld 328, 69120 Heidelberg, Germany.
Proc Natl Acad Sci U S A. 1998 Mar 3;95(5):2406-11. doi: 10.1073/pnas.95.5.2406.
Deletion of the SHOX region on the human sex chromosomes has been shown to result in idiopathic short stature and proposed to play a role in the short stature associated with Turner syndrome. We have identified a human paired-related homeobox gene, SHOT, by virtue of its homology to the human SHOX and mouse OG-12 genes. Two different isoforms were isolated, SHOTa and SHOTb, which have identical homeodomains and share a C-terminal 14-amino acid residue motif characteristic for craniofacially expressed homeodomain proteins. Differences between SHOTa and b reside within the N termini and an alternatively spliced exon in the C termini. In situ hybridization of the mouse equivalent, OG-12, on sections from staged mouse embryos detected highly restricted transcripts in the developing sinus venosus (aorta), female genitalia, diencephalon, mes- and myelencephalon, nasal capsula, palate, eyelid, and in the limbs. SHOT was mapped to human chromosome 3q25-q26 and OG-12 within a syntenic region on chromosome 3. Based on the localization and expression pattern of its mouse homologue during embryonic development, SHOT represents a candidate for the Cornelia de Lange syndrome.
人类性染色体上SHOX区域的缺失已被证明会导致特发性身材矮小,并被认为在与特纳综合征相关的身材矮小中起作用。我们通过与人类SHOX和小鼠OG-12基因的同源性,鉴定出了一个人类配对相关的同源盒基因SHOT。分离出了两种不同的异构体,SHOTa和SHOTb,它们具有相同的同源结构域,并共享一个C末端14个氨基酸残基的基序,这是颅面部表达的同源结构域蛋白的特征。SHOTa和b之间的差异存在于N末端和C末端的一个可变剪接外显子中。在分期小鼠胚胎切片上对小鼠同源物OG-12进行原位杂交,在发育中的静脉窦(主动脉)、雌性生殖器、间脑、中脑和延髓、鼻囊、腭、眼睑以及四肢中检测到高度受限的转录本。SHOT被定位到人类染色体3q25-q26,OG-12位于染色体3上的一个同线区域内。基于其小鼠同源物在胚胎发育过程中的定位和表达模式,SHOT代表科妮莉亚·德·朗热综合征的一个候选基因。
