奶牛weaver综合症研究进展

奶牛weaver综合症(奶牛进行性脑脊髓退化症)是一种隐性遗传疾病,与产奶性能密切相关。文中综述了奶牛weaver综合症的主要病症、检测方法、weaver基因的研究进展以及从weaver基因入手检测奶牛产奶性能QTL(数量性状座位)的进展情况。

奶牛weaver基因连锁微卫星位点多态性分析

根据小鼠与牛的遗传比较图谱选择了牛第1号染色体上与weaver基因连锁的7个微卫星位点,并在新疆褐牛和荷斯坦牛群体中对这些微卫星位点进行了群体遗传学特性分析。结果表明:7个微卫星位点中,BM6438、BMS2321和BMS711属于高度多态位点,TGLA116为中度多态位点,INRA117、BMS4020和CA095属于低度多态位点。BM6438、BMS2321、BMS711和TGLA116可作为奶牛产奶性能分析的微卫星标记位点。

帕金森氏综合症发病机理研究:weaver基因研究

目的研究帕金森氏综合症的发病机理,评估wvGirk2对神经细胞生长发育和生命力的影响。方法给一类酪氨酸脱氢酶阳性的神经细胞(一种中枢神经源细胞),又称CAD细胞,引入由DNA编码的野生型和突变型离子通道。采用DNA克隆、免疫组化、WesternBlots免疫印迹等技术进行检测分析。用不同浓度(0.25μg/ml,0.5μg/ml,1.0μg/ml)的Girk2cDNA(对照组)和wvGirk2cDNA(观察组)质粒转染CAD细胞后,观察两组基因对转染CAD细胞的数目、蛋白质合成、神经突生长等指标的影响作用;并且观察MK801和Kir2.3对wvGirk2的抑制作用。结果高浓度wvGirk2转染的CAD细胞存活数目减少到约60%的单纯Girk2转染细胞数目;低浓度wvGirk2没有引起细胞死亡但是减少转染基因的蛋白质产物,且神经突生长也受wvGirk2影响;MK801和Kir2.3对wvGirk2有抑制作用。结论wvGirk2基因在weaver动物中有一种特殊功能,阻断wvGirk2通道能够防止细胞死亡。离子通道的存在和wvGirk2的转染可能对wvGirk2细胞的命运有显著影响。

奶牛微卫星基因座与产奶性能关系的研究

根据小鼠与牛的遗传比较图谱及相关报道选择了与weaver基因连锁的 7个微卫星基因座 ,并在荷斯坦牛群体中对这些基因座进行群体遗传学特性分析。选择具有中度以上多态性的 4个微卫星基因座 (BM6 4 38、BMS2 32 1、BMS711和TGLA116 )进行产奶性能的相关分析。最小二乘分析结果表明 ,4个微卫星基因座对产奶量影响不显著(P >0 .0 5 ) ,BM6 4 38和BMS711基因座对乳成分影响不显著 (P >0 .0 5 ) ,BMS2 32 1基因座对乳蛋白量和乳蛋白率有极显著的影响 (P <0 .0 1) ,TGLA116对乳蛋白量和乳蛋白率的影响达到 0 .0

EZH2基因变异致Weaver综合征1例

对南京医科大学附属儿童医院内分泌科2018年10月接诊的1例Weaver综合征患儿的临床资料进行回顾性分析。患儿,女,9岁2月龄,因"发现生长较快9年"就诊。患儿出生后发现生长较快,智力反应欠佳,言语不清,视物不清,脸型长,前额突,眼距宽,内眦赘皮,鼻梁塌陷,双手足有指垫,走路步态不协调,双足呈内"八"字。基因检测:EZH2基因15号外显子c.1720A>G(p.K574E)杂合变异,国内外尚未见报道,经Sanger测序验证,未检测到患儿父母携带该变异,由于该病系常染色体显性遗传,且患儿父母及胞哥均无相应症状,因此推断该突变为自发突变。结合患儿的特殊面容、临床表现及分子遗传学结果,诊断为Weaver综合征。

Spectrum of NSD1 gene mutations in southern Chinese patients with Sotos syndrome

Background Sotos syndrome is an overgrowth syndrome with characteristic facial gestalt and mental retardation of variable severity. Haploinsufficiency of the NSD 1 gene has been implicated as the major cause of Sotos syndrome, with a predominance of microdeletions reported in Japanese patients. This study was conducted to investigate into the spectrum of NSD1 gene mutations in southern Chinese patients with Sotos syndrome. Methods Thirty-six Chinese patients with Sotos syndrome and two patients with Weaver syndrome were subject to molecular testing. Results NSD1 gene mutations were detected in 26 （72%） Sotos patients. Microdeletion was found in only 3 patients, while the other 23 had point mutations （6 frameshift, 8 nonsense, 2 spice site, and 7 missense）. Of these, 19 mutations were never reported. NSD1 gene mutations were not found in the two patients with Weaver syndrome. Conclusions Most cases of Sotos syndrome are caused by NSD1 gene defects, but the spectrum of mutations is different from that of Japanese patients. Genotype-phenotype correlation showed that patients with microdeletions might be more prone to congenital heart disease but less likely to have somatic overgrowth. The two patients with Weaver syndrome were not found to have NSD1 gene mutations, but the number was too small for any conclusion to be drawn.