腓骨肌萎缩症的分子遗传学研究

医学遗传学在中国公共卫生事业中发挥重要作用--北京2004医学遗传学国际学术研讨会报告

The International Conference of Medical Genetics 2004 (ICMG2004) was held at Peking University Health Science Center on July 14-18, 2004. This conference is a part of the series that have been organized by the North American Association of Chinese Medical Geneticists (NAACMG) and the Chinese Medical Genetics Association (CMGA) and was initialized by the year of 2000 at Nanjing (ICMG2000, Nanjing). The mission of the series is to promote research, education, and clinical practice on medical genetics in China as well as in south Asian countries. This year, more than 200 participants from Mainland China, Taiwan, Hong Kong, England, and United States attended the ICMG2004. The conference opened with a remark addressed by Dr. Qi-de Han, the Vice Chairman of the Standing Committee of National Congress, who is the Director of Peking University Health Science Center and the Executive President of Peking University. Dr. Owen Rennet, Scientific Director of NICHD, NIH, gave a keynote speech at the opening session. Six sessions, chaired by Drs. Virginia Anderson, Wai-Yee Chan, Tian-jian Chen, Jiang Gu, Jian Han, Tao-Sheng Huang, Marilyn Li, Gary Lu, Ming Qi, Bai-Lin Wu, Nanbert Zhong, Chun-Yan Zhou, have covered various aspects of medical genetics with focus on birth defect, which is different from the main focus of neurogenetic disorders at ICMG2000. These aspects include inborn error of metabolism, intervention of birth defects, prenatal diagnosis and newborn screening, chromosome abnormalities, molecular basis of genetic disorders, environmental factors and birth defects, and genetic counseling and clinical management.

作者： 刊期： 2005年第01期

血清生化标记物结合胎儿颈部半透明膜厚度产前筛查胎儿染色体异常

目的:探讨孕早期胎儿染色体异常的产前筛查方案.方法: 采用时间分辨荧光免疫法(TRFIA)对孕11～14周的2 739例孕妇血清中的人绒毛促性腺激素β亚单位(β-hCG)、妊娠相关血浆蛋白A(PAPP-A)进行检测,同时利用腹式或阴道B型超声波测量胎儿颈部半透明膜(NT)厚度,筛查出22例染色体异常胎儿(通过羊水细胞染色体核型分析明确诊断),比较分析22例染色体异常胎儿与870例对照组三种标记物水平.结果: 病例组NT和β-hCG值明显较对照组高,PAPP-A值明显比对照组低,差异有统计学意义,三项指标联合筛查,胎儿染色体异常检出率为91.67%,假阳性率为11.16%. 结论: 孕早期NT+β-hCG+PAPP-A三联筛查方案对孕早期产前筛查胎儿染色体异常有较好的实用价值.

作者：廖世秀；黄飞飞；杨艳丽；宋子博；王应太；王兆才；屈献忠；陈汉平 刊期： 2005年第01期

溶酶体内胱氨酸可促进细胞凋亡并导致胱氨酸贮积症的表型发生

SUMMARY　Nephropathic cystinosis is a lethal inborn error of metabolism that destroys kidney function by age 10 years. It is characterized by lysosomal cystine accumulation. How the cystine causes the phenotype is an open question. We propose that during apoptosis, permeablized lysosomes permit cystine to reach the cytosol where mixed disulfide formation occurs, augmenting apoptosis by interaction with a variety of pro-apoptotic proteins.

作者： 刊期： 2005年第01期

DNA错配修复(DNA mismatch repair,MMR)

作者： 刊期： 2005年第01期

一种筛查中国人遗传性耳聋和氨基糖苷耳毒性易感人群的分子遗传学方法

Objective: To develop a molecular screening test for genetic defects on hearing loss related genes has significant impacts on early identification of hereditary hearing loss and genetic susceptibility to aminoglycoside ototoxicity. Early identification of pre-lingual hearing loss is very important for patient's language development, academic achievement, and social skill. Two common mutations, the 235delC in GJB2 gene and the mutation A1555G in mitochondrial DNA, are included in the newly developed screening panel for Chinese population. Methods: A molecular genetic assay, based on fluorescent labeled multiplex PCR and automatic DNA fragment analyzing techniques, was developed to detect both mutations simultaneously. Results: This assay was able to detect both mutations from patient's samples, and pooled DNA tests, as well as suitable to detect mutation from the DNA extracted from dried blood spot and buccal swab. Conclusion: This assay could be a useful tool for newborn screening and carrier screening for the hereditary hearing loss for the Chinese population.

作者： 刊期： 2005年第01期

儿童青少年双生子胰岛素敏感性的遗传度估计及影响因素分析

目的:分析影响儿童青少年的胰岛素敏感性的遗传和环境因素,并探讨其中体质指数(body mass index, BMI)、年龄和性别的作用.方法:选择5～18岁同性别双生子296对,平均年龄(12.4±3.5)岁,其中同卵双生子(MZ)223对,异卵双生子(DZ)73对.在DNA卵性鉴定基础上,应用Mx软件模型拟合分别计算BMI调整前后稳态模型胰岛素抵抗指数(homeostasis model assessment insulin resistance index, HOMA IR)和β细胞功能指数(HOMA β-cell function index,HBCI)的遗传度,并检验年龄和性别对于模型的作用.结果:HOMA IR与年龄、性别和BMI相关,HBCI与年龄相关,遗传分析HOMA IR、HBCI的模型为ACE,BMI调整前后HOMA IR男女生遗传度不同,HBCI无明显变化.调整后HOMA IR、HBCI遗传度分别为0.25、0.24.结论:儿童青少年人群中HOMA IR、HBCI受遗传和环境因素共同作用,环境因素的影响似乎更大;BMI是影响机体胰岛素敏感性的重要因素;年龄和性别对遗传度的影响可能不大.

作者：陈天娇；季成叶；逄增昌；杨业鹏；王伟；李红娟；胡永华 刊期： 2005年第01期

人DNA修复基因HR24L/HRAD17校正酵母细胞减数分裂缺陷表型

啤酒酵母(Saccharomyces cerevisiae)DNA修复基因RAD24在进化上具有高度保守性, 非洲粟酒酵母(Schizosaccaromyces pombe)的同源物则是RAD17.我们分离了啤酒酵母RAD24基因温度敏感突变株rad24L,进而用遗传互补法克隆出人类同源基因HR24L (北京医科大学学报,1999,31:269) .继我们报道之后,美国哈佛大学学者通过分析基因组信息,比较与非洲粟酒酵母RAD17同源片段,利用PCR方法扩增出人类RAD17同源cDNA,然后筛选文库获得人类RAD17(HRAD17)基因(Cancer Research, 1999,59:2023-2028),序列测定结果表明与我们克隆的HR24L是同一个基因.该基因编码的产物不仅参与DNA损伤切除修复和重组修复,而且还参与细胞周期检定点调控.鉴于细胞周期检定点调控是体细胞进行有丝分裂(mitosis)和生殖细胞进行减数分裂(meiosis)共有的周期性事件,因此,我们用遗传学方法分离酵母细胞减数分裂突变株,用功能互补法研究人HR24L基因的互补作用.

作者：孙艳；韩云；朱应葆 刊期： 2005年第01期

同步多色荧光原位杂交技术的建立及临床应用

目的:建立同步多色荧光原位杂交技术在外周血、羊水及单个胚胎细胞及骨髓细胞等样本中的实验方法,探索其在细胞遗传学、产前诊断、胚胎种植前诊断以及在血液病中的应用. 方法: 取外周血淋巴细胞、羊水细胞和不适于胚胎移植及冷藏的受精胚胎细胞、骨髓细胞分别制片,用相应的荧光标记的探针进行原位杂交,荧光显微镜取图分析. 结果:建立获得稳定可行的各类标本的实验方法. 结论:应用多色荧光原位杂交技术可对染色体进行快速准确的诊断,并可应用于产前诊断和胚胎种植前诊断及血液病的诊断.

作者：黎青；孙筱放；陈欣洁；孔舒；郑育红；黄艳仪 刊期： 2005年第01期

腓骨肌萎缩症的分子遗传学研究

腓骨肌萎缩症也称为Charcot-Marie-Tooth病(CMT),是一类高发病率的周围神经系统单基因遗传病,可发生于世界范围的各个种族之中,发病率为1/2 500.遗传方式主要为常染色体显性遗传(AD),也可见常染色体隐性遗传(AR)及X连锁显性或隐性遗传(XD或XR).即使是同一家庭中的患者,其患病的严重程度也会不同.

作者：章远志；Nanbert Zhong 刊期： 2005年第01期

应用多重连接探针扩增法简便高效检测Prader-Willi综合征的基因缺失

Objective: Prader-Willi syndrome (PWS) is characterized by severe hypotonia and feeding difficulties in early infancy, followed by excessive eating and gradual development of morbid obesity in later infancy or early childhood. Patients with PWS are often too young to manifest sufficient features or have atypical findings, making genetic testing important to confirm the diagnosis of PWS. Approximately 99% of patients with PWS have a diagnostic abnormality in the parent-specific methylation imprint within the Prader-Willi critical region (PWCR) at chromosome 15q11.2-q12. Of them, 70% have a paternal deletion; 25% have a maternal uniparental disomy (UPD); and <5% have a mutation in the imprinting center. Methods: Current techniques can identify a diagnostic abnormality, such as paternal deletion or maternal UPD for most of patients with PWS, but they are labor-intensive and cost-expensive. Multiplex ligation-dependent probe amplification (MLPA) is a novel, simple, and cost-effective technique for analysis of relative quantification in a single assay, which has recently been applied for the detection of genomic deletions, duplications, and amplifications in a variety of genes. Results: Six out of 20 patients referred for genetic diagnosis of PWS were found to have a deletion by MLPA, confirmed by FISH and DNA methylation analysis with 100% concordance. Conclusion: MLPA's high sensitivity and specificity for deletion detection is the same as FISH or Southern blot based analysis. Additional collaborative effort for developing and validating the complete MLPA-PWS assay, for not only detecting deletion but also identifying methylation abnormality, is on going.

作者： 刊期： 2005年第01期

中国汉族人群腓骨肌萎缩症Cx32基因突变分析

Objective: To investigate the Cx32 mutation features and the clinical manifestations of Chinese patients with Charcot-Marie-Tooth disease(CMT). Methods: Twenty-four of 65 unrelated CMT patients were selected for Cx32 mutation screening after the exclusion of the CMT1A 1.5 Mb duplication and male-to-male transmission. The motor and sensory nerve conduction studies were performed in all probands and most of their affected family members to establish the clinical CMT1 ,CMT2 or CMT intermediate diagnosis. The presence of mutations in the coding region of Cx32 was detected by single-strand conformation polymorphism analysis combined with direct sequencing. Results: We found 7 different point mutations in the coding region of Cx32 in a total of 7 families. All the patients were mildly to moderately affected with a clinical CMT1 or CMT intermediate diagnosis. The mutation Arg15Gln was inherited with X-linked recessive trait in family 1 involved in our study. The Arg75Trp mutation was detected in a family with X-linked dominant CMT and autosomal recessive nonsydromic hearing loss. The clinical phenotype of the Thr188Ala mutation was firstly reported. Conclusion: Seven different Cx32 point mutations were detected and the percentage of Chinese CMT families with Cx32 mutation is about 10% in our study. The inheritance model of CMT secondary to Cx32 mutation could be X-linked dominant, X-linked recessive or sporadic. Male patients are usually more severely affected than females with slower nerve conduction velocities. Cx32 mutation screening should be firstly performed in those CMT families without male-to-male transmission and CMT1A duplication.

作者：张如旭；罗巍；资晓宏；夏昆；蔡芳；萧剑峰；赵国华；张付峰；沈潞；江泓；唐北沙 刊期： 2005年第01期

北京1200例汉族人群中长链脂肪酸氧化酶G1528C基因突变筛查

目的: 研究北京地区1 200例汉族人群线粒体脂肪酸氧化代谢中的三功能蛋白酶(mitochondrial trifunctional protein,MTP)α亚单位的长链三羟基酰基辅酶A脱氢酶(long chain 3-hydroxyacyl-CoA dehydrogenase,LCHAD)G1528C基因的突变频率.方法: 应用聚合酶链反应-限制性片段长度多态性(polymerase chain reaction-restricted fragment length polymorphism, PCR-RFLP)技术分析1 200例汉族正常产妇脐血MTP的α亚单位G1528C基因突变携带情况.实验以西方人种的G1528C杂合子标本为阳性对照,同时设立阴性和空白对照作为实验技术质控标准.结果: 1 200例汉族产妇脐血标本G1528C 基因经PCR-RFLP突变筛查检测后,未见有与阳性对照标本相对分子质量相同的条带出现.结论: 中国人群与白种人之间可能存在着种族差异,西方人种中常见的MTPα亚单位的G1528C基因突变可能不是中国人种中常见的突变位点.

作者：朱锦明；杨孜；余梅；王荣；叶蓉华；杨惠霞；翟桂荣；王琪 刊期： 2005年第01期

核纤层蛋白病--一个基因,多种疾病

核纤层蛋白病(laminopathies)是指由LMNA基因及其编码蛋白lamin A/C异常引起的一组人类遗传病[1].根据临床特征不同,至今被认识的核纤层蛋白病已有10种,除一种由影响成熟lamin A形成的FACE-1基因突变引起外[2],其余9种均由LMNA基因突变引起,其中包括2种既可以常染色体显性又可以常染色体隐性遗传的遗传病:Emery-Dreifuss 肌营养不良(Emery-Dreifuss muscular dystrophy, EDMD,常显EDMD2,常隐EDMD3)[3,4] 和腓骨肌萎缩症2型(Charcot-Marie-Tooth2,常显AD-CMT2,常隐AR-CMT2)[5,6];6种常染色体显性遗传病:肢带型肌营养不良1B(limb girdle muscular dystrophy1B,LGMD1B)[7],扩张性心肌病伴心脏传导阻滞1A(dilated cardiomyopathy and cardiac conduction defects1A, CMD1A)[8],家族部分性脂肪营养不良(familial partial lipodystrophy, FPLD)[9],脂肪营养不良、胰岛素抵抗型糖尿病、弥漫性白黑皮病样丘疹、肝脂肪变性和心肌病综合征(lipoatrophy & insulin-resistant diabetes & disseminated leukomelanodermic papules & liver steatosis and cardiomyopathy,LDHPC)[10],Werner综合征(Werner syndrome, WRN)[11]和早老症(Hutchinson-Gilford progeria syndrome,HGPS)[12];1种常染色体隐性遗传病: Mandibuloacral dysplasia(MAD)[13].

作者：宋书娟；章远志；Nanbert Zhong 刊期： 2005年第01期

基因表达与哺乳动物DNA碱基GC含量的关系:统计学意义和生物相关性

作者： 刊期： 2005年第01期

增加的淀粉样β蛋白(Ab42)和晚发型阿尔茨海默病与尿激酶型血纤维蛋白溶酶原激活因子基因中的单个核苷酸多态性相关

作者： 刊期： 2005年第01期

21三体与母亲年龄关系的新发现

作者： 刊期： 2005年第01期

细胞标志蛋白CK7,Vim和P53在子宫内膜癌不同亚型发生机制中的作用

目的:检测细胞标志蛋白及P53在子宫内膜癌细胞的表达,探讨它们参与不同亚型子宫内膜癌发病的可能机制,分析其与肿瘤生物学行为的关系.方法:采用免疫组织化学法检测131例子宫内膜癌患者不同亚型、不同临床分期及不同分化程度的子宫内膜细胞中CK7,Vim及P53的表达.结果:CK7及Vim的表达分别与P53的表达存在正相关性.内膜样腺癌细胞中CK7表达高于其他类型,而Vim及P53的表达降低.Vim的表达与临床分期呈正相关;Vim及P53的表达阳性率随细胞分化级别上升而增加,具有相关性.结论:CK7、Vim、P53的编码基因可能通过转录水平的相互调控机制参与不同亚型子宫内膜癌发生及发展过程,CK7,Vim及P53可作为判断肿瘤的预后及选择治疗方案有用的参考指标.

作者：曾琪；张红萍；刘惜时；Nanbert Zhong 刊期： 2005年第01期

先天性心脏病核心家庭血清同型半胱氨酸水平及相关基因多态性研究

目的:了解MTHFR C677T、MS A2756G、MTHFD G1958A和CBS 844 ins68bp位点在中国北方正常人群中的基因型分布,并评价单一或复合位点基因变异与叶酸、维生素B12、同型半胱氨酸(Hcy)水平及先天性心胖病(CHD)的关系.方法:选择辽宁省192例CHD患者及其父母作为病例组,同一地区年龄、性别匹配的124名正常人及其父母作为对照组,采用PCR-RFLP方法检测其基因型,放射免疫法和荧光偏振免疫法测定血清叶酸、维生素B12和Hcy水平,比较两组差异.结果:中国北方正常人群中,这四个位点的突变等位基因频率分别为MTHFR 51.18%, MS 7.58%, MTHFD 24.32%, CBS插入频率 2.36%;CBS 844 ins68bp位点杂合型频率病例组明显高于对照组(子代为12.57% 和 2.97%, 父亲为10.88% 和 3.09%,母亲为11.54% 和 1.02%),子代的OR值为4.70 (95% CI 1.34～25.15),父亲的OR值为3.83 (95% CI 1.05～20.98),母亲的OR值为12.65 (95% CI 1.92～532.47),其他三个位点两组差异无统计学意义;MTHFR、CBS和MTHFD三个位点联合基因变异的母亲、MTHFR 和 CBS两个位点联合基因变异的母亲(OR=8.44,95%CI:1.23～362.26)、MTHFD 和 CBS两个位点联合基因变异的母亲在病例组中所占的比例明显高于对照组;病例组父亲和母亲的血清叶酸水平明显高于对照组;病例组母亲的血清Hcy水平高于对照组,但差异无统计学意义;MTHFR 和 MTHFD两个位点为纯合型者的血清叶酸和维生素B12水平轻微下降,而血清Hcy水平轻微上升;联合基因变异使血清叶酸、维生素B12和Hcy水平出现下降趋势.结论:这四个位点的基因多态性存在着种族和地区差异,CBS 844 ins68bp位点突变可能是CHD发生的一个危险因素,亲代(尤其是母亲)的插入突变可使其后代发生CHD的危险性升高.

作者：李勇；成君；朱文丽；刀京晶；闫丽盈；李孟忆；李书琴 刊期： 2005年第01期

单细胞二重巢式PCR扩增影响因素初探

目的: 对影响单细胞二重巢式PCR扩增的因素进行初步探讨.方法:针对β-珠蛋白基因CD41-42、IVS-Ⅱ654突变位点区域采用二重巢式PCR,分别以不同的引物浓度组合、不同的Taq DNA聚合酶、不同的中和缓冲液、PCR反应前采用或不采用98 ℃预变性扩增单个淋巴细胞和/或单卵裂球,了解这些因素对PCR扩增效率的影响.结果: 不同的引物浓度组中,终浓度为0.25 μmol/L R1+F1引物对与 0.3 μmol/L R2+F2引物对配对扩增效率高;不同的Taq DNA聚合酶中TaKaRa EX Taq的扩增效率高;中和缓冲液-1(200 mmol/L Tricine)的扩增效率显著高于中和缓冲液-2(900 mmol/L Tris·HCl, pH 8.3/300 mmol/L KCl/200 mmol/L HCl)的扩增效率(P<0.05);单细胞PCR反应前采用98 ℃预变性与不采用98 ℃预变性的扩增效率间差异无统计学意义.结论:不同引物浓度组合、不同的Taq DNA聚合酶、不同的中和缓冲液对单细胞的二重巢式PCR的扩增效率存在明显差异,而PCR反应前采用98 ℃预变性不能提高PCR扩增效率.

作者：钟昌高；李麓芸；陆长富；林戈；卢光琇 刊期： 2005年第01期

新生儿EPHX1和GSTT1基因多态性与低出生体重的关系

目的:探讨微粒体环氧化物水解酶基因(microsomal epoxide hydrolase gene,EPHX1)139位点多态性和谷胱甘肽转硫酶theta1基因(the glutathione S-transferase theta1 gene,GSTT1)多态性对新生儿低出生体重的影响.方法:采用病例对照调查方法,使用统一设计的调查问卷,由经过培训的调查员于1998年至1999年在安徽省安庆市各县级医院对入院分娩孕妇及其单胎、活产的低出生体重儿和正常出生体重的对照新生儿进行调查,共得到246个母亲-新生儿对,其中低出生体重组73对, 正常出生体重对照组173对,用PCR-RFLP方法确定基因型.结果:EPHX1 His139His纯合子基因型与His139Arg杂合子基因/Arg139Arg纯合子基因型比较, GSTT1缺失基因型与存在基因型比较,多因素Logistic回归模型在经混杂因素(母亲年龄、文化程度、生育史、新生儿性别、孕周)调整前后,均未见导致低出生体重的危险性有显著性增加.进一步分析EPHX1139位点多态性和GSTT1位点多态性之间对低出生体重的影响,结果显示GSTT1缺失基因型和EPHX1His139His纯合子基因型之间有明显联合作用,导致低出生体重的危险因素增加(OR＝3.46, P=0.035).结论:基因EPHX1 139位点多态性和GSTT1位点多态性对低出生体重的影响有明显联合作用.

作者：梁红业；陈大方；张涛；杨帆；汪六六；陈栎；吴白燕 刊期： 2005年第01期