Crawford F C, Freeman M J, Schinka J, Abdullah L I, Richards D, Sevush S, Duara R, Mullan M J
Roskamp Institute and the University of South Florida Memory Disorder Clinic, 3515 E. Fletcher Avenue, Tampa, FL 33613, USA.
Neurosci Lett. 2000 Jul 28;289(1):61-5. doi: 10.1016/s0304-3940(00)01260-x.
The aspartyl protease Cathepsin D has previously been suggested to play a role in the Alzheimer's disease (AD) process because of its ability to cleave the beta-amyloid precursor protein and the possibility that it may be one of the 'secretase' enzymes. A functional C-->T polymorphism in the Cathepsin D gene (CATD) has been reported to be associated with increased risk for AD in Caucasian case-control studies; specifically, the T-carrying genotypes confer increased risk. We have examined this association in our own Caucasian dataset of 210 AD cases and 120 controls, and in an additional Hispanic dataset comprising 79 AD cases and 112 controls. In Hispanics we find a modest interaction between CATD genotype and age of onset on risk for AD, such that the non-T-carrying genotype confers increased risk. In our Caucasian dataset we find no evidence for association between the CATD polymorphism and AD, although we do observe a small tendency towards an increase in the T-carrying genotypes in the case group, consistent with previous studies. We conducted an aggregate analysis of the published Caucasian datasets and found evidence that this CATD polymorphism (or another locus in linkage disequilibrium) does contribute significant, but small (<2%) risk for AD.
天冬氨酸蛋白酶组织蛋白酶D先前被认为在阿尔茨海默病(AD)进程中发挥作用,因为它能够切割β-淀粉样前体蛋白,并且有可能是“分泌酶”之一。在白种人的病例对照研究中,据报道组织蛋白酶D基因(CATD)中的一种功能性C→T多态性与AD风险增加相关;具体而言,携带T的基因型会增加风险。我们在我们自己的由210例AD病例和120例对照组成的白种人数据集中,以及在另一个由79例AD病例和112例对照组成的西班牙裔数据集中研究了这种关联。在西班牙裔人群中,我们发现CATD基因型与AD发病年龄之间对AD风险存在适度的相互作用,使得非携带T的基因型会增加风险。在我们的白种人数据集中,我们没有发现CATD多态性与AD之间存在关联的证据,尽管我们确实观察到病例组中携带T的基因型有小幅增加的趋势,这与先前的研究一致。我们对已发表的白种人数据集进行了汇总分析,发现有证据表明这种CATD多态性(或处于连锁不平衡的另一个位点)确实对AD有显著但较小(<2%)的风险贡献。
