Yuasa I, Umetsu K, Ago K, Iijima K, Nakagawa M, Irizawa Y
Department of Legal Medicine, Faculty of Medicine, Tottori University, Yonago, Japan.
Leg Med (Tokyo). 2001 Dec;3(4):213-9. doi: 10.1016/s1344-6223(01)00040-2.
In this study alpha-1-antitrypsin (AAT) phenotypes at the protease inhibitor (PI) locus were determined by isoelectric focusing of native and desialylated serum samples from 236 Japanese subjects living in the western part of Japan. The shifts in relative mobility between some PI types were observed before and after desialylation. This technique was useful in distinguishing between some PI M subtypes and variants. The molecular basis of four variant alleles, including two new alleles found in this study, was characterized: PI E(tokyo) [Lys(335)(AAG)--> Glu(GAG)] and PI N(nagato) [Leu(276)(CTG)-->Pro(CCG)] arose from PI M1(Val(213)) and PI M2, respectively. A new PI P(yonago) [Asp(19)(GAT)-->Ala(GCT)] originated from PI M1(Val(213)). A new PI M5(gunma) [Pro(362)(CCC)-->Ser(TCC)], arising from PI M3, was the sixth allele involving a mutation at codon 362, which is suggested to be a mutation hot spot. PI M5(gunma) was likely to show normal AAT levels and function although the mutations occurred near codon 358 for Met(358). The molecular basis of PI variant alleles found in Japanese was different from that reported in previous studies.
在本研究中,通过对居住在日本西部的236名日本受试者的天然和去唾液酸化血清样本进行等电聚焦,确定了蛋白酶抑制剂(PI)位点的α1-抗胰蛋白酶(AAT)表型。观察到去唾液酸化前后一些PI类型之间相对迁移率的变化。该技术有助于区分一些PI M亚型和变体。对四个变异等位基因的分子基础进行了表征,包括本研究中发现的两个新等位基因:PI E(东京)[Lys(335)(AAG)→Glu(GAG)]和PI N(长门)[Leu(276)(CTG)→Pro(CCG)]分别源自PI M1(Val(213))和PI M2。一个新的PI P(米子)[Asp(19)(GAT)→Ala(GCT)]源自PI M1(Val(213))。一个新的PI M5(群马)[Pro(362)(CCC)→Ser(TCC)]源自PI M3,是第六个涉及密码子362突变的等位基因,该密码子被认为是一个突变热点。尽管突变发生在Met(358)的密码子358附近,但PI M5(群马)可能显示正常的AAT水平和功能。在日本人中发现的PI变异等位基因的分子基础与先前研究报道的不同。
