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兔的κ链同种异型和同种型:编码b9的克隆的cDNA序列揭示了一种进化途径以及结构域间二硫键在定量同种异型表达中的可能作用。

Kappa-chain allotypes and isotypes in the rabbit: cDNA sequences of clones encoding b9 suggest an evolutionary pathway and possible role of the interdomain disulfide bond in quantitative allotype expression.

作者信息

McCartney-Francis N, Skurla R M, Mage R G, Bernstein K E

出版信息

Proc Natl Acad Sci U S A. 1984 Mar;81(6):1794-8. doi: 10.1073/pnas.81.6.1794.

Abstract

The constant regions of rabbit kappa light chains are unusual because the sequences of the allotypic forms can differ more from each other than do some variable regions with which they associate. We report the nucleic acid sequence of a full-length cDNA clone of b9 allotype and show comparisons to available sequences of the rabbit kappa allotypes b4, b5, and bas-N4. Our analyses suggest that the primordial rabbit kappa gene encoded a bas-like sequence. They also reveal a surprising difference in the position of the variable region cysteine that forms the interdomain disulfide bond that is unique to most rabbit kappa chains. One b9 cDNA sequence lacks the usual cysteine-80 and instead encodes cysteine-108, which in three-dimensional models appears capable of forming the interdomain disulfide bond with cysteine-171 in the constant region. A partial sequence of a second b9 clone encodes both cysteine-80 and cysteine-108; the translation product of this clone could have a free reactive sulfhydryl group that might lead to an unstable nonfunctional Ig molecule. The fact that pre-B cells with b9 kappa chains do not differentiate and expand into productive Ig-producing cells with frequencies comparable to the other allotypes may be explained if a substantial proportion of the gene products have a free sulfhydryl group. Our sequence results suggest that in cells differentiating to produce kappa light chains of b9 allotype the number and location of the cysteines influence immunoglobulin expression.

摘要

兔κ轻链的恒定区不同寻常,因为同种异型形式的序列彼此之间的差异可能比它们与之相关联的一些可变区之间的差异更大。我们报道了b9同种异型全长cDNA克隆的核酸序列,并与兔κ同种异型b4、b5和bas-N4的现有序列进行了比较。我们的分析表明,原始兔κ基因编码了一种bas样序列。它们还揭示了可变区半胱氨酸位置的惊人差异,该半胱氨酸形成了大多数兔κ链特有的结构域间二硫键。一个b9 cDNA序列缺少通常的半胱氨酸-80,取而代之的是编码半胱氨酸-108,在三维模型中,它似乎能够与恒定区的半胱氨酸-171形成结构域间二硫键。第二个b9克隆的部分序列同时编码半胱氨酸-80和半胱氨酸-108;该克隆的翻译产物可能有一个游离的反应性巯基,这可能导致不稳定的无功能Ig分子。如果相当一部分基因产物有一个游离的巯基,那么带有b9κ链的前B细胞不能以与其他同种异型相当的频率分化并扩展为产生有功能的Ig的细胞这一事实就可以得到解释。我们的序列结果表明,在分化产生b9同种异型κ轻链的细胞中,半胱氨酸的数量和位置会影响免疫球蛋白的表达。

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