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VH基因片段的差异使用由顺式元件介导。

Differential usage of VH gene segments is mediated by cis elements.

作者信息

Yu C C, Larijani M, Miljanic I N, Wu G E

机构信息

The Hooper Foundation, San Francisco, CA 94143, USA.

出版信息

J Immunol. 1998 Oct 1;161(7):3444-54.

PMID:9759863
Abstract

Ig diversity is generated in large part by the combinatorial joining of the Ig gene segments, VH, D, and JH, that together encode the variable domain of Ig. The final Ig repertoire, however, not only reflects the diversity generated through V(D)J recombinatorial joining, but it is also the product of a number of developmental restraints and selections. To avoid such restrictions and assess the recombination potential of individual Ig gene segments, we constructed Ig heavy (H) chain microlocus plasmids, each of which contain germline coding, recombination signal, and flanking sequences of a VH, D, and JH gene segment. These plasmids allow us to assess the recombination potential of the segments in the context of their natural flanking DNA sequences, but in the absence of any higher order chromatin structure or cellular selection. We found that the frequency and extent of deletions and additions at the recombination breakpoints are similar to those observed at rearranged Ig H chain loci in intact animals. The relative frequencies of the types of rearrangements--VD-J, V-DJ, VinvD-J (invD = inverted D), and VDJ--however, differ strongly. Moreover, V81x, the most used VH gene segment in intact mice, also is overused in this plasmid assay, 15 to 30 times that of another VH segment. This result indicates that the overuse of V81x in the early B cell repertoire can be a consequence of its DNA sequence and not of cellular activities.

摘要

Ig多样性在很大程度上是由Ig基因片段VH、D和JH的组合连接产生的,这些片段共同编码Ig的可变结构域。然而,最终的Ig库不仅反映了通过V(D)J重组连接产生的多样性,它也是多种发育限制和选择的产物。为了避免此类限制并评估单个Ig基因片段的重组潜力,我们构建了Ig重链(H)链微基因座质粒,每个质粒都包含一个VH、D和JH基因片段的种系编码、重组信号及侧翼序列。这些质粒使我们能够在其天然侧翼DNA序列的背景下评估各片段的重组潜力,但不存在任何高级染色质结构或细胞选择。我们发现,重组断点处缺失和添加的频率及程度与在完整动物中重排的Ig H链基因座处观察到的情况相似。然而,各种重排类型——VD-J、V-DJ、VinvD-J(invD = 反向D)和VDJ——的相对频率差异很大。此外,V81x是完整小鼠中使用最多的VH基因片段,在该质粒检测中也被过度使用,是另一个VH片段的15至30倍。这一结果表明,早期B细胞库中V81x的过度使用可能是其DNA序列的结果,而非细胞活动的结果。

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