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JH近端VH基因的偏向性表达出现在新生小鼠和成年小鼠新产生的抗体库中。

Biased expression of JH-proximal VH genes occurs in the newly generated repertoire of neonatal and adult mice.

作者信息

Malynn B A, Yancopoulos G D, Barth J E, Bona C A, Alt F W

机构信息

Howard Hughes Medical Institute, Department of Biochemistry, College of Physicians and Surgeons, Columbia University, New York, New York 10032.

出版信息

J Exp Med. 1990 Mar 1;171(3):843-59. doi: 10.1084/jem.171.3.843.

Abstract

We have previously demonstrated a dramatic preference for utilization of the most JH-proximal VH gene segments in the newborn liver versus adult spleen. We now examine in detail the relative expression of different VH gene families throughout ontogeny and in immunodeficient mice to gain insight into factors that cause the shift in VH usage. We find that the relative expression of VH gene families remains constant and biased throughout fetal and neonatal liver development. In addition, the primary VH repertoire expressed in neonatal spleen displays a similarly biased, position-dependent VH repertoire. The pattern of VH gene expression begins to change at 5-7 d postnatally and reaches the adult randomized pattern at approximately 2 wk of age. We also find biased expression of JH-proximal VH gene families in adult bone marrow and in spleens of adult leaky scid mice, suggesting that the spontaneously generated repertoire of adult mice is similar to that observed in neonates. Together, these data suggest that a position-dependent repertoire is generated in differentiating pre-B cells at all stages of ontogeny, at least in part, as a result of preferential rearrangement of proximal VH gene segments. Therefore, mechanisms subsequent to V gene rearrangement, such as regulatory interactions and antigen selection, must play a major role in normalizing the repertoire.

摘要

我们之前已经证明,与成年脾脏相比,新生肝脏对利用最靠近连接区(JH)的重链可变区(VH)基因片段具有显著偏好。我们现在详细研究不同VH基因家族在个体发育过程中以及免疫缺陷小鼠中的相对表达情况,以深入了解导致VH使用发生变化的因素。我们发现,在胎儿和新生肝脏发育过程中,VH基因家族的相对表达保持恒定且存在偏向性。此外,新生脾脏中表达的主要VH库也显示出类似的偏向性、位置依赖性VH库。VH基因表达模式在出生后5 - 7天开始变化,并在大约2周龄时达到成年随机模式。我们还在成年骨髓和成年渗漏型重症联合免疫缺陷(leaky scid)小鼠的脾脏中发现了靠近连接区(JH)的VH基因家族的偏向性表达,这表明成年小鼠自发产生的库与在新生儿中观察到的相似。总之,这些数据表明,在个体发育的所有阶段,至少部分是由于近端VH基因片段的优先重排,在分化的前B细胞中产生了位置依赖性库。因此,V基因重排后的机制,如调节相互作用和抗原选择,必定在使库正常化方面发挥主要作用。

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