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健康个体正常BCR库中与慢性淋巴细胞白血病相关的定型B细胞受体的存在随年龄增长而增加。

The presence of CLL-associated stereotypic B cell receptors in the normal BCR repertoire from healthy individuals increases with age.

作者信息

Muggen Alice F, de Jong Madelon, Wolvers-Tettero Ingrid L M, Kallemeijn Martine J, Teodósio Cristina, Darzentas Nikos, Stadhouders Ralph, IJspeert Hanna, van der Burg Mirjam, van IJcken Wilfred Fj, Verhaar Jan A N, Abdulahad Wayel H, Brouwer Elisabeth, Boots Annemieke M H, Hendriks Rudi W, van Dongen Jacques J M, Langerak Anton W

机构信息

1Department Immunology, Laboratory Medical Immunology, Erasmus MC, Dr. Molewaterplein 40, 3015 GD Rotterdam, The Netherlands.

2Present Address: Department Immunohematology and Blood Transfusion, Leiden University Medical Center, Leiden, The Netherlands.

出版信息

Immun Ageing. 2019 Aug 28;16:22. doi: 10.1186/s12979-019-0163-x. eCollection 2019.

Abstract

BACKGROUND

Aging is known to induce immunosenescence, resulting in alterations in both the innate and adaptive immune system. Here we evaluated the effects of aging on B cell subsets in peripheral blood of 155 immunologically healthy individuals in four age categories (range 20-95y) via multi-parameter flow cytometry. Furthermore, we studied the naive and antigen-experienced B cell receptor (BCR) repertoire of different age groups and compared it to the clonal BCR repertoire of chronic lymphocytic leukemia (CLL), a disease typically presenting in elderly individuals.

RESULTS

Total numbers and relative frequencies of B cells were found to decline upon aging, with reductions in transitional B cells, memory cell types, and plasma blasts in the 70 + y group. The BCR repertoire of naive mature B cells and antigen-experienced B cells did not clearly alter until age 70y. Clear changes in IGHV gene usage were observed in naive mature B cells of 70 + y individuals, with a transitional pattern in the 50-70y group. IGHV gene usage of naive mature B cells of the 50-70y, but not the 70 + y, age group resembled that of both younger (50-70y) and older (70 + y) CLL patients. Additionally, CLL-associated stereotypic BCR were found as part of the healthy control BCR repertoire, with an age-associated increase in frequency of several stereotypic BCR (particularly subsets #2 and #5).

CONCLUSION

Composition of the peripheral B cell compartment changes with ageing, with clear reductions in non-switched and CD27 + IgG+ switched memory B cells and plasma blasts in especially the 70 + y group. The BCR repertoire is relatively stable until 70y, whereafter differences in IGHV gene usage are seen. Upon ageing, an increasing trend in the occurrence of particular CLL-associated stereotypic BCR is observed.

摘要

背景

已知衰老会引发免疫衰老,导致固有免疫系统和适应性免疫系统均发生改变。在此,我们通过多参数流式细胞术评估了衰老对155名免疫功能正常的个体(年龄范围20 - 95岁,分为四个年龄组)外周血B细胞亚群的影响。此外,我们研究了不同年龄组的初始B细胞和抗原接触过的B细胞受体(BCR)库,并将其与慢性淋巴细胞白血病(CLL,一种典型的老年疾病)的克隆性BCR库进行比较。

结果

发现B细胞总数和相对频率随衰老而下降,在70岁及以上年龄组中,过渡性B细胞、记忆细胞类型和浆母细胞数量减少。初始成熟B细胞和抗原接触过的B细胞的BCR库在70岁之前没有明显改变。在70岁及以上个体的初始成熟B细胞中观察到IGHV基因使用的明显变化,在50 - 70岁组呈现过渡模式。50 - 70岁年龄组的初始成熟B细胞的IGHV基因使用情况与年轻(50 - 70岁)和老年(70岁及以上)CLL患者相似,但70岁及以上年龄组则不同。此外,发现与CLL相关的定型BCR是健康对照BCR库的一部分,几种定型BCR(特别是亚型#2和#5)的频率随年龄增加。

结论

外周B细胞区室的组成随年龄增长而变化,尤其是在70岁及以上年龄组中,未转换和CD27 + IgG +转换记忆B细胞以及浆母细胞明显减少。BCR库在70岁之前相对稳定,此后可观察到IGHV基因使用的差异。随着年龄增长,特定的与CLL相关的定型BCR的出现呈增加趋势。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e684/6714092/5fcd5410ee2d/12979_2019_163_Fig1_HTML.jpg

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