白细胞 CBL 杂合子缺失患者的自身炎症是由组成型 ERK 介导的单核细胞活化引起的。

Jonathan Bohlen,Ivan Bagarić,Taja Vatovec,Masato Ogishi,Syed F Ahmed,Axel Cederholm,Lori Buetow,Steicy Sobrino,Corentin Le Floc'h,Carlos A Arango-Franco,Luis Seabra,Marine Michelet,Federica Barzaghi,Davide Leardini,Francesco Saettini,Francesca Vendemini,Francesco Baccelli,Albert Catala,Eleonora Gambineri,Marinella Veltroni,Yurena Aguilar de la Red,Gillian I Rice,Filippo Consonni,Laureline Berteloot,Laetitia Largeaud,Francesca Conti,Cécile Roullion,Cécile Masson,Boris Bessot,Yoann Seeleuthner,Tom Le Voyer,Darawan Rinchai,Jérémie Rosain,Anna-Lena Neehus,Lucia Erazo-Borrás,Hailun Li,Zarah Janda,En-Jui Cho,Edoardo Muratore,Camille Soudée,Candice Lainé,Eric Delabesse,Claire Goulvestre,Cindy S Ma,Anne Puel,Stuart G Tangye,Isabelle André,Christine Bole-Feysot,Laurent Abel,Miriam Erlacher,Shen-Ying Zhang,Vivien Béziat,Chantal Lagresle-Peyrou,Emmanuelle Six,Marlène Pasquet,Laia Alsina,Alessandro Aiuti,Peng Zhang,Yanick J Crow,Nils Landegren,Riccardo Masetti,Danny T Huang,Jean-Laurent Casanova,Jacinta Bustamante
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引用次数: 0

摘要

种系CBL功能缺失(LOF)变体的杂合子患者,如果其部分或全部白细胞通过单亲同源异位切除术发生体细胞杂合子缺失(LOH)而成为这些变体的同源变体,就会患上髓系恶性肿瘤、自身炎症或两者兼而有之。我们在这些患者的全血中观察到炎症基因表达特征的上调,模拟了自身炎症的单基因先天性错误。值得注意的是,与健康人和无 LOH 的 CBL LOF 杂合子相比,这些患者的构成性活化单核细胞分泌的炎症细胞因子要多 10 到 100 倍。CBL-LOH 造血干细胞和祖细胞(HSPCs)超越了其他细胞,这就是CBL LOF变体同源的外周单核细胞持续存在的原因。正如在单核细胞系中所显示的,静息和受刺激的 CBL-LOF 单核细胞都需要激活 ERK 通路,才能产生过多的细胞因子。最后,我们发现英国生物库中每一万人中就有一人是CBL LOF变体的杂合子,这些携带者患血液病和炎症的风险很高。
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Autoinflammation in patients with leukocytic CBL loss of heterozygosity is caused by constitutive ERK-mediated monocyte activation.
Patients heterozygous for germline CBL loss-of-function (LOF) variants can develop myeloid malignancy, autoinflammation, or both, if some or all of their leukocytes become homozygous for these variants through somatic loss of heterozygosity (LOH) via uniparental isodisomy. We observed an upregulation of the inflammatory gene expression signature in whole blood from these patients, mimicking monogenic inborn errors underlying autoinflammation. Remarkably, these patients had constitutively activated monocytes that secreted 10 to 100 times more inflammatory cytokines than those of healthy individuals and CBL LOF heterozygotes without LOH. CBL-LOH hematopoietic stem and progenitor cells (HSPCs) outgrew the other cells, accounting for the persistence of peripheral monocytes homozygous for the CBL LOF variant. ERK pathway activation was required for the excessive production of cytokines by both resting and stimulated CBL-LOF monocytes, as shown in monocytic cell lines. Finally, we found that about 1 in 10,000 individuals in the UK Biobank were heterozygous for CBL LOF variants and that these carriers were at high risk of hematological and inflammatory conditions.
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