HSP110 通过稳定 MyD88 维持激活 B 细胞弥漫大 B 细胞淋巴瘤中的慢性 NF-κB 信号传导。
HSP110 sustains chronic NF-κB signaling in activated B-cell diffuse large B-cell lymphoma through MyD88 stabilization.
机构信息
INSERM, LNC Unité Mixte de Recherche (UMR) 1231, Equipe Labellisée Ligue Nationale Contre le Cancer, Dijon, France.
Faculté des sciences de santé, Université Bourgogne Franche-Comté, Dijon, France.
出版信息
Blood. 2018 Aug 2;132(5):510-520. doi: 10.1182/blood-2017-12-819706. Epub 2018 Jun 5.
Activated B-cell diffuse large B-cell lymphoma (ABC-DLBCL) is an aggressive lymphoproliferative disorder involving chronic NF-κB activation. Several mutations in the BCR and MyD88 signaling pathway components, such as MyD88 L265P, are implicated in this aberrant activation. Among heat shock proteins, HSP110 has recently been identified as a prosurvival and/or proliferation factor in many cancers, but its role in ABC-DLBCL survival mechanisms remained to be established. We observed that short hairpin RNA-mediated HSP110 silencing decreased the survival of several ABC-DLBCL cell lines and decreased immunoglobulin M-MyD88 co-localization and subsequent NF-κB signaling. Conversely, overexpression of HSP110 in ABC-DLBCL or non-DLBCL cell lines increased NF-κB signaling, indicating a tight interplay between HSP110 and the NF-κB pathway. By using immunoprecipitation and proximity ligation assays, we identified an interaction between HSP110 and both wild-type MyD88 and MyD88 L265P. HSP110 stabilized both MyD88 forms with a stronger effect on MyD88 L265P, thus facilitating chronic NF-κB activation. Finally, HSP110 expression was higher in lymph node biopsies from patients with ABC-DLBCL than in normal reactive lymph nodes, and a strong correlation was found between the level of HSP110 and MyD88. In conclusion, we identified HSP110 as a regulator of NF-κB signaling through MyD88 stabilization in ABC-DLBCL. This finding reveals HSP110 as a new potential therapeutic target in ABC-DLBCL.
活化 B 细胞弥漫性大 B 细胞淋巴瘤(ABC-DLBCL)是一种涉及慢性 NF-κB 激活的侵袭性淋巴增生性疾病。BCR 和 MyD88 信号通路成分中的几种突变,如 MyD88 L265P,与这种异常激活有关。在热休克蛋白中,HSP110 最近被确定为许多癌症中的生存和/或增殖因子,但它在 ABC-DLBCL 生存机制中的作用仍有待确定。我们观察到,短发夹 RNA 介导的 HSP110 沉默降低了几种 ABC-DLBCL 细胞系的存活率,并减少了免疫球蛋白 M-MyD88 共定位和随后的 NF-κB 信号转导。相反,在 ABC-DLBCL 或非-DLBCL 细胞系中过表达 HSP110 增加了 NF-κB 信号转导,表明 HSP110 和 NF-κB 通路之间存在紧密的相互作用。通过使用免疫沉淀和邻近连接测定,我们鉴定出 HSP110 与野生型 MyD88 和 MyD88 L265P 之间存在相互作用。HSP110 稳定了两种 MyD88 形式,对 MyD88 L265P 的稳定作用更强,从而促进了慢性 NF-κB 激活。最后,与正常反应性淋巴结相比,HSP110 在 ABC-DLBCL 患者的淋巴结活检组织中表达更高,并且发现 HSP110 水平与 MyD88 之间存在很强的相关性。总之,我们确定 HSP110 通过稳定 MyD88 成为 ABC-DLBCL 中 NF-κB 信号转导的调节剂。这一发现表明 HSP110 是 ABC-DLBCL 的一个新的潜在治疗靶点。
Zotero 插件