Increased IgD and CD27 Double Negative (DN) B cell population in pediatric onset autoimmune hepatitis.

IF 3.3 4区医学 Q3 IMMUNOLOGY Autoimmunity Pub Date : 2024-12-01 Epub Date: 2024-05-21 DOI:10.1080/08916934.2024.2356089

Vasantha L Kolachala, Chungwen Wei, Suresh Venkateswaran, Aisha Latrece Hill, Vivian Warren, Hillary Espinoza, Iñaki Sanz, Nitika A Gupta

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Abstract

Autoimmune hepatitis (AIH) is a chronic, inflammatory liver disease of unknown aetiology which requires lifelong immunosuppression. Most therapeutic and outcome studies of AIH have been conducted predominantly in Caucasian (European Ancestry, EA) cohorts, with the exclusion of African American (AA) patients due to inadequate sample size. It is known that AA patients have a severe phenotype of autoimmune diseases and demonstrate a poor response to conventional medical therapy. Understanding cellular and molecular pathways which determine AIH severity and progression in AA patients is likely to lead to the discovery of novel, personalised and better tolerated therapies. The aim of the study is to determine the distinct effector B cell phenotypes which contribute to disease severity and progression of AIH in AA children as compared to their EA cohorts. PBMCs were isolated from blood samples collected from patients visiting Children's Healthcare of Atlanta (CHOA) and were grouped into AA, (n = 12), EA, (n = 11) and controls (n = 12) and were processed for flow cytometry. Markers of B cell development, maturation and activation were assessed namely CD19, CD21, IgD, CD27, CD38, CD11c, CD24, CD138. AA children with AIH demonstrated an expansion of CD19 + ve, Activated Naïve (aN), (CD19⁺ IgD^-/CD27^- Double Negative (DN₂) ([CD19+/IgD^-/CD27⁺⁺CD38⁺⁺) cells. Plasmablasts were significantly higher along with Signalling Lymphocytic activation molecule F7 (SLAMF7). Unswitched memory [CD19+] IgD⁺CD27⁺ (USM) B cells were significantly contracted in AA patients with AIH. B cell phenotyping reveals a distinct profile in AA AIH patients with a major skewing towards the expansion of effector pathways which have been previously characterised in severe SLE in AA patients. These results suggest that the quantification and therapeutic target of B cell pathway could contribute substantially to the clinical approach to AIH especially in the AA population.

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小儿自身免疫性肝炎中 IgD 和 CD27 双阴性 (DN) B 细胞数量增加。

自身免疫性肝炎（AIH）是一种病因不明的慢性炎症性肝病，需要终身免疫抑制。大多数关于自身免疫性肝炎的治疗和疗效研究主要是在白种人（欧洲血统，EA）队列中进行的，由于样本量不足，非裔美国人（AA）患者被排除在外。众所周知，AA 患者具有严重的自身免疫性疾病表型，对常规药物治疗反应不佳。了解决定 AA 患者 AIH 严重程度和进展的细胞和分子途径可能有助于发现新型、个性化和耐受性更好的疗法。本研究的目的是确定AA儿童与EA儿童相比，导致AIH疾病严重程度和进展的不同效应B细胞表型。研究人员从亚特兰大儿童医疗保健中心（CHOA）就诊患者的血样中分离出PBMCs，将其分为AA组（n = 12）、EA组（n = 11）和对照组（n = 12），并进行流式细胞术处理。评估了 B 细胞发育、成熟和活化的标志物，即 CD19、CD21、IgD、CD27、CD38、CD11c、CD24 和 CD138。患有AIH的AA儿童表现出CD19 + ve、活化新生（aN）、（CD19 + IgD-/CD27- 双阴性（DN2）（[CD19+/IgD-/CD27++CD38+++）细胞的扩增。浆细胞和信号淋巴细胞活化分子 F7（SLAMF7）明显增多。AIH患者的未转换记忆[CD19+] IgD+CD27+（USM）B细胞明显减少。B细胞表型显示，AA AIH患者的B细胞有一个独特的轮廓，主要偏向于效应途径的扩展，这在以前的AA患者重症系统性红斑狼疮中已被证实。这些结果表明，B细胞通路的量化和治疗目标可大大有助于AIH的临床治疗，尤其是在AA人群中。

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来源期刊

Autoimmunity 医学-免疫学

CiteScore

5.70

自引率

8.60%

发文量

审稿时长

6-12 weeks

期刊介绍： Autoimmunity is an international, peer reviewed journal that publishes articles on cell and molecular immunology, immunogenetics, molecular biology and autoimmunity. Current understanding of immunity and autoimmunity is being furthered by the progress in new molecular sciences that has recently been little short of spectacular. In addition to the basic elements and mechanisms of the immune system, Autoimmunity is interested in the cellular and molecular processes associated with systemic lupus erythematosus, rheumatoid arthritis, Sjogren syndrome, type I diabetes, multiple sclerosis and other systemic and organ-specific autoimmune disorders. The journal reflects the immunology areas where scientific progress is most rapid. It is a valuable tool to basic and translational researchers in cell biology, genetics and molecular biology of immunity and autoimmunity.