Histological heterogeneity in a large clinical cohort of juvenile idiopathic inflammatory myopathy: analysis by myositis autoantibody and pathological features

Yasin S. A.; Schutz P. W.; Deakin C. T.; Sag E.; Varsani H.; Simou S.; Marshall L. R.; Tansley S. L.; McHugh N. J.; Holton J. L.; Wedderburn L. R.; Jacques T. S.; the UK Juvenile Dermatomyositis Research Group (UK and Ireland); Armon Kate; Ellis‐Gage Joe; Roper Holly; Briggs Vanja; Watts Joanna; McCann Liza; Roberts Ian; Baildam Eileen; Hanna Lou; Lloyd Olivia; Wadeson Susan; Riley Phil; McGovern Ann; Ryder Clive; Scott Janis; Thomas Beverley; Southwood Taunton; Al‐Abadi Eslam; Wyatt Sue; Jackson Gillian; Amin Tania; Wood Mark; VanRooyen Vanessa; Burton Deborah; Davidson Joyce; Gardner‐Medwin Janet; Martin Neil; Ferguson Sue; Waxman Liz; Browne Michael; Friswell Mark; Foster Helen; Swift Alison; Jandial Sharmila; Stevenson Vicky; Wade Debbie; Sen Ethan; Smith Eve; Qiao Lisa; Watson Stuart; Duong Claire; Venning Helen; Satyapal Rangaraj; Stretton Elizabeth; Jordan Mary; Mosley Ellen; Frost Anna; Crate Lindsay; Warrier Kishore; ord Stefanie; Pilkington Clarissa; Hasson Nathan; Maillard Sue; Halkon Elizabeth; Brown Virginia; Juggins Audrey; Smith Sally; Lunt Sian; Enayat Elli; Kassoumeri Laura; Beard Laura; Arnold Katie; Glackin Yvonne; Simou Stephanie; Almeida Beverley; Nistala Kiran; Marques Raquel; Dowle Stefanie; Papadopoulou Charis; Johnson‐Moore Cer; Robinson Emily; Murray Kevin; Ioannou John; Suffield Linda; Al‐Obaidi Muthana; Lee Helen; Leach Sam; Smith Helen; McMahon Anne‐Marie; Chisem Heather; Kingshott Ruth; Wilkinson Nick; Inness Emma; Kendall Eunice; Mayers David; Etherton Ruth; Miller Danielle; Bailey Kathryn; Clinch Jacqui; Fineman Natalie; Pluess‐Hall Helen; Vallance Lindsay; Akeroyd Lou; Leahy Alice; Collier Amy; Cutts Rebecca; Macleod Emma; De Graaf Hans; Davidson Brian; Hartfree Sarah; Pratt Danny

首页> 外文期刊>Neuropathology and applied neurobiology >Histological heterogeneity in a large clinical cohort of juvenile idiopathic inflammatory myopathy: analysis by myositis autoantibody and pathological features

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Histological heterogeneity in a large clinical cohort of juvenile idiopathic inflammatory myopathy: analysis by myositis autoantibody and pathological features

机译：大型特发性炎症性肌病的大临床群体中的组织学异质性：肌炎自身抗体和病理特征分析

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Aim Juvenile idiopathic inflammatory myopathies have been recently reclassified into clinico‐serological subgroups. Myopathological correlates of the subgroups are incompletely understood. Methods We studied muscle biopsies from 101 children with clinically and serologically defined juvenile idiopathic inflammatory myopathies from the UK JDM Cohort and Biomarker Study by applying the international JDM score tool, myopathological review and C5b‐9 complement analysis. Results Autoantibody data were available for 90/101 cases with 18/90 cases positive for anti‐TIF1γ, 15/90 anti‐NXP2, 11/90 anti‐MDA5, 5/90 anti‐Mi2 and 6/90 anti‐PmScl. JDM biopsy severity scores were consistently low in the anti‐MDA5 group, high in the anti‐Mi2 group, and widely distributed in the other groups. Biopsies were classified histologically as perifascicular atrophy (22/101), macrophage‐rich necrosis (6/101), scattered necrosis (2/101), clustered necrosis (2/101), inflammatory fibre invasion (2/101), chronic myopathic change (1/101), diffuse endomysial macrophage infiltrates (40/101) and minimal change (24/101). MDA5 cases segregated with the minimal change group and showed no capillary C5b‐9‐deposition. The Mi2 group displayed high severity scores and a tendency towards sarcolemmal complement deposition. NXP2 and TIF1γ groups showed a variety of pathologies with a high proportion of diffuse endomysial macrophage infiltrates and a high proportion of capillary C5b‐9 deposition. Conclusion We have shown that juvenile idiopathic inflammatory myopathies have a spectrum of histopathological phenotypes and show distinct complement attack complex deposition patterns. Both correlate in some cases with the serological subtypes. Most cases do not show typical histological features associated with dermatomyositis (e.g. perifascicular atrophy). In contrast, more than half show relatively mild histopathological changes.

机译：目标幼年特发性炎症肌病已被重新分类为临床血清群。亚组的肌病理学相关性不完全理解。方法通过应用国际JDM评分工具，肌病理学综述和C5B-9补充分析，从英国JDM队列和生物标志物研究中使用临床和血清学患儿进行肌肉活组织检查。结果可用于90/101例抗TIF1γ，15/90抗NXP2,11 / 90抗MY2和6/90抗PMSC1，可自身抗体数据提供90/101患者18/90例阳性，15/90例抗NXP2，11/90抗MI2和6/90抗PMSC1。 JDM活检严重程度分数在抗MDA5组中始终低，抗MI2组高，并广泛分布在其他组中。活组织检查在组织学上分类为血糖萎缩（22/101），富噬细胞富含坏死（6/101），分散坏死（2/101），聚集坏死（2/101），炎症纤维入侵（2/101），慢性肌病变化（1/101），弥漫性子系统巨噬细胞渗透（40/101）和最小变化（24/101）。 MDA5患者与最小变化组隔离，显示出毛细管C5B-9沉积。 MI2组显示出高度严重性分数和对Sarcolemmal补充沉积的趋势。 NXP2和TIF1γ基团显示出各种具有高比例的弥漫性子宫巨噬细胞浸润性和高比例毛细管C5B-9沉积的病理学。结论我们已经表明，少年特发性炎症性肌病具有一定的组织病理学表型，并显示出明显的补体攻击复合沉积图案。在某些情况下都与血清亚型相关联。大多数病例不显示与皮肤病肌炎相关的典型组织学特征（例如血糖萎缩）。相比之下，一半以上的表现出相对温和的组织病理学变化。

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《Neuropathology and applied neurobiology》 |2019年第5期|共18页
作者
Yasin S. A.; Schutz P. W.; Deakin C. T.; Sag E.; Varsani H.; Simou S.; Marshall L. R.; Tansley S. L.; McHugh N. J.; Holton J. L.; Wedderburn L. R.; Jacques T. S.; the UK Juvenile Dermatomyositis Research Group (UK and Ireland); Armon Kate; Ellis‐Gage Joe; Roper Holly; Briggs Vanja; Watts Joanna; McCann Liza; Roberts Ian; Baildam Eileen; Hanna Lou; Lloyd Olivia; Wadeson Susan; Riley Phil; McGovern Ann; Ryder Clive; Scott Janis; Thomas Beverley; Southwood Taunton; Al‐Abadi Eslam; Wyatt Sue; Jackson Gillian; Amin Tania; Wood Mark; VanRooyen Vanessa; Burton Deborah; Davidson Joyce; Gardner‐Medwin Janet; Martin Neil; Ferguson Sue; Waxman Liz; Browne Michael; Friswell Mark; Foster Helen; Swift Alison; Jandial Sharmila; Stevenson Vicky; Wade Debbie; Sen Ethan; Smith Eve; Qiao Lisa; Watson Stuart; Duong Claire; Venning Helen; Satyapal Rangaraj; Stretton Elizabeth; Jordan Mary; Mosley Ellen; Frost Anna; Crate Lindsay; Warrier Kishore; ord Stefanie; Pilkington Clarissa; Hasson Nathan; Maillard Sue; Halkon Elizabeth; Brown Virginia; Juggins Audrey; Smith Sally; Lunt Sian; Enayat Elli; Kassoumeri Laura; Beard Laura; Arnold Katie; Glackin Yvonne; Simou Stephanie; Almeida Beverley; Nistala Kiran; Marques Raquel; Dowle Stefanie; Papadopoulou Charis; Johnson‐Moore Cer; Robinson Emily; Murray Kevin; Ioannou John; Suffield Linda; Al‐Obaidi Muthana; Lee Helen; Leach Sam; Smith Helen; McMahon Anne‐Marie; Chisem Heather; Kingshott Ruth; Wilkinson Nick; Inness Emma; Kendall Eunice; Mayers David; Etherton Ruth; Miller Danielle; Bailey Kathryn; Clinch Jacqui; Fineman Natalie; Pluess‐Hall Helen; Vallance Lindsay; Akeroyd Lou; Leahy Alice; Collier Amy; Cutts Rebecca; Macleod Emma; De Graaf Hans; Davidson Brian; Hartfree Sarah; Pratt Danny;
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作者单位

Infection Immunity Inflammation ProgrammeUCL GOS Institute of Child HealthLondon UK;

Infection Immunity Inflammation ProgrammeUCL GOS Institute of Child HealthLondon UK;

Infection Immunity Inflammation ProgrammeUCL GOS Institute of Child HealthLondon UK;

Infection Immunity Inflammation ProgrammeUCL GOS Institute of Child HealthLondon UK;

Infection Immunity Inflammation ProgrammeUCL GOS Institute of Child HealthLondon UK;

Infection Immunity Inflammation ProgrammeUCL GOS Institute of Child HealthLondon UK;

Infection Immunity Inflammation ProgrammeUCL GOS Institute of Child HealthLondon UK;

Department of Pharmacy and PharmacologyUniversity of BathBath UK;

Department of Pharmacy and PharmacologyUniversity of BathBath UK;

Department of Molecular NeuroscienceUCL Institute of NeurologyLondon UK;

Infection Immunity Inflammation ProgrammeUCL GOS Institute of Child HealthLondon UK;

Developmental Biology and Cancer ProgrammeUCL GOS Institute of Child HealthLondon UK;

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正文语种 eng
中图分类病理学;
关键词
anti‐SRP; dermatomyositis; immune mediated necrotizing myopathy; JDM score tool; polymyositis; principal component analysis;

机译：抗SRP;Dermatomyositis;免疫介导的坏死性肌病;JDM评分工具;多核;主要成分分析;

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专利

1. Histological heterogeneity in a large clinical cohort of juvenile idiopathic inflammatory myopathy: analysis by myositis autoantibody and pathological features [J] . Yasin S. A., Schutz P. W., Deakin C. T., Neuropathology and applied neurobiology . 2019,第5期

机译：大型特发性炎症性肌病的大临床群体中的组织学异质性：肌炎自身抗体和病理特征分析
2. Clinical and serological characteristics of 125 Dutch myositis patients. Myositis specific autoantibodies aid in the differential diagnosis of the idiopathic inflammatory myopathies. [J] . Hengstman GJ, Brouwer R, Egberts WT, Journal of neurology . 2002,第1期

机译：125例荷兰肌炎患者的临床和血清学特征。肌炎特异性自身抗体有助于对特发性炎症性肌病的鉴别诊断。
3. Clinical epidemiology and multidimensional analysis of idiopathic inflammatory myopathies: to a classification based on myositis specific autoantibodies [J] . Mariampillai K., Granger B., Guiguet M., Neuromuscular disorders: NMD . 2017,第Suppla2期

机译：特发性炎症性肌病的临床流行病学与多维分析：基于肌炎特异性自身抗体的分类
4. Autophagy as a link between immunity and inflammation in idiopathic inflammatory myopathies [C] . Cappelletti C., Vattemi G.N.A., Tonin P., International Congress of Immunology. . 2014

机译：自噬作为特发性炎症性肌病中免疫和炎症之间的联系
5. Defining Clinical and Autoantibody Phenotypes in Patients with Juvenile Idiopathic Inflammatory Myopathies. [D] . Shah, Mona N. 2012

机译：定义青少年特发性炎症性肌病患者的临床和自身抗体表型。
6. Histological heterogeneity in a large clinical cohort of juvenile idiopathic inflammatory myopathy: analysis by myositis autoantibody and pathological features [O] . S. A. Yasin, P. W. Schutz, C. T. Deakin, -1

机译：少年特发性炎性肌病的大型临床队列中的组织学异质性：通过肌炎自身抗体和病理特征进行分析
7. Frequency, mutual exclusivity and clinical associations of myositis autoantibodies in a combined European cohort of idiopathic inflammatory myopathy patients [O] . Z. Betteridge, S. Tansley, G. Shaddick, 2019

机译：肌炎自身抗体在欧洲成交炎症肌病患者组合群组中的频率，互联性和临床关联

Histological heterogeneity in a large clinical cohort of juvenile idiopathic inflammatory myopathy: analysis by myositis autoantibody and pathological features

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