Midfacial toddler excoriation syndrome (MiTES): case series, diagnostic criteria and evidence for a pathogenic mechanism.

IF 11 1区 医学 Q1 DERMATOLOGY
Nivedita Sarveswaran, Yunisa Pamela, Akhila A N Reddy, Akash P Mustari, Anchala Parthasarathi, Anthony J Mancini, Anuradha Bishnoi, Arun C Inamadar, Bayanne Olabi, Fiona Browne, Gargi N Deshmukh, Kenneth McWilliam, Keshavamurthy Vinay, Sahana Srinivas, Samantha Ibbs, Sivakumar Natarajan, Vadlamudi R Rao, Vijay Zawar, Vykuntaraju K Gowda, Samiha S Shaikh, Celia Moss, Christopher G Woods, Ichrak Drissi
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引用次数: 0

Abstract

Background: PRDM12 polyalanine tract expansions cause two different disorders: midfacial toddler excoriation syndrome (MiTES; itch with normal pain sensation associated with 18 homozygous alanines (18A); and congenital insensitivity to pain (CIP) with normal itch associated with 19 homozygous alanines (19A). Knowledge of the phenotype, genotype and disease mechanism of MiTES is incomplete. Why 18A vs. 19A PRDM12 can cause almost opposite phenotypes is unknown; no other polyalanine or polyglutamine tract expansion disease causes two such disparate phenotypes.

Objectives: To assess the genotype and phenotype of nine new, nine atypical and six previously reported patients diagnosed with MiTES.

Methods: Using cell lines with homozygous PR domain zinc finger protein 12 (PRDM12) containing 12 alanines (12A; normal), 18A (MiTES) and 19A (CIP), we examined PRDM12 aggregation and subcellular localization by image-separation confocal microscopy and subcellular fractionation Western blotting.

Results: MiTES presents in the first year of life; in all cases the condition regresses over the first decade, leaving scarring. The MiTES phenotype is highly distinctive. Features overlapping with PRDM12 CIP are rarely found. The genotype-phenotype study of the PRDM12 polyalanine tract shows that having 7-15 alanines is normal; 16-18 alanines is associated with MiTES; 19 alanines leads to CIP; and no clinically atypical cases of MiTES had a polyalanine tract expansion. PRDM12 aggregation and subcellular localization differed significantly between 18A and normal 12A cell lines and between 18A and 19A cell lines. MiTES is a new protein-aggregation disease.

Conclusions: We provide diagnostic criteria for MiTES and improved longitudinal data. MiTES and CIP are distinct phenotypes, despite their genotypes varying by a single alanine in the PRDM12 polyalanine tract. We found clear distinctions between the cellular phenotypes of normal, MiTES and CIP cells. We hypothesize that the developmental environment of the trigeminal ganglion is unique and critically sensitive to pre- and postnatal levels of PRDM12.

面中部幼儿剥脱综合征(MiTES):病例系列、诊断标准和致病机制证据。
背景:PRDM12多丙氨酸束扩张会导致两种不同的疾病:中面部幼儿搔痒综合征(MiTES)--同型18丙氨酸(18A)伴有正常痛觉的痒,以及同型19A伴有正常痒的先天性痛觉不敏感(CIP)。对 MiTES 的表型、基因型和疾病机制的了解还不全面。为什么 PRDM12 18A 与 19A 可导致几乎相反的表型,目前尚不清楚;没有其他多丙氨酸或多谷氨酰胺道扩增疾病会导致两种如此不同的表型:我们评估了 9 例新诊断出的 MiTES 患者、9 例非典型患者和 6 例先前报告过的患者的基因型和表型。我们使用12A(正常)、18A(MiTES)和19A(CIP)的同基因PRDM12细胞系,通过图像分离共聚焦显微镜和亚细胞分馏Western印迹检查了PRDM12的聚集和亚细胞定位:结果:MiTES 在婴儿出生后第一年发病,所有病例都会在出生后十年内消退,留下疤痕。MiTES 的表型非常独特。很少发现与 PRDM12-CIP 重叠的特征。对 PRDM12 多丙氨酸束的基因型-表型研究显示,7A -15A 正常;16A -18A 与 MiTES 相关;19A 导致 CIP;临床上没有非典型 MiTES 病例出现扩增。18A 和正常 12A 细胞系之间以及 18A 和 19A 细胞系之间的 PRDM12 聚集和亚细胞定位存在显著差异。MiTES是一种新的蛋白质聚集性疾病:我们提供了 MiTES 的诊断标准,并改进了纵向数据。尽管 MiTES 和 CIP 的基因型在 PRDM12 多丙氨酸道上只有一个丙氨酸的差异,但它们的表型却截然不同。我们发现正常细胞、MiTES 细胞和 CIP 细胞的细胞表型有明显区别。我们假设三叉神经节的发育环境是独特的,并且对出生前和出生后的 PRDM12 水平非常敏感。
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来源期刊
British Journal of Dermatology
British Journal of Dermatology 医学-皮肤病学
CiteScore
16.30
自引率
3.90%
发文量
1062
审稿时长
2-4 weeks
期刊介绍: The British Journal of Dermatology (BJD) is committed to publishing the highest quality dermatological research. Through its publications, the journal seeks to advance the understanding, management, and treatment of skin diseases, ultimately aiming to improve patient outcomes.
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