Midfacial toddler excoriation syndrome (MiTES): case series, diagnostic criteria and evidence for a pathogenic mechanism-Reference-Cited by-同舟云学术

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

Published:2024-04-09 Issue:3 Volume:191 Page:437-446
ISSN:0007-0963
Container-title:British Journal of Dermatology
language:en
Short-container-title:

Author:

Sarveswaran Nivedita¹,Pamela Yunisa¹²,Reddy Akhila A N³,Mustari Akash P⁴^ORCID,Parthasarathi Anchala³,Mancini Anthony J⁵,Bishnoi Anuradha⁴,Inamadar Arun C⁶,Olabi Bayanne⁷,Browne Fiona⁸,Deshmukh Gargi N⁹,McWilliam Kenneth¹⁰,Vinay Keshavamurthy⁴,Srinivas Sahana¹¹,Ibbs Samantha¹²,Natarajan Sivakumar¹³,Rao Vadlamudi R⁹,Zawar Vijay¹⁴,Gowda Vykuntaraju K¹⁵,Shaikh Samiha S¹,Moss Celia¹²¹⁶^ORCID,Woods Christopher G¹,Drissi Ichrak¹

Affiliation:

1. Cambridge Institute for Medical Research, University of Cambridge , Cambridge , UK

2. Department of Biomedical Sciences, Faculty of Medicine, Universitas Padjadjaran , Bandung , Indonesia

3. Dr. Anchala Skin Institute and Research Center , Hyderabad , India

4. Department of Dermatology, Venereology and Leprology, Postgraduate Institute of Medical Education and Research , Chandigarh , India

5. Division of Dermatology, Department of Pediatrics, Ann & Robert H. Lurie Children’s Hospital of Chicago, Northwestern University Feinberg School of Medicine , Chicago, IL , USA

6. Department of Dermatology, Shri BM Patil Medical College & Hospital, BLDE University , Bijapur , India

7. Department of Dermatology, Edinburgh Royal Infirmary , UK

8. Department of Paediatric Dermatology, Children’s Health Ireland (CHI) at Crumlin , Crumlin , Ireland

9. Genome Foundation , Hyderabad , India

10. Paediatric Neurology, Neurosciences Department, Royal Hospital for Children and Young People , Edinburgh , UK

11. Department of Pediatric Dermatology, Indira Gandhi Institute of Child Health , Bangalore , India

12. Department of Paediatric Dermatology, Birmingham Children’s Women’s and Children’s NHS Foundation Trust , Birmingham , UK

13. The Newcastle Upon Tyne Hospitals NHS Foundation Trust , UK

14. Department of Dermatology, Dr. Vasantrao Pawar Medical College and Research Center , Nashik , India

15. Department of Pediatric Neurology, Indira Gandhi Institute of Child Health , Bangalore, Karnataka , India

16. College of Medical and Dental Sciences, University of Birmingham , Birmingham , UK

Abstract

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.

Funder

MRC CASE studentship with AstraZeneca

Indonesian Endowment Fund for Education

Ministry of Finance of Republic of Indonesia

Wellcome Trust

National Institute for Health and Care Research

Cambridge Biomedical Research Centre

Department of Health and Social Care

Publisher

Oxford University Press (OUP)

Link

https://academic.oup.com/bjd/advance-article-pdf/doi/10.1093/bjd/ljae151/57955022/ljae151.pdf