Papillon-Lefèvre syndrome (PLS) with novel compound heterozygous mutation in the exclusion and Peptidase C1A domains of Cathepsin C gene.


Journal

Molecular biology reports
ISSN: 1573-4978
Titre abrégé: Mol Biol Rep
Pays: Netherlands
ID NLM: 0403234

Informations de publication

Date de publication:
Jul 2020
Historique:
received: 29 04 2020
accepted: 22 06 2020
revised: 13 06 2020
pubmed: 1 7 2020
medline: 8 6 2021
entrez: 1 7 2020
Statut: ppublish

Résumé

Papillon Lefevre syndrome (PLS) manifests with palmoplantar keratoderma, combined with a rapidly progressive periodontitis associated with mutations in Cathepsin C (CTSC) gene. This article reports a 15-year old male proband with typical PLS traits having a novel compound heterozygote with p.Q49X mutation in exon 1 and p.Y259C missense mutation in exon 6 of CTSC gene respectively. The exon 1 mutation, p.Q49X, (found in proband's mother) was located in exclusion domain and exon 6 mutation, p.Y259C (found in proband's father), was present in peptidase C1A, papain C-terminal domain. Interestingly, missense mutation p.Y259C identified in this study was found to be not reported so far. Upon computational analysis, this missense mutation was found to be lethal. Moreover, our protein modelling approach using mutant protein revealed the presence of monomeric structure on contrary to the tetrameric structure of the wild type protein. In addition, in vitro functional characterization of mutant p.Y259C expressed in HEK293 cells showed a significant reduction in CTSC activity (0.015 ± 0.009 mU/ml) when compared with wild type protein (0.21 ± 0.008 mU/ml). Thus, in this study, we have demonstrated that the pathogenic missense mutant p.Y259C might cause PLS by impaired CTSC function.

Identifiants

pubmed: 32601924
doi: 10.1007/s11033-020-05622-0
pii: 10.1007/s11033-020-05622-0
doi:

Substances chimiques

CTSC protein, human EC 3.4.14.1
Cathepsin C EC 3.4.14.1

Types de publication

Case Reports Journal Article

Langues

eng

Sous-ensembles de citation

IM

Pagination

5681-5687

Auteurs

S Meenu (S)

PSG Center for Molecular Medicine & Therapeutics, PSG Institute of Medical Sciences and Research, Coimbatore, Tamil Nadu, 641 004, India.

B Pradeep (B)

Department of Dermatology, PSG Institute of Medical Sciences and Research (Affiliated to the Tamil Nadu Dr MGR Medical University, Coimbatore, Tamil Nadu, India), Coimbatore, Tamil Nadu, India.

Sudha Ramalingam (S)

PSG Center for Molecular Medicine & Therapeutics, PSG Institute of Medical Sciences and Research, Coimbatore, Tamil Nadu, 641 004, India.

Thiagarajan Sairam (T)

PSG Center for Molecular Medicine & Therapeutics, PSG Institute of Medical Sciences and Research, Coimbatore, Tamil Nadu, 641 004, India. thiagarajan.sairam@gmail.com.
Academic Research Consultant (Molecular Biology), Coimbatore, Tamil Nadu, India. thiagarajan.sairam@gmail.com.

Reena Rai (R)

Department of Dermatology, PSG Institute of Medical Sciences and Research (Affiliated to the Tamil Nadu Dr MGR Medical University, Coimbatore, Tamil Nadu, India), Coimbatore, Tamil Nadu, India. drreena_rai@yahoo.co.in.
Department of Dermatology, PSG Institute of Medical Sciences and Research, Off Avanashi Road, Peelamedu, 641 004, Coimbatore, Tamil Nadu, India. drreena_rai@yahoo.co.in.

Ramalingam Sankaran (R)

PSG Center for Molecular Medicine & Therapeutics, PSG Institute of Medical Sciences and Research, Coimbatore, Tamil Nadu, 641 004, India. drrampsg@gmail.com.

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