Gene polymorphisms of TNF-238G/A, TNF-308G/A, IL10-1082G/A, TNFAIP3, and MC4R and comorbidity occurrence in a Romanian population with psoriasis • JML Journal of Medicine and Life

2018, Volume 11, Issue 1, pp 69 – 74

Gene polymorphisms of TNF-238G/A, TNF-308G/A, IL10-1082G/A, TNFAIP3, and MC4R and comorbidity occurrence in a Romanian population with psoriasis

Issues

Special Issues

Authors and Affiliations

Voiculescu Vlad Mihai ^{* **}

Solomon Iulia ^**

Popa Alexandra ^**

Draghici Carmen Cristina ^**

Dobre Maria ^***

Giurcaneanu Calin ^{* **}

Papagheorghe Laura Maria Lucia ^****

Lupu Mihai ^*****

* *Discipline of Clinical Dermatology and Allergology, „Carol Davila” University of Medicine and Pharmacy, Bucharest

** **Dermatology Department, „Elias” University Emergency Hospital, Bucharest

*** ***„Victor Babeș” National Research Institute, Bucharest

**** ****Dermatology Ambulatory Center, „Colțea” Clinical Hospital, Bucharest

***** *****Department of Dermatology, MEDAS Medical Center, Bucharest

Correspondence to:Voiculescu VM “Carol Davila” University of Medicine and Pharmacy, 8 Eroilor Sanitari Blvd., District 5, code 050474, Bucharest, Romania; Phone: +40.21318.0762, E-mail: voiculescuvlad@yahoo.com

Abstract

Rationale.Psoriasis is a prevalent chronic inflammatory disease with worldwide distribution affecting approximately 2% of the Caucasian population. There have been many population- and family-based studies that agree on the strong genetic component of this disease. Several studies have investigated the relationship between cytokine gene polymorphisms, psoriasis, and the occurrence of comorbidities but their data are conflicting.

Objective.This study examines cytokine gene single-nucleotide polymorphisms (SNPs) in the context of psoriasis and metabolic syndrome, with a focus on the occurrence of comorbidities in psoriasis patients. The working hypothesis is that particular SNPs may predispose to an accelerated disease course and more comorbidities in psoriasis patients.

Methods:This cross-sectional study was carried out in 2016 in the Dermatology Department of “Elias” University Emergency Hospital, Bucharest and included 82 psoriasis patients. Several clinical and laboratory parameters were recorded, and the presence of metabolic syndrome (MetS) was noted. Using real-time PCR, we tested for the following SNPs: rs361525, rs1800629, rs1800896, rs610604, rs17782313.

Results:Disease severity was not significantly influenced by any of the five studied SNPs. Gene polymorphism of rs17782313 was found to influence the occurrence of psoriatic arthritis. In these patients, rs610604 and rs17782313 polymorphisms were associated with the presence of diabetes mellitus. Furthermore, rs17782313 influenced the presence of obesity, heterozygotes being more at risk. Our data suggested that MetS occurred independently of the five studied SNPs.

Discussion.The influence of certain cytokine gene polymorphisms on multiple organ systems is justification enough for further analysis of the genetic and molecular mechanisms of metabolic syndrome development in psoriasis patients.

Abbreviations:single-nucleotide polymorphisms – SNPs, metabolic syndrome – MetS

Keywords

Metabolic SyndromePolymorphismSingle NucleotidePsoriasisComorbidityCytokines

Preview

JMedLife-11-69

Download PDF

About this article

PMC ID: 5909949
PubMed ID: 29696068
DOI:

Article Publishing Date (print): Jan-Mar 2018
Available Online:

Journal information

ISSN Printing: 1844-122X
ISSN Online: 1844-3117
Journal Title: Journal of Medicine and Life

Copyright License: Open Access

This article is distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use and redistribution provided that the original author and source are credited.