Iraj Shahramian
1 , Hossein Shahdadi
2, Ali Bazi
3, 4* , Nosratollah Masinaeinejad
3, Mojtaba Delaramnasab
3, 41 Pediatric Ward, Amir-Al-Momenin Hospital, Zabol University of Medical Sciences, Zabol, Iran
2 Faculty of Nursing, Zabol University of Medical Sciences, Zabol, Iran
3 Faculty of Allied Medical Sciences, Zabol University of Medical Sciences, Zabol, Iran
4 Clinical Research Development Unit, Amir-Al-Momenin Hospital, Zabol University of Medical Sciences, Zabol, Iran
Abstract
Although extensive studies have been performed to explore the role of various alleles within the
human leukocyte antigen (HLA) in susceptibility to coeliac disease (CD) and type 1 diabetes
(T1D), less attention has been dedicated to the role of shred non-HLA loci. In the present report,
we have provided a review on the role of genetic variants in seven shared non-HLA loci in
determining the risk of either CD or T1D. The literature search was done on the Web of Knowledge,
PubMed, and Scopus databases using keywords of polymorphism, coeliac disease, and type 1
diabetes. The literature published within 2000-2017 were recruited. Seven discussed shared loci
between CD and T1D were those resided within cytotoxic T-lymphocyte associated protein 4
(CTL4), regulator of G protein signaling (RGS1), SH2B adaptor protein (SH2B3), T cell activation
Rho GTPase activating protein (TAGAP), interleukin 18 receptor accessory protein (IL18RAP),
protein tyrosine phosphatase, non-receptor type (PTPN2), and C-C motif chemokine receptor
(CCR5). The interaction between polymorphisms of these genes seems to exert a substantial
impact on determining the risk of CD and T1D in context of each other. Polymorphisms residing
in these loci can exert synergistic or opposing effects toward either protection or predisposition
to CD and T1D. The majority of these polymorphisms affect the function of cytokine signaling
or T cell activating pathways. The net outcome deems to be delineated by a complex interaction
between these adaptor arms, as well as the modulatory effects of other components of immune
system, in particular, HLA alleles.
Keywords: Coeliac disease, Type 1 diabetes, Single nucleotide polymorphism, Human leukocyte antigen