% pubman genre = article @article{item_3338839, title = {{Interaction of HLA Class II rs9272219 and TMPO rs17028450 (Arg690Cys) Variants Affects Neuromyelitis Optica Spectrum Disorder Susceptibility in an Admixed Mexican Population}}, author = {Rosas-Madrigal, Sandra and Villarreal-Molina, Mar{\'\i}a Teresa and Flores-Rivera, Jos{\'e} and Rivas-Alonso, Ver{\'o}nica and Macias-Kauffer, Luis Rodrigo and Ordo{\~n}ez, Graciela and Chima-Gal{\'a}n, Mar{\'\i}a Del Carmen and Acu{\~n}a-Alonzo, V{\'\i}ctor and Mac{\'\i}n-P{\'e}rez, Gast{\'o}n and Barquera, Rodrigo and Granados, Julio and Valle-Rios, Ricardo and Corona, Teresa and Carnevale, Alessandra and Romero-Hidalgo, Sandra}, language = {eng}, issn = {1664-8021}, doi = {10.3389/fgene.2021.647343}, publisher = {Frontiers Media}, address = {Lausanne}, year = {2021}, abstract = {{Neuromyelitis Optica Spectrum Disorder (NMOSD) is a demyelinating autoimmune disease of the central nervous system, more prevalent in individuals of non-European ancestry. Few studies have analyzed genetic risk factors in NMOSD, and HLA class II gene variation has been associated NMOSD risk in various populations including Mexicans. Thymopoietin (TMPO) has not been tested as a candidate gene for NMOSD or other autoimmune disease, however, experimental evidence suggests this gene may be involved in negative selection of autoreactive T cells and autoimmunity. We thus investigated whether the missense TMPO variant rs17028450 (Arg630Cys, frequent in Latin America) is associated with NMOSD, and whether this variant shows an interaction with HLA-class II rs9272219, previously associated with NMOSD risk. A total of 119 Mexican NMOSD patients, 1208 controls and 357 Native Mexican individuals were included. The HLA rs9272219 "T" risk allele frequency ranged from 21 to 68{\textpercent}, while the rs17028450 "T" minor allele frequency was as high as 18{\textpercent} in Native Mexican groups. Both rs9272219 and rs17028450 were significantly associated with NMOSD risk under additive models (OR {\textequals} 2.48; p {\textequals} 8 $\times$ 10(-10) and OR {\textequals} 1.59; p {\textequals} 0.0075, respectively), and a significant interaction between both variants was identified with logistic regression models (p {\textequals} 0.048). Individuals bearing both risk alleles had an estimated 3.9-fold increased risk of NMOSD. To our knowledge, this is the first study reporting an association of TMPO gene variation with an autoimmune disorder and the interaction of specific susceptibility gene variants, that may contribute to the genetic architecture of NMOSD in admixed Latin American populations.}}, journal = {{Frontiers in Genetics}}, volume = {12}, eid = {647343}, }