Literature DB >> 21505366

Amerindian mtDNA haplogroups and celiac disease risk HLA haplotypes in mixed-blood Latin American patients.

Alejandra Parada1, Magdalena Araya, Francisco Pérez-Bravo, Marco Méndez, Adriana Mimbacas, Patricia Motta, Graciela Martín, Gabriela Martín, Jorge Botero, Nelly Espinosa, Teresa Alarcon, Paulina Canales.   

Abstract

BACKGROUND AND
OBJECTIVE: Risk haplotypes have been described in celiac disease (CD), but the influence of native genes on CD in Hispanic Americans is unknown. The aim of the study was to measure the frequency of Amerindian mitochondrial DNA (mtDNA) haplogroups (inherited by the maternal line) in mixed-blood patients with CD from Chile, Argentina, and Uruguay, and to assess the relation between these and human leukocyte antigen (HLA) alleles and haplotypes and clinical presentations. PATIENTS AND METHODS: Clinical history, histological data, and genetic studies were conducted following 2 protocols: a case-control study of 72 Chilean patients with CD and controls, and an assessment of 43 (additional) samples of celiac patients from Chile, 96 from Argentina, and 57 from Uruguay, compared with the mtDNA frequency in the corresponding country. HLA typing was performed by a commercial kit, and mtDNA was determined by means of polymerase chain reaction and restriction fragment length polymorphisms analysis.
RESULTS: A total of 73.6% of cases had typical presentations. The most frequent HLA alleles were HLA-DQB*201 and 202. No-DQ2/DQ8 HLA haplotypes were found in 7% of cases. mtDNA frequencies for typical Amerindian haplogroups were found in 71% of cases and 64% of controls (P χ2 = 0.016); in the comparative analysis, mtDNA distribution was not different from the figures reported for the respective general country population. No relation was found between haplotypes or haplogroups and clinical presentations.
CONCLUSIONS: mtDNA haplogroups A/B/C/D were frequently found in celiac patients and controls, but no relations appeared between haplogroups, haplotypes, and clinical presentations.

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Year:  2011        PMID: 21505366     DOI: 10.1097/MPG.0b013e31821de3fc

Source DB:  PubMed          Journal:  J Pediatr Gastroenterol Nutr        ISSN: 0277-2116            Impact factor:   2.839


  6 in total

1.  Sex and racial disparities in duodenal biopsy to evaluate for celiac disease.

Authors:  Benjamin Lebwohl; Christina A Tennyson; Jennifer L Holub; David A Lieberman; Alfred I Neugut; Peter H R Green
Journal:  Gastrointest Endosc       Date:  2012-06-23       Impact factor: 9.427

2.  Prevalence of celiac disease and celiac autoimmunity in the Toba Native Amerindian community of Argentina.

Authors:  Horacio Vázquez; María de la Paz Temprano; Emilia Sugai; Stella M Scacchi; Cecilia Souza; Daniel Cisterna; Edgardo Smecuol; María Laura Moreno; Gabriela Longarini; Roberto Mazure; María A Bartellini; Elena F Verdú; Andrea González; Eduardo Mauriño; Julio Bai
Journal:  Can J Gastroenterol Hepatol       Date:  2015-07-24

3.  DQ2, DQ7 and DQ8 Distribution and Clinical Manifestations in Celiac Cases and Their First-Degree Relatives.

Authors:  Magdalena Araya; Amaya Oyarzun; Yalda Lucero; Nelly Espinosa; Francisco Pérez-Bravo
Journal:  Nutrients       Date:  2015-06-18       Impact factor: 5.717

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Journal:  PLoS One       Date:  2015-05-05       Impact factor: 3.240

5.  Changes in Age at Diagnosis and Nutritional Course of Celiac Disease in the Last Two Decades.

Authors:  Mónica Villanueva; Amaya Oyarzún; Bárbara Leyton; Mónica González; Elizabeth Navarro; Paulina Canales; Cristobal Ossa; María Paz Muñoz; Karla A Bascuñán; Magdalena Araya
Journal:  Nutrients       Date:  2020-01-06       Impact factor: 5.717

6.  Epidemiological, clinical, and histological presentation of celiac disease in Northwest China.

Authors:  Man Wang; Wen-Jie Kong; Yan Feng; Jia-Jie Lu; Wen-Jia Hui; Wei-Dong Liu; Zi-Qiong Li; Tian Shi; Mei Cui; Zhen-Zhu Sun; Feng Gao
Journal:  World J Gastroenterol       Date:  2022-03-28       Impact factor: 5.742

  6 in total

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