Identification of new genetic variants of HLA-DQB1 associated with human longevity and lipid homeostasis—a cross-sectional study in a Chinese population

نویسندگان

  • Fan Yang
  • Liang Sun
  • Xiaoquan Zhu
  • Jing Han
  • Yi Zeng
  • Chao Nie
  • Huiping Yuan
  • Xiaoling Li
  • Xiaohong Shi
  • Yige Yang
  • Caiyou Hu
  • Zeping Lv
  • Zezhi Huang
  • Chenguang Zheng
  • Siying Liang
  • Jin Huang
  • Gang Wan
  • Keyan Qi
  • Bin Qin
  • Suyan Cao
  • Xin Zhao
  • Yongqiang Zhang
  • Ze Yang
چکیده

Healthy longevity has been an unremitting pursuit of human, but its genetic and the environment causes are still unclear. As longevity population is a good healthy aging model for understanding how the body begin aging and the process of aging, and plasma lipids metabolism and balance is a very important to life maintain and physiologic functional turnover. It is important to explore how the effect of genetic variants associated long-life individuals on lipids metabolism and balance. Therefore, we developed a comparative study based population which contains 2816 longevity and 2819 control. Through whole-exome sequencing and sanger sequencing genotypes, we identified four new single nucleotide polymorphisms of HLA-DQB1(major histocompatibility complex, class II, DQ beta 1), rs41542812 rs1049107 rs1049100 rs3891176(Prange=0.048-2.811×10-8 for allele frequencies), associated with longevity in Chinese Longevity Cohort. Further, by analysis of the longevity-variants linked to blood lipids, we identified HLA-DQB1 rs1049107, T-carriers (PHDL=0.006, OR: 11.277; PTG=9.095×10-7, OR: 0.025; PLDL/HDL=0.047, OR: 1.901) and HLA-DQB1 rs1049100, T-carriers (PTG=1.799×10-6, OR: 0.028) associated with lipid homeostasis in long lived individuals. Our finding showed that longevity and lipid homeostasis were associated with HLA-DQB1 and suggested that immune gene variants could act on both new function of maintaining the homeostasis and anti-aging in longevity.

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عنوان ژورنال:

دوره 9  شماره 

صفحات  -

تاریخ انتشار 2017