TY - JOUR
T1 - The correlation of copy number variations with longevity in a genome-wide association study of Han Chinese
AU - Zhao, Xin
AU - Liu, Xiaomin
AU - Zhang, Aiping
AU - Chen, Huashuai
AU - Huo, Qing
AU - Li, Weiyang
AU - Ye, Rui
AU - Chen, Zhihua
AU - Liang, Liping
AU - Liu, Qiong A.
AU - Shen, Juan
AU - Jin, Xin
AU - Li, W.
AU - Nygaard, Marianne
AU - Liu, Xiao
AU - Hou, Yong
AU - Ni, Ting
AU - Bolund, Lars
AU - Gottschalk, William
AU - Tao, Wei
AU - Gu, Jun
AU - Tian, Xiao Li
AU - Yang, Huanming
AU - Wang, Jian
AU - Xu, Xun
AU - Lutz, Michael W.
AU - Min, Junxia
AU - Zeng, Yi
AU - Nie, Chao
N1 - Publisher Copyright:
© 2018, Impact Journals LLC.
PY - 2018/6/1
Y1 - 2018/6/1
N2 - Copy number variations (CNVs) have been shown to cause numerous diseases, however, their roles in human lifespan remain elusive. In this study, we investigate the association of CNVs with longevity by comparing the Han Chinese genomes of long-lived individuals from 90 to 117 years of age and the middle-aged from 30 to 65. Our data demonstrate that the numbers of CNVs, especially deletions, increase significantly in a direct correlation with longevity. We identify eleven CNVs that strongly associate with longevity; four of them locate in the chromosome bands, 7p11.2, 20q13.33, 19p12 and 8p23.3 and overlap partially with the CNVs identified in long-lived Danish or U.S. populations, while the other seven have not been reported previously. These CNV regions encode nineteen known genes, and some of which have been shown to affect aging-related phenotypes such as the shortening of telomere length (ZNF208), the risk of cancer (FOXA1, LAMA5, ZNF716), and vascular and immune-related diseases (ARHGEF10, TOR2A, SH2D3C). In addition, we found several pathways enriched in long-lived genomes, including FOXA1 and FOXA transcription factor networks involved in regulating aging or age-dependent diseases such as cancer. Thus, our study has identified longevity-associated CNV regions and their affected genes and pathways. Our results suggest that the human genome structures such as CNVs might play an important role in determining a long life in human.
AB - Copy number variations (CNVs) have been shown to cause numerous diseases, however, their roles in human lifespan remain elusive. In this study, we investigate the association of CNVs with longevity by comparing the Han Chinese genomes of long-lived individuals from 90 to 117 years of age and the middle-aged from 30 to 65. Our data demonstrate that the numbers of CNVs, especially deletions, increase significantly in a direct correlation with longevity. We identify eleven CNVs that strongly associate with longevity; four of them locate in the chromosome bands, 7p11.2, 20q13.33, 19p12 and 8p23.3 and overlap partially with the CNVs identified in long-lived Danish or U.S. populations, while the other seven have not been reported previously. These CNV regions encode nineteen known genes, and some of which have been shown to affect aging-related phenotypes such as the shortening of telomere length (ZNF208), the risk of cancer (FOXA1, LAMA5, ZNF716), and vascular and immune-related diseases (ARHGEF10, TOR2A, SH2D3C). In addition, we found several pathways enriched in long-lived genomes, including FOXA1 and FOXA transcription factor networks involved in regulating aging or age-dependent diseases such as cancer. Thus, our study has identified longevity-associated CNV regions and their affected genes and pathways. Our results suggest that the human genome structures such as CNVs might play an important role in determining a long life in human.
KW - Copy number variation
KW - Genome association study
KW - Han Chinese
KW - Long-lived
KW - Longevity
KW - Middle-aged controls
UR - https://www.scopus.com/pages/publications/85049526325
U2 - 10.18632/aging.101461
DO - 10.18632/aging.101461
M3 - 文章
C2 - 29883365
AN - SCOPUS:85049526325
SN - 1945-4589
VL - 10
SP - 1206
EP - 1222
JO - Aging
JF - Aging
IS - 6
ER -
