TY - JOUR
T1 - Genetic origins of lactase persistence and the spread of pastoralism in africa
AU - Ranciaro, Alessia
AU - Campbell, Michael C.
AU - Hirbo, Jibril B.
AU - Ko, Wen Ya
AU - Froment, Alain
AU - Anagnostou, Paolo
AU - Kotze, Maritha J.
AU - Ibrahim, Muntaser
AU - Nyambo, Thomas
AU - Omar, Sabah A.
AU - Tishkoff, Sarah A.
N1 - Funding Information:
We thank Jacques Loiselet and Charles Wambebe for providing Lebanese and Nigerian samples, respectively. We thank Lilian A. Nyndodo, Eva Aluvalla, Daniel Kariuki, Godfrey Lema, Kweli Powell, Holly Mortensen, Maha Osman, Floyd A. Reed, Alex Tibwitta, George Ogutu, and Hussein Musa for assisting in sample collection. We thank Floyd A. Reed, Guido Barbujani, Dongbo Hu, Laura B. Scheinfeldt, and Karuna Panchapakesan for technical assistance and for valuable discussions. Most of all, we thank all of the African participants who generously donated DNA and phenotype information so that we might learn more about the genetic basis of lactase persistence and the spread of pastoralism in Africa. This research was funded by National Science Foundation grants BCS-0196183 and BCS-0827436 and National Institutes of Health grants 5-R01-GM076637-05 and 8DP1ES022577-04 to S.A.T.
PY - 2014/4/3
Y1 - 2014/4/3
N2 - In humans, the ability to digest lactose, the sugar in milk, declines after weaning because of decreasing levels of the enzyme lactase-phlorizin hydrolase, encoded by LCT. However, some individuals maintain high enzyme amounts and are able to digest lactose into adulthood (i.e., they have the lactase-persistence [LP] trait). It is thought that selection has played a major role in maintaining this genetically determined phenotypic trait in different human populations that practice pastoralism. To identify variants associated with the LP trait and to study its evolutionary history in Africa, we sequenced MCM6 introns 9 and 13 and ∼2 kb of the LCT promoter region in 819 individuals from 63 African populations and in 154 non-Africans from nine populations. We also genotyped four microsatellites in an ∼198 kb region in a subset of 252 individuals to reconstruct the origin and spread of LP-associated variants in Africa. Additionally, we examined the association between LP and genetic variability at candidate regulatory regions in 513 individuals from eastern Africa. Our analyses confirmed the association between the LP trait and three common variants in intron 13 (C-14010, G-13907, and G-13915). Furthermore, we identified two additional LP-associated SNPs in intron 13 and the promoter region (G-12962 and T-956, respectively). Using neutrality tests based on the allele frequency spectrum and long-range linkage disequilibrium, we detected strong signatures of recent positive selection in eastern African populations and the Fulani from central Africa. In addition, haplotype analysis supported an eastern African origin of the C-14010 LP-associated mutation in southern Africa.
AB - In humans, the ability to digest lactose, the sugar in milk, declines after weaning because of decreasing levels of the enzyme lactase-phlorizin hydrolase, encoded by LCT. However, some individuals maintain high enzyme amounts and are able to digest lactose into adulthood (i.e., they have the lactase-persistence [LP] trait). It is thought that selection has played a major role in maintaining this genetically determined phenotypic trait in different human populations that practice pastoralism. To identify variants associated with the LP trait and to study its evolutionary history in Africa, we sequenced MCM6 introns 9 and 13 and ∼2 kb of the LCT promoter region in 819 individuals from 63 African populations and in 154 non-Africans from nine populations. We also genotyped four microsatellites in an ∼198 kb region in a subset of 252 individuals to reconstruct the origin and spread of LP-associated variants in Africa. Additionally, we examined the association between LP and genetic variability at candidate regulatory regions in 513 individuals from eastern Africa. Our analyses confirmed the association between the LP trait and three common variants in intron 13 (C-14010, G-13907, and G-13915). Furthermore, we identified two additional LP-associated SNPs in intron 13 and the promoter region (G-12962 and T-956, respectively). Using neutrality tests based on the allele frequency spectrum and long-range linkage disequilibrium, we detected strong signatures of recent positive selection in eastern African populations and the Fulani from central Africa. In addition, haplotype analysis supported an eastern African origin of the C-14010 LP-associated mutation in southern Africa.
UR - http://www.scopus.com/inward/record.url?scp=84897979695&partnerID=8YFLogxK
U2 - 10.1016/j.ajhg.2014.02.009
DO - 10.1016/j.ajhg.2014.02.009
M3 - Article
C2 - 24630847
AN - SCOPUS:84897979695
SN - 0002-9297
VL - 94
SP - 496
EP - 510
JO - American Journal of Human Genetics
JF - American Journal of Human Genetics
IS - 4
ER -