David Zeitlyn scite author profile

The ability to digest the milk sugar lactose as an adult (lactase persistence) is a variable genetic trait in human populations. The lactase-persistence phenotype is found at low frequencies in the majority of populations in sub-Saharan Africa that have been tested, but, in some populations, particularly pastoral groups, it is significantly more frequent. Recently, a CT polymorphism located 13.9 kb upstream of exon 1 of the lactase gene (LCT) was shown in a Finnish population to be closely associated with the lactase-persistence phenotype (Enattah et al. 2002). We typed this polymorphism in 1,671 individuals from 20 distinct cultural groups in seven African countries. It was possible to match seven of the groups tested with groups from the literature for whom phenotypic information is available. In five of these groups, the published frequencies of lactase persistence are >/=25%. We found the T allele to be so rare that it cannot explain the frequency of the lactase-persistence phenotype throughout Africa. By use of a statistical procedure to take phenotyping and sampling errors into account, the T-allele frequency was shown to be significantly different from that predicted in five of the African groups. Only the Fulbe and Hausa from Cameroon possessed the T allele at a level consistent with phenotypic observations (as well as an Irish sample used for comparison). We conclude that the C-13.9kbT polymorphism is not a predictor of lactase persistence in sub-Saharan Africans. We also present Y-chromosome data that are consistent with previously reported evidence for a back-migration event into Cameroon, and we comment on the implications for the introgression of the -13.9kb*T allele.

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Gift economies in the development of open source software: anthropological reflections

Zeitlyn

2003

Research Policy

188

110

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Prevalence of Clinically Relevant UGT1A Alleles and Haplotypes in African Populations

Horsfall

Zeitlyn

Tarekegn

et al. 2011

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SummaryVariation of a short (TA) n repeat sequence (rs8175347) covering the TATA box of UGT1A1 (UDPglucuronosyltransferase1A1) is associated with hyperbilirubinaemia (Gilbert's syndrome) and adverse drug reactions, and is used for dosage advice for irinotecan. Several reports indicate that the low-activity (risk) alleles ((TA) 7 and (TA) 8 )) are very frequent in Africans but the patterns of association with other variants in the UGT1A gene complex that may modulate these responses are not well known. rs8175347 and two other clinically relevant UGT1A variants (rs11692021 and rs10929302) were assayed in 2616 people from Europe and Africa. Low-activity (TA) n alleles frequencies were highest in equatorial Africa, (TA) 7, being the most common in Cameroon, Ghana, southern Sudan, and in Ethiopian Anuak. Haplotypic diversity was also greatest in equatorial Africa, but in Ethiopia was very variable across ethnic groups. Resequencing of the promoter of a sample subset revealed no novel variations, but rs34547608 and rs887829 were typed and shown to be tightly associated with (TA) n . Our results illustrate the need for investigation of the effect of UGT1A variants other than (TA) n on the risk of irinotecan toxicity, as well as hyperbilirubinaemia due to hemolytic anaemia or human immunodeficiency virus protease inhibitors, so that appropriate pharmacogenetic advice can be given.

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Anthropology in and of the Archives: Possible Futures and Contingent Pasts. Archives as Anthropological Surrogates

Zeitlyn¹

2012

Annu. Rev. Anthropol.

170

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Derrida and Foucault provide key starting points to understanding archives. They see archives as hegemonic, characterizing ways of thought, modes of colonization, and the control of citizens. However, they also make clear that archives can be read subversively. With patience, counter-readings allow the excavation of the voices (sometimes names) of subaltern and otherwise suppressed others from the archive. By reading along and across the archival grain, researchers can follow the development of ideas and processes across historical periods. Archives can be seen as orphanages, containing surrogates of performances. Archives (paper and digital) also provide access to the results of anthropological research in ways mandated by ethics codes, but these are subject to controversy. What sorts of consent and what sorts of anonymization should be provided? Archives run by the groups traditionally studied by anthropologists provide models of radical archives that are very different from those conceived of by traditional archivists. Read a French translation of this article.

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The potentially deleterious functional variant flavin-containing monooxygenase 2*1 is at high frequency throughout sub-Saharan Africa

Veeramah

Thomas²,

Weale³

et al. 2008

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Background-The drug-metabolizing enzyme flavin-containing monooxygenase 2 (FMO2) is the predominant FMO isoform present in the lung of most mammals, including non-human primates. All Europeans and Asians tested have been shown to be homozygous for a nonfunctional variant, FMO2*2A, which contains a premature stop codon due to a single-nucleotide change in exon 9 (g. 23238C > T). The ancestral allele, FMO2*1, encodes a functionally active protein and has been found in African-Americans (26%) and Hispanics (2% to 7%). Possessing this variant increases the risk of pulmonary toxicity when exposed to thioureas, a widely used class of industrial compounds. FMO2 may also be involved in the metabolism of drugs that are used to treat diseases that are prevalent in Africa.

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David Zeitlyn

The T Allele of a Single-Nucleotide Polymorphism 13.9 kb Upstream of the Lactase Gene (LCT) (C−13.9kbT) Does Not Predict or Cause the Lactase-Persistence Phenotype in Africans

Gift economies in the development of open source software: anthropological reflections

Prevalence of Clinically Relevant UGT1A Alleles and Haplotypes in African Populations

Anthropology in and of the Archives: Possible Futures and Contingent Pasts. Archives as Anthropological Surrogates

The potentially deleterious functional variant flavin-containing monooxygenase 2*1 is at high frequency throughout sub-Saharan Africa

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