Lactase persistence DNA variant enhances lactase promoter activity in vitro: functional role as a cis regulatory element

doi:10.1093/hmg/ddg244

Human Molecular Genetics Advance Access originally published online on July 22, 2003

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Human Molecular Genetics, 2003, Vol. 12, No. 18 2333-2340
DOI: 10.1093/hmg/ddg244
© 2003 Oxford University Press

Lactase persistence DNA variant enhances lactase promoter activity in vitro: functional role as a cis regulatory element

Lynne C. Olds and Eric Sibley^*

Department of Pediatrics, Stanford University Medical Center, Stanford, CA 94305, USA

Received May 2, 2003; Accepted July 7, 2003

Lactase persistence is a heritable, autosomal dominant, conditionthat results in a sustained ability to digest the milk sugarlactose throughout adulthood. The majority of the world's humanpopulation experiences a decline in production of the digestiveenzyme lactase-phlorizin hydrolase during maturation. However,individuals with lactase persistence continue to express highlevels of the lactase gene into adulthood. Lactase persistencehas been strongly correlated with single nucleotide geneticvariants, C/T_-13910 and G/A_-22018, located 13.9 and 22 kbupstream from the lactase structural gene. We aimed to characterizea functional role for the polymorphisms in regulating lactasegene transcription. DNA in the region of the C/T_-13910 or G/A_-22018human lactase variants was cloned upstream of the 3.0 kbrat lactase gene promoter in a luciferase reporter construct.Human intestinal Caco-2 cells were transfected with the lactasevariant/promoter–reporter constructs and assayed for promoteractivity. A 200 bp region surrounding the C_-13910 variant,associated with lactase non-persistence, results in a 2.2-foldincrease in lactase promoter activity. The T_-13910 variant,associated with lactase persistence, results in an even greater2.8-fold increase. The DNA sequence of the C/T_-13910 variantsdifferentially interacts with intestinal cell nuclear proteinson EMSAs. AP2 co-transfection results in a similar repressionof the C/T_-13910 variant/promoter–reporter constructs.The DNA region of the C/T_-13910 lactase persistence/non-persistencevariant functions in vitro as a cis element capable of enhancingdifferential transcriptional activation of the lactase promoter.Such differential regulation by the C and T variants is consistentwith a causative role in the mechanism specifying the lactasepersistence/non-persistence phenotypes in humans.

^* To whom correspondence should be addressed at: Department ofPediatrics, Stanford University School of Medicine, 750 WelchRoad, Suite 116, Palo Alto, CA 943404, USA. Tel: +1 6507235070;Fax: +1 6504985608; Email: erc{at}stanford.edu

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