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Literature DB >> 28253084

Organic Cation Transporter 2 (OCT2/SLC22A2) Gene Variation in the South African Bantu-Speaking Population and Functional Promoter Variants.

Nina C Wilson¹, Ananyo Choudhury², Nadia Carstens³, Demetra Mavri-Damelin¹.

Abstract

SLC22A2 facilitates the transport of endogenous and exogenous cationic compounds. Many pharmacologically significant compounds are transported by SLC22A2, including the antidiabetic drug metformin, anticancer agent cisplatin, and antiretroviral lamivudine. Genetic polymorphisms in SLC22A2 can modify the pharmacokinetic profiles of such important medicines and could therefore prove useful as precision medicine biomarkers. Since the frequency of SLC22A2 polymorphisms varies among different ethnic populations, we evaluated these in South African Bantu speakers, a majority group in the South African population, who exhibit unique genetic diversity, and we subsequently functionally characterized promoter polymorphisms. We identified 11 polymorphisms within the promoter and 9 single-nucleotide polymorphisms (SNPs) within the coding region of SLC22A2. While some polymorphisms appeared with minor allele frequencies similar to other African and non-African populations, some differed considerably; this was especially notable for three missense polymorphisms. In addition, we functionally characterized two promoter polymorphisms; rs138765638, a three base-pair deletion that bioinformatics analysis suggested could alter c-Ets-1/2, Elk1, and/or STAT4 binding, and rs59695691, an SNP that could abolish TFII-I binding. Significantly higher luciferase reporter gene expression was found for rs138765638 (increase of 37%; p = 0.001) and significantly lower expression for rs59695691 (decrease of 25%; p = 0.038), in comparison to the wild-type control. These observations highlight the importance of identifying and functionally characterizing genetic variation in genes of pharmacological significance. Finally, our data for SLC22A2 attest to the importance of considering genetic variation in different populations for drug safety, response, and global pharmacogenomics, through, for example, projects such as the Human Heredity and Health in Africa initiative.

Entities: Chemical Gene Mutation Species

Keywords: South Africa; genetic variation; organic cation transporters; personalized medicine; pharmacogenetics

Mesh：

Substances：

Year: 2017 PMID： 28253084 PMCID： PMC5972774 DOI： 10.1089/omi.2016.0165

Source DB: PubMed Journal: OMICS ISSN： 1536-2310

43 in total

1. PROMO: detection of known transcription regulatory elements using species-tailored searches.

Authors: Xavier Messeguer; Ruth Escudero; Domènec Farré; Oscar Núñez; Javier Martínez; M Mar Albà
Journal: Bioinformatics Date: 2002-02 Impact factor: 6.937

2. How can we help? From "sociology in" to "sociology of" bioethics.

Authors: Raymond De Vries
Journal: J Law Med Ethics Date: 2004 Impact factor: 1.718

3. The effects of genetic polymorphisms in the organic cation transporters OCT1, OCT2, and OCT3 on the renal clearance of metformin.

Authors: M V Tzvetkov; S V Vormfelde; D Balen; I Meineke; T Schmidt; D Sehrt; I Sabolić; H Koepsell; J Brockmöller
Journal: Clin Pharmacol Ther Date: 2009-06-17 Impact factor: 6.875

4. Gene expression levels and immunolocalization of organic ion transporters in the human kidney.

Authors: Hideyuki Motohashi; Yuji Sakurai; Hideyuki Saito; Satohiro Masuda; Yumiko Urakami; Maki Goto; Atsushi Fukatsu; Osamu Ogawa; Ken-Ichi Inui
Journal: J Am Soc Nephrol Date: 2002-04 Impact factor: 10.121

5. Cloning and characterization of two human polyspecific organic cation transporters.

Authors: V Gorboulev; J C Ulzheimer; A Akhoundova; I Ulzheimer-Teuber; U Karbach; S Quester; C Baumann; F Lang; A E Busch; H Koepsell
Journal: DNA Cell Biol Date: 1997-07 Impact factor: 3.311

6. Polymorphisms in a human kidney xenobiotic transporter, OCT2, exhibit altered function.

Authors: Maya K Leabman; Conrad C Huang; Michiko Kawamoto; Susan J Johns; Douglas Stryke; Thomas E Ferrin; Joseph DeYoung; Travis Taylor; Andrew G Clark; Ira Herskowitz; Kathleen M Giacomini
Journal: Pharmacogenetics Date: 2002-07

7. Human neurons express the polyspecific cation transporter hOCT2, which translocates monoamine neurotransmitters, amantadine, and memantine.

Authors: A E Busch; U Karbach; D Miska; V Gorboulev; A Akhoundova; C Volk; P Arndt; J C Ulzheimer; M S Sonders; C Baumann; S Waldegger; F Lang; H Koepsell
Journal: Mol Pharmacol Date: 1998-08 Impact factor: 4.436

Organic Cation Transporter 2 (OCT2/SLC22A2) Gene Variation in the South African Bantu-Speaking Population and Functional Promoter Variants.

1. PROMO: detection of known transcription regulatory elements using species-tailored searches.

2. How can we help? From "sociology in" to "sociology of" bioethics.

3. The effects of genetic polymorphisms in the organic cation transporters OCT1, OCT2, and OCT3 on the renal clearance of metformin.

4. Gene expression levels and immunolocalization of organic ion transporters in the human kidney.

5. Cloning and characterization of two human polyspecific organic cation transporters.

6. Polymorphisms in a human kidney xenobiotic transporter, OCT2, exhibit altered function.

7. Human neurons express the polyspecific cation transporter hOCT2, which translocates monoamine neurotransmitters, amantadine, and memantine.

8. Genetic variants of the organic cation transporter 2 influence the disposition of metformin.

9. A global reference for human genetic variation.

10. The Ensembl Variant Effect Predictor.

Review 1. Genetic Diversity in Drug Transporters: Impact in African Populations.

Review 2. Comparison of Anticancer Drug Toxicities: Paradigm Shift in Adverse Effect Profile.