Loss-of-function mutations in SLC30A8 protect against type 2 diabetes

Flannick, Jason; Þorleifsson, Guðmar; Beer, Nicola L.; Jacobs, Suzanne B.R.; Grarup, Niels; Burtt, Noél P.; Mahajan, Anubha; Fuchsberger, Christian; Atzmon, Gil; Benediktsson, Rafn; Blangero, John; Bowden, Don; Brandslund, Ivan; Brosnan, Julia; Burslem, Frank; Chambers, John C.; Cho, Yoon Shin; Christensen, Cramer; Douglas, Desiree; Duggirala, Ravindranath; Dymek, Zachary; Farjoun, Yossi; Fennell, Timothy; Fontanillas, Pierre; Forsén, Tom; Gabriel, Stacey; Gläser, Benjamin; Guðbjartsson, Daníel F.; Hanis, Craig L.; Hansen, Torben; Hreiðarsson, Ástráður B.; Hveem, Kristian; Ingelsson, Erik; Isomaa, Bo; Johansson, Stefan; Jørgensen, Torben; Jørgensen, Marit E.; Kathiresan, Sekar; Kong, Augustine; Kooner, Jaspal S.; Kravić, Jasmina; Laakso, Markku; Lee, Jong‐Young; Lind, Lars; Lindgren, Cecilia M.; Linneberg, Allan; Másson, Gísli; Meitinger, Thomas; Mohlke, Karen L.; Molven, Anders; Morris, Andrew P.; Potluri, Shobha; Rauramaa, Rainer; Ribel‐Madsen, Rasmus; Richard, Ann-Marie; Rolph, Tim; Salomaa, Veikko; Segrè, Ayellet V.; Skärstrand, Hanna; Steinthórsdóttir, Valgerður; Stringham, Heather M.; Sulem, Patrick; Tai, E Shyong; Teo, Yik Ying; Teslovich, Tanya M.; Þorsteinsdóttir, Unnur; Trimmer, Jeff K.; Tuomi, Tiinamaija; Tuomilehto, Jaakko; Vaziri-Sani, Fariba; Voight, Benjamin F.; Wilson, James G.; Boehnke, Michael; McCarthy, Mark; Njølstad, Pål R.; Pedersen, Oluf; Groop, Leif; Cox, David; Stefánsson, Kāri; Altshuler, David

doi:10.1038/ng.2915

Cited by 445 publications

(396 citation statements)

References 27 publications

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“…Among the variants, the two most common sequences failed to express a stable protein. Thus, SLC30A8 haploinsufficiency leading to a lower expression of the transporter appears from these studies to protect against T2D [73].…”

Section: Znt8 and T2d: Gwas Studiesmentioning

confidence: 80%

Section: Znt8 Studies In Vivomentioning

confidence: 99%

“…These findings thus uncovered a more complex role for ZnT8 in glucose homeostasis, and in particular in tissue-tissue interactions, than previously thought. Importantly, these complex interactions might contribute to the differences in the impact of genetic deletion of ZnT8 in mice versus reduction in levels (by 50 %) in rare allele carriers [73] or inheritance of risk variants (R325W) [77].The effects of exposure to a high fat diet as a means of promoting the development of T2D in mice have been studied in global and β cell-specific ZnT8 KO animals [83]. β cell specific null mice displayed similar bodyweights to controls but insulin secretion was impaired and these animals and were glucose-intolerant compared to control littermates.…”

mentioning

confidence: 99%

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Zinc and diabetes

Chabosseau

Rutter

2016

Archives of Biochemistry and Biophysics

149

104

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Zn 2+ ions are essential for the normal processing and storage of insulin and altered pancreatic insulin content is associated with all forms of diabetes mellitus. Work of the past decade has identified variants in the human SLC30A8 gene, encoding the zinc transporter ZnT8 which is expressed highly selectively on the secretory granule of pancreatic islet β and α cells, as affecting the risk of Type 2 Diabetes. Here, we review the regulation and roles of Zn 2+ ions in islet cells, the mechanisms through which SLC30A8 variants might affect glucose homeostasis and diabetes risk, and the novel technologies including recombinant targeted zinc probes and knockout mice which have been developed to explore these questions. Abbreviation ISG: Insulin Secreting Granules; T2D: Type 2 Diabetes; T1D: Type 1 Diabetes; 2 Diabetes mellitus is a common metabolic disease, affecting approximately 9% of the adult population worldwide. It is characterized by high circulating glucose levels over a prolonged period of time which leads to long-term health complications [1]. Type 1 Diabetes (T1D) involves the autoimmune destruction of insulin-secreting β cells while Type 2 Diabetes (T2D) is linked to both a decrease of insulin release and deficient hormone action on targeted organs [2].The links among Zn 2+ , diabetes and insulin were established in the 1930s, a decade after the discovery of the hormone, when a study showed crystallized insulin contains Zn 2+ and that Zn 2+ , along with other metal ions, could reversibly trigger insulin crystallization [3]. Zinc was later demonstrated to prolong insulin action when co-injected with the hormone [4].These early studies, as well as much more recent findings showing association between T2D risk and the inheritance of gene variants encoding a critical β cell Zn 2+ transporter, ZnT8[5] have generated considerable interest in the role of Zn 2+ in diabetes aetiology and as a possible therapeutic target [6]. Zinc and the diabetic patientScott and Fisher were the first to report a direct link between zinc and diabetes in patients.While assessing the insulin content in the pancreas of diabetic patients compared to nondiabetic cadavers, they showed that in the former group zinc content was reduced by 75 % [7].Epidemiological studies also demonstrated that diabetes and whole body zinc status are associated [8][9][10][11]. In T1D and T2D patients, serum zinc levels are significantly decreased [9][10][11], this being associated with an increased zinc urinary loss [8].Zinc may have important anti-oxidant properties, as it acts as a cofactor of the superoxide dismutase enzyme which regulates the detoxification of reactive oxygen species, regulating the expression and protecting against the oxidative stress induced by chronic hyperglycaemia (for review, [12]). Furthermore, zinc inhibits alpha-ketoglutarate-dependent mitochondrial respiration suggesting that Zn 2+ can interfere with mitochondrial antioxidant production and may also stimulate production of reactive oxygen [13].Zinc supplementation h...

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Section: Znt8 and T2d: Gwas Studiesmentioning

confidence: 80%

Section: Znt8 Studies In Vivomentioning

confidence: 99%

mentioning

confidence: 99%

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Zinc and diabetes

Chabosseau

Rutter

2016

Archives of Biochemistry and Biophysics

149

104

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“…As is the case in other analytic settings, the use of phenotypic extremes tends to lead to an overestimate of the effect of the variant and tends to overestimate the proportion of functionally active variants in a region, both of which support the value of population-based samples. 34 However, much larger sample sizes will be needed in order to have the power to detect associations in these instances.…”

Section: Discussionmentioning

confidence: 99%

Phenotypic extremes in rare variant study designs

et al. 2015

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Currently, next-generation sequencing studies aim to identify rare and low-frequency variation that may contribute to disease. For a given effect size, as the allele frequency decreases, the power to detect genes or variants of interest also decreases. Although many methods have been proposed for the analysis of such data, study design and analytic issues still persist in data interpretation. In this study we present sequencing data for ABCA1 that has known rare variants associated with high-density lipoprotein cholesterol (HDL-C). We contrast empirical findings from two study designs: a phenotypic extreme sample and a population-based random sample. We found differing strengths of association with HDL-C across the two study designs (P = 0.0006 with n = 701 phenotypic extremes vs P = 0.03 with n = 1600 randomly sampled individuals). To explore this apparent difference in evidence for association, we performed a simulation study focused on the impact of phenotypic selection on power. We demonstrate that the power gain for an extreme phenotypic selection study design is much greater in rare variant studies than for studies of common variants. Our study confirms that studying phenotypic extremes is critical in rare variant studies because it boosts power in two ways: the typical increases from extreme sampling and increasing the proportion of relevant functional variants ascertained and thereby tested for association. Furthermore, we show that when combining statistical evidence through meta-analysis from an extreme-selected sample and a second separate population-based random sample, power is lower when a traditional sample size weighting is used compared with weighting by the noncentrality parameter.

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“…Examples from T2D research highlight the diverse routes by which human genetics can inform translational medicine: (1) the combination of common-variant GWASs and candidate-gene resequencing has demonstrated that loss-of-function mutations in SLC30A8 (MIM: 611145; encoding a zinc transporter expressed in pancreatic islets) are protective for T2D, leading to efforts by several pharma companies to develop ZnT-8 antagonists; 93 (2) the use of genetic variants as instruments that ''simulate'' variation in environmental and biochemical exposures has clarified the extent to which vitamin D intake, early nutrition, circulating lipid levels, and chronic inflammation play causal roles with respect to the development of T2D [94][95][96][97][98] and has defined the relationship between insulin resistance and the distribution of adipose tissue; 99 (3) the identification of genetic variants associated with individual variation in response to commonly used therapeutic agents has refined our understanding of the mechanisms through which those agents operate 100,101 and, in some instances, has led to therapeutic optimization on the basis of genetic and/or clinical phenotype; 102 and (4) the combination of -omic measurements, longitudinal clinical phenotypes, and GWAS data has highlighted sets of molecules (e.g., branched-chain amino acids) that not only are prospectively associated with T2D progression but could also play a causal role in T2D development and thereby provide valuable clinical tools for stratification and prognostication. 103,104 Auto-immune Diseases Variant and Gene Discovery.…”

Section: Type 2 Diabetesmentioning

confidence: 99%