Concept and design of a genome-wide association genotyping array tailored for transplantation-specific studies

Li, Yun R.; Setten, Jessica van; Verma, Shefali S.; Lu, Yontao; Holmes, Michael V.; Gao, Hui; Lek, Monkol; Nair, Nikhil; Chandrupatla, Hareesh R.; Chang, Bao‐Li; Karczewski, Konrad J.; Wong, Chanel; Mohebnasab, Maede; Mukhtar, Eyas H.; Phillips, Randy; Tragante, Vinicius; Hou, Cuiping; Steel, Laura F.; Lee, Takesha; Garifallou, James; Guettouche, Toumy; Cao, Hongzhi; Guan, Weihua; Himes, Aubree; Houten, Jacob van; Pasquier, Andrew; Yu, Reina; Carrigan, Elena; Miller, Michael B.; Schladt, David; Akdere, Abdullah; González, Ana; Llyod, Kelsey M.; McGinn, Daniel; Gangasani, Abhinav; Michaud, Zach; Colasacco, Abigail; Snyder, James W.; Thomas, Kelly; Wang, Tiancheng; Wu, Baolin; Alzahrani, Alhusain J.; Al-Ali, Amein K.; Al-Muhanna, Fahad; Al-Rubaish, Abdullah M.; Al-Mueilo, Samir; Monos, Dimitri; Murphy, Barbara; Olthoff, Kim M.; Wijmenga, Cisca; Webster, Teresa A.; Kamoun, Malek; Balasubramanian, Suganthi; Lanktree, Matthew B.; Oetting, William S.; García‐Pavía, Pablo; MacArthur, Daniel G.; Bakker, Paul I. W. de; Hákonarson, Hákon; Birdwell, Kelly A.; Jacobson, Pamala A.; Ritchie, Marylyn D.; Asselbergs, Folkert W.; Israni, Ajay K.; Shaked, Abraham; Keating, Brendan J.

doi:10.1186/s13073-015-0211-x

Cited by 51 publications

(60 citation statements)

References 47 publications

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“…Pre‐transplant recipient DNA was obtained at the time of transplant from peripheral blood lymphocytes after red blood cell lysis and isolation by centrifugation. A customized exome‐plus Affymetrix TxArray SNP chip (Affymetrix, Santa Clara, CA, USA) was used to genotype DNA for genetic variants . This chip contains approximately 782 000 genetic markers including 168 000 exonic or coding variants and over 16 000 putative loss‐of‐function variants.…”

Section: Methodsmentioning

confidence: 99%

“…A customized exome-plus Affymetrix TxArray SNP chip (Affymetrix, Santa Clara, CA, USA) was used to genotype DNA for genetic variants. 34 This chip contains approximately 782 000 genetic markers including 168 000 exonic or coding variants and over 16 000 putative loss-of-function variants. The CYP3A5*3 (rs776746), CYP3A5*6 (rs10264272), and CYP3A5*7 (rs41303343) loss-of-function variants were used in this study and taken from this chip.…”

Section: Genotypingmentioning

confidence: 99%

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Tacrolimus trough and dose intra‐patient variability and CYP3A5 genotype: Effects on acute rejection and graft failure in European American and African American kidney transplant recipients

Seibert

Schladt

et al. 2018

Clinical Transplantation

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Background: Suboptimal immunosuppression after kidney transplantation contributes to toxicity and loss of efficacy. Little is known regarding the impact of intra-patient variability of tacrolimus (TAC) doses and troughs in the early post-transplant period or the influence of genetic variants on variability. Methods: Coefficients of variation (CV) of TAC troughs and doses of 1226 European American (EA) and 246 African American (AA) adult recipients enrolled in DeKAF Genomics were compared for association with acute rejection and graft failure. Additionally, the influence of recipients’ number of CYP3A5 loss-of-function alleles was assessed. Results: Acute rejection was associated with greater CV of dose in AA (p<0.001) and EA recipients (p=0.012). Graft failure was associated with a greater CV of dose (p=0.022) and trough (p<0.001) in AA, and higher CV of trough (p=0.024) in EA recipients. In EA, CYP3A5 loss-of-function alleles were associated with decreased CV of trough (p=0.0042) and increased CV of dose (p<0.0001). Conclusion: CYP3A5 loss-of-function alleles influence intra-patient TAC trough and dose variability. High variability of TAC dose increases risk of acute rejection. High variability of TAC trough increases risk of graft failure. Early clinical recognition of TAC dose and trough variability may improve patient management and outcomes.

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Section: Methodsmentioning

confidence: 99%

Section: Genotypingmentioning

confidence: 99%

Tacrolimus trough and dose intra‐patient variability and CYP3A5 genotype: Effects on acute rejection and graft failure in European American and African American kidney transplant recipients

Seibert

Schladt

et al. 2018

Clinical Transplantation

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“…Genotyping was conducted on an exome-plus Affymetrix Transplant Array chip (Affymetrix, Santa Clara, CA) with ~800 000 high-quality genomic markers after quality control and >34 M markers after imputation using the 1000 Genomes phase 3 and Genome of the Netherlands v5. [27][28][29][30][31] Data quality control was carried out with PLINK software (version 1.90b1a, Harvard University, Cambridge, MA). 32 Genotypes were phased using SHAPEIT2 (v2.r644, University of Oxford, UK) 33 ; and imputed with IMPUTE2 (University of Oxford, UK) 34 Imputed variants with information score more than 0.8 were considered of good quality and used in the analysis.…”

Section: Genotypingmentioning

confidence: 99%

Tacrolimus troughs and genetic determinants of metabolism in kidney transplant recipients: A comparison of four ancestry groups

Mohamed

Schladt

Guan

et al. 2019

American Journal of Transplantation

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Tacrolimus trough and dose requirements vary dramatically between individuals ofEuropean and African American ancestry. These differences are less well described in other populations. We conducted an observational, prospective, multicenter study from which 2595 kidney transplant recipients of European, African, Native American, and Asian ancestry were studied for tacrolimus trough, doses, and genetic determinants of metabolism. We studied the well-known variants and conducted a CYP3A4/5 gene-wide analysis to identify new variants. Daily doses, and dose-normalized troughs were significantly different between the four groups (P < .001). CYP3A5*3 (rs776746) was associated with higher dose-normalized tacrolimus troughs in all groups but occurred at different allele frequencies and had differing effect sizes. The CYP3A5*6 (rs10264272) and *7 (rs413003343) variants were only present in African Americans. CYP3A4*22 (rs35599367) was not found in any of the Asian ancestry samples. We identified seven suggestive variants in the CYP3A4/5 genes associated with dose-normalized troughs in Native Americans (P = 1.1 × 10 −5 -8.8 × 10 −6 ) and

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“…GWASs have been applied to numerous hematologic endpoints and have advanced our knowledge of the genetic underpinnings of modifiers of complete blood count, hematopoiesis, cardiovascular diseases, and sickle cell anemia . Transplant research has benefitted from GWASs by identifying novel genes and alleles that are associated with kidney transplant rejection and clinical outcomes in patients with renal and lung transplants . Although advances in whole genome sequencing have made it possible to interrogate causal variants directly as opposed to evaluating variants that are in linkage disequilibrium with causal variants, array‐based genotyping remains a cost‐effective method for genotyping large cohorts, such as the UK Biobank cohort, in which half a million participants have been enrolled and genotyped .…”

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confidence: 99%

Development and evaluation of a transfusion medicine genome wide genotyping array

et al. 2018

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BACKGROUND: Many aspects of transfusion medicine are affected by genetics. Current single-nucleotide polymorphism (SNP) arrays are limited in the number of targets that can be interrogated and cannot detect all variation of interest. We designed a transfusion medicine array (TM-Array) for study of both common and rare transfusion-relevant variations in genetically diverse donor and recipient populations.STUDY DESIGN AND METHODS: The array was designed by conducting extensive bioinformatics mining and consulting experts to identify genes and genetic variation related to a wide range of transfusion medicine clinical relevant and research-related topics. Copy number polymorphisms were added in the alpha globin, beta globin, and Rh gene clusters. RESULTS:The final array contains approximately 879,000 SNP and copy number polymorphism markers. Over 99% of SNPs were called reliably. Technical replication showed the array to be robust and reproducible, with an error rate less than 0.03%. The array also had a very low Mendelian error rate (average parent-child trio accuracy of 0.9997). Blood group results were in concordance with serology testing results, and the array accurately identifies rare variants (minor allele frequency of 0.5%). The array achieved high genome-wide imputation coverage for African-American (97.5%), Hispanic (96.1%), East Asian (94.6%), and white (96.1%) genomes at a minor allele frequency of 5%. CONCLUSIONS: A custom array for transfusionmedicine research has been designed and evaluated. It gives wide coverage and accurate identification of rare SNPs in diverse populations. The TM-Array will be useful for future genetic studies in the diverse fields of transfusion medicine research. T ransfusion medicine encompasses diverse medical services and fields of research including blood donation, component processing, immunohematology, infectious disease, recipient outcomes, ABBREVIATIONS: BGMUT = blood group antigen gene mutation; CNPs = copy number polymorphisms; GWASs = genome-wide association studies; MAF = minor allele frequency; NHLBI = National Heart, Lung, and Blood Institute; RBC-Omics = Red Blood Cell Omics; REDS-III = Recipient Epidemiology Donor Evaluation Study-III; SCD = sickle cell disease; SNP = single-nucleotide polymorphism

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Concept and design of a genome-wide association genotyping array tailored for transplantation-specific studies

Cited by 51 publications

References 47 publications

Tacrolimus trough and dose intra‐patient variability and CYP3A5 genotype: Effects on acute rejection and graft failure in European American and African American kidney transplant recipients

Tacrolimus trough and dose intra‐patient variability and CYP3A5 genotype: Effects on acute rejection and graft failure in European American and African American kidney transplant recipients

Tacrolimus troughs and genetic determinants of metabolism in kidney transplant recipients: A comparison of four ancestry groups

Development and evaluation of a transfusion medicine genome wide genotyping array

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