Characterization of Coding Synonymous and Non-Synonymous Variants in ADAMTS13 Using Ex Vivo and In Silico Approaches

Edwards, Nathan C.; Hing, Zachary A.; Perry, Avital; Blaisdell, Adam; Kopelman, David B.; Fathke, Robert; Plum, William; Newell, Jordan M.; Allen, Courtni E.; Geetha, S.; Shapiro, Aaron; Okunji, Chinyere; Kosti, Idit; Shomron, Noam; Grigoryan, Vahan; Przytycka, Teresa M.; Sauna, Zuben E.; Salari, Raheleh; Mandel-Gutfreund, Yael; Komar, Anton A.; Kimchi-Sarfaty, Chava

doi:10.1371/journal.pone.0038864

Cited by 61 publications

(57 citation statements)

References 78 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…These 2 common ADAMTS13 variants have been examined in 2 previous studies. One study examined expression and secretion of Q448E in cell culture and found results similar to those of our study but an increased specific activity of this variant compared with wild-type, 39 and another article examined both the Q448E and A732V variants expressed in cell culture and found similar decreases in secretion into culture media and ;25% reduction in enzyme activity as measured by a collagen binding assay. 40 However, both previous studies used transient transfection methods which may have altered patterns of synthesis and secretion compared with our experiments in cell lines with stable expression from the same locus.…”

Section: Discussionsupporting

confidence: 81%

Genetic variants in ADAMTS13 as well as smoking are major determinants of plasma ADAMTS13 levels

Ma¹,

Jacobi

Emmer³

et al. 2017

Blood Advances

Self Cite

View full text Add to dashboard Cite

Key Points• Three independent association signals at ADAMTS13 and smoking were identified as major predictors of plasma ADAMTS13 levels.• Evidence was presented that 2 nonsynonymous ADAMTS13 variants were driving the variation of plasma ADAMTS13 concentrations. P 5 1.2E-30) and rs3124762 (b, 3.5%; P 5 8.9E-9) close to ADAMTS13 and rs4075970 (b, 2.4%; P 5 6.8E-9) on 21q22.3. Linkage analysis also identified the region around ADAMTS13 (9q34.2) as the top signal (LOD 3.5), consistent with our SNP association analyses. Two nonsynonymous ADAMTS13 variants in the top 2 independent linkage disequilibrium blocks (Q448E and A732V) were identified and characterized in vitro. This study uncovered specific common genetic polymorphisms that are key genetic determinants of the variation in plasma ADAMTS13 levels in healthy individuals.

show abstract

Section: Discussionsupporting

confidence: 81%

Genetic variants in ADAMTS13 as well as smoking are major determinants of plasma ADAMTS13 levels

Ma¹,

Jacobi

Emmer³

et al. 2017

Blood Advances

Self Cite

View full text Add to dashboard Cite

show abstract

“…1 However, an independent causal relationship between ADAMTS13 levels could not be established because of the unavailability of prospective studies. Recent studies aiming at the characterization of single nucleotide variants in ADAMTS13 through mRNA studies and in silico approaches 9,10 suggest that single nucleotide variants in ADAMTS13 influence its gene expression in a complex fashion, thus explaining interindividual variability in ADAMTS13 activity beyond nonsynonymous coding mutations affecting vWF-cleaving properties.…”

mentioning

confidence: 99%

Rare Variants in the ADAMTS13 Von Willebrand Factor–Binding Domain Contribute to Pediatric Stroke

Stoll

Rühle

Witten

et al. 2016

Circ Cardiovasc Genet

View full text Add to dashboard Cite

Background-Recently, we reported a gene network of ADAMTS (A Disintegrin-like and Metalloprotease with Thrombospondin motifs) genes as central component of the genetic risk contributing to pediatric stroke. ADAMTS13 is a prime example for such a key component as it cleaves von Willebrand factor multimers, reduces platelet adhesion and aggregation, and downregulates thrombus formation and inflammation. Methods and Results-We characterized the genetic architecture of ADAMTS13 through targeted next-generation sequencing of 48 affected children and their unaffected siblings and identified in total 241 variants (single nucleotide polymorphisms or insertions/deletions) in the ADAMTS13 gene. From these, based on significance in the sibship disequilibrium test (P<0.05) or protein-altering properties, we selected 21 common variants covering the complete ADAMTS13 gene for genotyping in 270 trios and subsequent association analyses. Transmission disequilibrium testing was performed for affection status and ADAMTS13 activity levels using PLINK and FBAT, respectively. Ten single nucleotide polymorphisms were significantly associated with pediatric stroke (P<0.05 to P<0.001), 2 of which (rs2285489 and rs28793911) were also significantly associated with ADAMTS13 levels (P=0. 0004 and P=0.0092 In 2012, we reported a genome-wide association study in 270 affected offspring trios, which demonstrates the association of several members of the ADAMTS gene family with pediatric stroke 11 including a moderate association of single nucleotide polymorphisms (SNPs) in the vicinity of ADAMTS13. In parallel, we extended our studies to include the association of ADAMTS13 plasma levels as an intermediate phenotype and the risk for pediatric stroke 2 and demonstrated that decreased ADAMTS13 activity is a risk factor (odds ratio, 6.70; 95% confidence interval, 2.58-17.38) for incident ischemic stroke in children without underlying disease.In the present study, we characterized the genomic architecture underlying ADAMTS13 through a targeted nextgeneration sequencing approach in 48 pairs of patients with pediatric stroke and their unaffected siblings. Twenty-one ADAMTS13 variants identified in this discovery stage were subsequently genotyped in the above-mentioned cohort of 270 affected offspring trios and analyzed by transmission disequilibrium testing for association with stroke affection status and ADAMTS13 serum levels. By this, we establish a causal relationship between ADAMTS13 single nucleotide variants, ADAMTS13 levels, and pediatric stroke susceptibility. Methods Subjects EthicsThe present study was performed in accordance with the ethical standards laid down in the updated version of the 1964 Declaration of Helsinki and was approved by the medical ethics committee of the University of Münster, Germany. Written informed consent was obtained from all participants or their parent(s). PatientsEnrollment and characterization of affected family trios have been described in detail in our initial genome-wide association study publication.11 In ...

show abstract

“…Fluorogenic FRETS-VWF73 (Peptides International; Louisville, KY, USA) was prepared and assayed (Sauna et al, 2009). The kinetic characteristics of ADAMTS13 were obtained using GraphPad Prism software.ADAMTS13 sequencing revealed both children to be homozygous and their parents to be heterozygous for the previously described, cTTP-causing, single-base-substitution mutation 20506C > T (Table IA) (Levy et al, 2001;Snider et al, 2004;Hing et al, 2013). The children's VWF-CPase antigen and activity levels were undetectable, although steady-state levels of the ADAMTS13 mRNA were >2Á5-fold higher in the daughter than in the son.…”

mentioning

confidence: 90%

“…While prior studies have shown that the synonymous (s)-and ns-SNVs 3944C > T (c.864C > T ⇒ 140Ala > Ala) and 23789C > T (c.3143C > T ⇒ 900Ala > Val), respectively, are associated in vitro with no or only minor effects on VWF-CPase secretion compared to their more frequent wildtype alleles (Plaimauer et al, 2006;Edwards et al, 2012), the seven other allelically distinct, parental ADAMTS13 potential quantitative-trait nucleotides (QTNs) have never been experimentally investigated, individually or in combination with each other. The candidate functional SNVs, 11610G > C (IVS10[-32G > C]) and 18320G > A (IVS15[-26G > A]), are located in intronic regions known to contain cis-elements comprising 3'-splice junctions, and their alleles may, for example, influence precursor mRNA processing differentially.…”

mentioning

confidence: 99%

Single-nucleotide variations defining previously unreportedADAMTS13haplotypes are associated with differential expression and activity of the VWF-cleaving protease in a Salvadoran congenital thrombotic thrombocytopenic purpura family

Kim

Hing

et al. 2014

Br J Haematol

Self Cite

View full text Add to dashboard Cite

Single-nucleotide variations defining previously unreported ADAMTS13 haplotypes are associated with differential expression and activity of the VWF-cleaving protease in a Salvadoran congenital thrombotic thrombocytopenic purpura familyAlthough autosomal recessive haematological disorders, such as congenital thrombotic thrombocytopenic purpura (cTTP), are individually rare and difficult to ascertain, studies involving one or more homozygous affected children and their unaffected heterozygous parents have led to expanded understanding of known and discovery of previously unknown molecular-genetic characteristics. We present an in-depth examination of ADAMTS13 haplotypes, mRNA levels and protein expression, activity, and enzyme kinetics in this case study of two Salvadoran children with cTTP -the first reported cases of this disease in individuals originally from Central America -and their parents.The propositi -a son and a daughter born to asymptomatic, non-consanguineous (but possibly distantly related) parents from the same town in El Salvador -were diagnosed with cTTP at ages 6 and 2 years, respectively. Although they developed haemolytic anaemia and thrombocytopenia 2 d (son) and 17 months (daughter) after birth, their cTTP diagnosis was not rendered until both were hospitalized simultaneously with fever, respiratory symptoms, haemolytic anaemia and thrombocytopenia. Peripheral blood smears for both demonstrated schistocytes, and their von Willebrand factor-cleaving protease (VWF-CPase) activities were <1% without ADAMTS13 IgG antibodies. Fresh frozen plasma (FFP) infusion induced rapid (within 48 h) normalization of their blood counts and resolution of the microangiopathic changes. Both children have been treated with prophylactic infusions of FFP (10 ml/kg every 2Á5 weeks) without long-term neurological or renal sequelae.Following approval by institutional review boards and receipt of informed consent, blood samples were collected from the children, prior to FFP administration, and from both parents. Genomic DNA and total RNA were extracted from peripheral blood leukocytes using QIAamp DNA Blood Maxi and PAXgene Blood RNA kits, respectively (Qiagen; Germantown, MD, USA). All ADAMTS13 exons, at least 50 base pairs (bp) of each flanking intron junction,~500 bp 5' of the promoter, and~200 bp of 3'-flanking genomic DNA were amplified using polymerase chain reaction (PCR), cleaned using Exo-SAP-IT (Affymetrix; Santa Clara, CA, USA), and subjected to direct bi-directional Sanger sequencing followed by capillary electrophoresis and analysis on ABI-3730 instruments. Reverse transcription was performed (Shomron et al, 2010), and plasma VWF-CPase antigen was measured using the Technozym ADAMTS13 enzyme-linked immunosorbent assay (Technoclone; Vienna, Austria) and the Victor X3 multilabel plate reader (PerkinElmer; Waltham, MA, USA). Fluorogenic FRETS-VWF73 (Peptides International; Louisville, KY, USA) was prepared and assayed (Sauna et al, 2009). The kinetic characteristics of ADAMTS13 were obtained using GraphPad Pri...

show abstract

Characterization of Coding Synonymous and Non-Synonymous Variants in ADAMTS13 Using Ex Vivo and In Silico Approaches

Cited by 61 publications

References 78 publications

Genetic variants in ADAMTS13 as well as smoking are major determinants of plasma ADAMTS13 levels

Genetic variants in ADAMTS13 as well as smoking are major determinants of plasma ADAMTS13 levels

Rare Variants in the ADAMTS13 Von Willebrand Factor–Binding Domain Contribute to Pediatric Stroke

Single-nucleotide variations defining previously unreportedADAMTS13haplotypes are associated with differential expression and activity of the VWF-cleaving protease in a Salvadoran congenital thrombotic thrombocytopenic purpura family

Contact Info

Product

Resources

About