Child-onset thrombotic thrombocytopenic purpura caused by p.R498C and p.G259PfsX133 mutations in ADAMTS13

An-Sofie Schelpe; Christelle Orlando; Bogac Ercig; Chloe Geeroms; Inge Pareyn; Nele Vandeputte; Leydi Carolina Pereira; Elien Roose; Karel Fostier; Gerry A. F. Nicolaes; Hans Deckmyn; Simon F. De Meyer; Karen Vanhoorelbeke; Kristin Jochmans

doi:10.1111/ejh.13094

Child-onset thrombotic thrombocytopenic purpura caused by p.R498C and p.G259PfsX133 mutations in ADAMTS13

An-Sofie Schelpe, Christelle Orlando, Bogac Ercig, Chloe Geeroms, Inge Pareyn, Nele Vandeputte, Leydi Carolina Pereira, Elien Roose, Karel Fostier, Gerry A. F. Nicolaes, Hans Deckmyn, Simon F. De Meyer, Karen Vanhoorelbeke^*, Kristin Jochmans

^*Corresponding author for this work

Biochemie

Research output: Contribution to journal › Article › Academic › peer-review

69 Downloads (Pure)

Abstract

IntroductionPatients suffering from congenital thrombotic thrombocytopenic purpura (cTTP) have a deficiency in ADAMTS13 due to mutations in their ADAMTS13 gene. ObjectiveThe aim of this study was to determine ADAMTS13 parameters (activity, antigen, and mutations), to investigate if the propositus suffered from child-onset cTTP, and to study the in vitro effect of the ADAMTS13 mutations. MethodsADAMTS13 activity and antigen were determined using the FRETS VWF73 assay and ELISA and ADAMTS13 mutations via sequencing of the exons. Mutant proteins were expressed in Chinese hamster ovary cells, and their expression was studied using fluorescence microscopy and ELISA. Molecular modeling was used to evaluate the effect of the mutations on ADAMTS13 structure and stability. ResultsThe propositus was diagnosed with cTTP at the age of 20. ADAMTS13 activity was below 10%, and 2 compound heterozygous mutations, the p.R498C point and the p.G259PfsX133 frameshift mutation, were identified. Expression of ADAMTS13 mutants revealed that the p.R498C and the p.G259PfsX133 mutation cause secretion and translation defects in vitro, respectively. Molecular modeling showed that the R498 intra-domain interactions are lacking in the p.R498C mutant, resulting in protein instability. ConclusionThe ADAMTS13 mutations result in a severe ADAMTS13 deficiency explaining the patient's phenotype.

Original language	English
Pages (from-to)	191-199
Number of pages	9
Journal	European Journal of Haematology
Volume	101
Issue number	2
DOIs	https://doi.org/10.1111/ejh.13094
Publication status	Published - 1 Aug 2018

Keywords

ADAMTS13
mutation
thrombotic thrombocytopenic purpura
VON-WILLEBRAND-FACTOR
FACTOR-CLEAVING PROTEASE
UPSHAW-SCHULMAN-SYNDROME
MISSENSE MUTATION
GENE
DEFICIENCY
PLASMA
MICROANGIOPATHIES
POLYMORPHISMS
PREVALENCE

Access to Document

10.1111/ejh.13094

Full text Final published version, 604 KBLicence: Taverne

Cite this

Schelpe, A.-S., Orlando, C., Ercig, B., Geeroms, C., Pareyn, I., Vandeputte, N., Pereira, L. C., Roose, E., Fostier, K., Nicolaes, G. A. F., Deckmyn, H., De Meyer, S. F., Vanhoorelbeke, K., & Jochmans, K. (2018). Child-onset thrombotic thrombocytopenic purpura caused by p.R498C and p.G259PfsX133 mutations in ADAMTS13. European Journal of Haematology, 101(2), 191-199. https://doi.org/10.1111/ejh.13094

@article{4b03cbfd920640b1b1c6397638a63ed4,

title = "Child-onset thrombotic thrombocytopenic purpura caused by p.R498C and p.G259PfsX133 mutations in ADAMTS13",

abstract = "IntroductionPatients suffering from congenital thrombotic thrombocytopenic purpura (cTTP) have a deficiency in ADAMTS13 due to mutations in their ADAMTS13 gene. ObjectiveThe aim of this study was to determine ADAMTS13 parameters (activity, antigen, and mutations), to investigate if the propositus suffered from child-onset cTTP, and to study the in vitro effect of the ADAMTS13 mutations. MethodsADAMTS13 activity and antigen were determined using the FRETS VWF73 assay and ELISA and ADAMTS13 mutations via sequencing of the exons. Mutant proteins were expressed in Chinese hamster ovary cells, and their expression was studied using fluorescence microscopy and ELISA. Molecular modeling was used to evaluate the effect of the mutations on ADAMTS13 structure and stability. ResultsThe propositus was diagnosed with cTTP at the age of 20. ADAMTS13 activity was below 10%, and 2 compound heterozygous mutations, the p.R498C point and the p.G259PfsX133 frameshift mutation, were identified. Expression of ADAMTS13 mutants revealed that the p.R498C and the p.G259PfsX133 mutation cause secretion and translation defects in vitro, respectively. Molecular modeling showed that the R498 intra-domain interactions are lacking in the p.R498C mutant, resulting in protein instability. ConclusionThe ADAMTS13 mutations result in a severe ADAMTS13 deficiency explaining the patient's phenotype.",

keywords = "ADAMTS13, mutation, thrombotic thrombocytopenic purpura, VON-WILLEBRAND-FACTOR, FACTOR-CLEAVING PROTEASE, UPSHAW-SCHULMAN-SYNDROME, MISSENSE MUTATION, GENE, DEFICIENCY, PLASMA, MICROANGIOPATHIES, POLYMORPHISMS, PREVALENCE",

author = "An-Sofie Schelpe and Christelle Orlando and Bogac Ercig and Chloe Geeroms and Inge Pareyn and Nele Vandeputte and Pereira, {Leydi Carolina} and Elien Roose and Karel Fostier and Nicolaes, {Gerry A. F.} and Hans Deckmyn and {De Meyer}, {Simon F.} and Karen Vanhoorelbeke and Kristin Jochmans",

year = "2018",

month = aug,

day = "1",

doi = "10.1111/ejh.13094",

language = "English",

volume = "101",

pages = "191--199",

journal = "European Journal of Haematology",

issn = "0902-4441",

publisher = "Wiley",

number = "2",

}

Schelpe, A-S, Orlando, C, Ercig, B, Geeroms, C, Pareyn, I, Vandeputte, N, Pereira, LC, Roose, E, Fostier, K, Nicolaes, GAF, Deckmyn, H, De Meyer, SF, Vanhoorelbeke, K & Jochmans, K 2018, 'Child-onset thrombotic thrombocytopenic purpura caused by p.R498C and p.G259PfsX133 mutations in ADAMTS13', European Journal of Haematology, vol. 101, no. 2, pp. 191-199. https://doi.org/10.1111/ejh.13094

TY - JOUR

T1 - Child-onset thrombotic thrombocytopenic purpura caused by p.R498C and p.G259PfsX133 mutations in ADAMTS13

AU - Schelpe, An-Sofie

AU - Orlando, Christelle

AU - Ercig, Bogac

AU - Geeroms, Chloe

AU - Pareyn, Inge

AU - Vandeputte, Nele

AU - Pereira, Leydi Carolina

AU - Roose, Elien

AU - Fostier, Karel

AU - Nicolaes, Gerry A. F.

AU - Deckmyn, Hans

AU - De Meyer, Simon F.

AU - Vanhoorelbeke, Karen

AU - Jochmans, Kristin

PY - 2018/8/1

Y1 - 2018/8/1

N2 - IntroductionPatients suffering from congenital thrombotic thrombocytopenic purpura (cTTP) have a deficiency in ADAMTS13 due to mutations in their ADAMTS13 gene. ObjectiveThe aim of this study was to determine ADAMTS13 parameters (activity, antigen, and mutations), to investigate if the propositus suffered from child-onset cTTP, and to study the in vitro effect of the ADAMTS13 mutations. MethodsADAMTS13 activity and antigen were determined using the FRETS VWF73 assay and ELISA and ADAMTS13 mutations via sequencing of the exons. Mutant proteins were expressed in Chinese hamster ovary cells, and their expression was studied using fluorescence microscopy and ELISA. Molecular modeling was used to evaluate the effect of the mutations on ADAMTS13 structure and stability. ResultsThe propositus was diagnosed with cTTP at the age of 20. ADAMTS13 activity was below 10%, and 2 compound heterozygous mutations, the p.R498C point and the p.G259PfsX133 frameshift mutation, were identified. Expression of ADAMTS13 mutants revealed that the p.R498C and the p.G259PfsX133 mutation cause secretion and translation defects in vitro, respectively. Molecular modeling showed that the R498 intra-domain interactions are lacking in the p.R498C mutant, resulting in protein instability. ConclusionThe ADAMTS13 mutations result in a severe ADAMTS13 deficiency explaining the patient's phenotype.

AB - IntroductionPatients suffering from congenital thrombotic thrombocytopenic purpura (cTTP) have a deficiency in ADAMTS13 due to mutations in their ADAMTS13 gene. ObjectiveThe aim of this study was to determine ADAMTS13 parameters (activity, antigen, and mutations), to investigate if the propositus suffered from child-onset cTTP, and to study the in vitro effect of the ADAMTS13 mutations. MethodsADAMTS13 activity and antigen were determined using the FRETS VWF73 assay and ELISA and ADAMTS13 mutations via sequencing of the exons. Mutant proteins were expressed in Chinese hamster ovary cells, and their expression was studied using fluorescence microscopy and ELISA. Molecular modeling was used to evaluate the effect of the mutations on ADAMTS13 structure and stability. ResultsThe propositus was diagnosed with cTTP at the age of 20. ADAMTS13 activity was below 10%, and 2 compound heterozygous mutations, the p.R498C point and the p.G259PfsX133 frameshift mutation, were identified. Expression of ADAMTS13 mutants revealed that the p.R498C and the p.G259PfsX133 mutation cause secretion and translation defects in vitro, respectively. Molecular modeling showed that the R498 intra-domain interactions are lacking in the p.R498C mutant, resulting in protein instability. ConclusionThe ADAMTS13 mutations result in a severe ADAMTS13 deficiency explaining the patient's phenotype.

KW - ADAMTS13

KW - mutation

KW - thrombotic thrombocytopenic purpura

KW - VON-WILLEBRAND-FACTOR

KW - FACTOR-CLEAVING PROTEASE

KW - UPSHAW-SCHULMAN-SYNDROME

KW - MISSENSE MUTATION

KW - GENE

KW - DEFICIENCY

KW - PLASMA

KW - MICROANGIOPATHIES

KW - POLYMORPHISMS

KW - PREVALENCE

U2 - 10.1111/ejh.13094

DO - 10.1111/ejh.13094

M3 - Article

C2 - 29763513

SN - 0902-4441

VL - 101

SP - 191

EP - 199

JO - European Journal of Haematology

JF - European Journal of Haematology

IS - 2

ER -