A novel RUNX1 exon 3 - 7 deletion causing a familial platelet disorder

Ibrahim Abdullah F Almazni; Pavel Chudakou; Alison Dawson-Meadows; Kate Downes; Kathleen Freson; Joanne Mason; Paula Page; Kim Reay; Bethan Myers; Neil Morgan

doi:10.1080/09537104.2021.1887470

A novel RUNX1 exon 3 - 7 deletion causing a familial platelet disorder

Ibrahim Abdullah F Almazni, Pavel Chudakou, Alison Dawson-Meadows, Kate Downes, Kathleen Freson, Joanne Mason, Paula Page, Kim Reay, Bethan Myers, Neil Morgan

Cardiovascular Sciences

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Abstract

Familial Platelet Disorder with associated Myeloid Malignancy (FPDMM) is a rare inherited disorder confirmed with the presence of a pathogenic germline RUNX1 variant and is thought to be heavily underdiagnosed. RUNX1 has also been found to be mutated in up to 10% of adult AML cases and other cell malignancies. We performed targeted next-generation sequencing and subsequent MLPA analysis in a kindred with multiple affected individuals with low platelet counts and a bleeding history. We detected a novel heterozygous exon 3–7 large deletion in the RUNX1 gene in all affected family members which is predicted to remove all of the Runt-homology DNA-binding domain and a portion of the Activation domain. Our results show that the combination of targeted NGS and MLPA analysis is an effective way to detect copy number variants (CNVs) which would be missed by conventional sequencing methods. This precise diagnosis offers the possibility of accurate counseling and clinical management in such patients who could go onto develop other cell malignancies.

Original language	English
Journal	Platelets
Early online date	22 Feb 2021
DOIs	https://doi.org/10.1080/09537104.2021.1887470
Publication status	E-pub ahead of print - 22 Feb 2021

Bibliographical note

Funding
This work was supported by the British Heart Foundation [FS/15/18/31317,FS/18/11/33443,PG/13/36/30275, PG/16/103/32650]; Saudi Arabia Cultural Bureau in London.

Keywords

Bleeding
CNV
NGS
RUNX1
platelet disorder
thrombocytopenia

ASJC Scopus subject areas

Hematology

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10.1080/09537104.2021.1887470Licence: None: All rights reserved

AlmazniI2021novel
This is an Accepted Manuscript version of the following article, accepted for publication in Platelets. Ibrahim Almazni, Pavel Chudakou, Alison Dawson-Meadows, Kate Downes, Kathleen Freson, Joanne Mason, Paula Page, Kim Reay, Bethan Myers & Neil V Morgan (2021) A novel RUNX1 exon 3 - 7 deletion causing a familial platelet disorder, Platelets, DOI: 10.1080/09537104.2021.1887470. It is deposited under the terms of the Creative Commons Attribution-NonCommercial-NoDerivatives License (http://creativecommons.org/licenses/by-nc-nd/4.0/), which permits non-commercial re-use, distribution, and reproduction in any medium, provided the original work is properly cited, and is not altered, transformed, or built upon in any way.
Accepted author manuscript, 741 KBLicence: Creative Commons: Attribution-NonCommercial-NoDerivs (CC BY-NC-ND)

Cite this

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title = "A novel RUNX1 exon 3 - 7 deletion causing a familial platelet disorder",

abstract = "Familial Platelet Disorder with associated Myeloid Malignancy (FPDMM) is a rare inherited disorder confirmed with the presence of a pathogenic germline RUNX1 variant and is thought to be heavily underdiagnosed. RUNX1 has also been found to be mutated in up to 10% of adult AML cases and other cell malignancies. We performed targeted next-generation sequencing and subsequent MLPA analysis in a kindred with multiple affected individuals with low platelet counts and a bleeding history. We detected a novel heterozygous exon 3–7 large deletion in the RUNX1 gene in all affected family members which is predicted to remove all of the Runt-homology DNA-binding domain and a portion of the Activation domain. Our results show that the combination of targeted NGS and MLPA analysis is an effective way to detect copy number variants (CNVs) which would be missed by conventional sequencing methods. This precise diagnosis offers the possibility of accurate counseling and clinical management in such patients who could go onto develop other cell malignancies.",

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note = "Funding This work was supported by the British Heart Foundation [FS/15/18/31317,FS/18/11/33443,PG/13/36/30275, PG/16/103/32650]; Saudi Arabia Cultural Bureau in London.",

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AU - Freson, Kathleen

AU - Mason, Joanne

AU - Page, Paula

AU - Reay, Kim

AU - Myers, Bethan

AU - Morgan, Neil

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N2 - Familial Platelet Disorder with associated Myeloid Malignancy (FPDMM) is a rare inherited disorder confirmed with the presence of a pathogenic germline RUNX1 variant and is thought to be heavily underdiagnosed. RUNX1 has also been found to be mutated in up to 10% of adult AML cases and other cell malignancies. We performed targeted next-generation sequencing and subsequent MLPA analysis in a kindred with multiple affected individuals with low platelet counts and a bleeding history. We detected a novel heterozygous exon 3–7 large deletion in the RUNX1 gene in all affected family members which is predicted to remove all of the Runt-homology DNA-binding domain and a portion of the Activation domain. Our results show that the combination of targeted NGS and MLPA analysis is an effective way to detect copy number variants (CNVs) which would be missed by conventional sequencing methods. This precise diagnosis offers the possibility of accurate counseling and clinical management in such patients who could go onto develop other cell malignancies.

AB - Familial Platelet Disorder with associated Myeloid Malignancy (FPDMM) is a rare inherited disorder confirmed with the presence of a pathogenic germline RUNX1 variant and is thought to be heavily underdiagnosed. RUNX1 has also been found to be mutated in up to 10% of adult AML cases and other cell malignancies. We performed targeted next-generation sequencing and subsequent MLPA analysis in a kindred with multiple affected individuals with low platelet counts and a bleeding history. We detected a novel heterozygous exon 3–7 large deletion in the RUNX1 gene in all affected family members which is predicted to remove all of the Runt-homology DNA-binding domain and a portion of the Activation domain. Our results show that the combination of targeted NGS and MLPA analysis is an effective way to detect copy number variants (CNVs) which would be missed by conventional sequencing methods. This precise diagnosis offers the possibility of accurate counseling and clinical management in such patients who could go onto develop other cell malignancies.

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A novel RUNX1 exon 3 - 7 deletion causing a familial platelet disorder

Abstract

Bibliographical note

Keywords

ASJC Scopus subject areas

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