Novel gene variants in patients with platelet-based bleeding using combined exome sequencing and RNAseq murine expression data

UK GAPP Study Group

doi:10.1111/jth.15119

Novel gene variants in patients with platelet-based bleeding using combined exome sequencing and RNAseq murine expression data

UK GAPP Study Group

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

2 Citations (Scopus)

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Abstract

Essentials Identifying genetic variants in platelet disorders is challenging due to its heterogenous nature. We combine WES, RNAseq, and python-based bioinformatics to identify novel gene variants. We find novel candidates in patient data by cross-referencing against a murine RNAseq model of thrombopoiesis. This innovative combined bioinformatic approach provides novel data for future research in the field. Abstract: Background The UK Genotyping and Phenotyping of Platelets study has recruited and analyzed 129 patients with suspected heritable bleeding. Previously, 55 individuals had a definitive genetic diagnosis based on whole exome sequencing (WES) and platelet morphological and functional testing. A significant challenge in this field is defining filtering criteria to identify the most likely candidate mutations for diagnosis and further study. Objective Identify candidate gene mutations for the remaining 74 patients with platelet-based bleeding with unknown genetic cause, forming the basis of future re-recruitment and further functional testing and assessment. Methods Using python-based data frame indexing, we first identify and filter all novel and rare variants using a panel of 116 genes known to cause bleeding across the full cohort of WES data. This identified new variants not previously reported in this cohort. We then index the remaining patients, with rare or novel variants in known bleeding genes against a murine RNA sequencing dataset that models proplatelet-forming megakaryocytes. Results Filtering against known genes identified candidate variants in 59 individuals, including novel variants in several known genes. In the remaining cohort of “unknown” patients, indexing against differentially expressed genes revealed candidate gene variants in several novel unreported genes, focusing on 14 patients with a severe clinical presentation. Conclusions We identified candidate mutations in a cohort of patients with no previous genetic diagnosis. This work involves innovative coupling of RNA sequencing and WES to identify candidate variants forming the basis of future study in a significant number of undiagnosed patients.

Original language	English
Pages (from-to)	262-268
Number of pages	7
Journal	Journal of Thrombosis and Haemostasis
Volume	19
Issue number	1
Early online date	6 Oct 2020
DOIs	https://doi.org/10.1111/jth.15119
Publication status	Published - Jan 2021

Bibliographical note

Funding Information:
The work in the authors' laboratories is supported by the British Heart Foundation (PG/13/36/30275; FS/15/18/31317; PG/16/103/32650; FS/18/11/33443) (N.V.M.) and the Saudi Arabia Cultural Bureau in London (I.A.). A.O.K. is a Wellcome‐funded Sir Henry Wellcome Fellow (218649/Z/19/Z). K.R.M. is supported by the National Institute of Diabetes and Digestive and Kidney Diseases (K01DK111515) at the National Institutes of Health, and is an American Society of Hematology Scholar.

Publisher Copyright:
© 2020 The Authors. Journal of Thrombosis and Haemostasis published by Wiley Periodicals LLC on behalf of International Society on Thrombosis and Haemostasis

Keywords

RNAseq
bleeding
genetics
megakaryocytes
platelets

ASJC Scopus subject areas

Hematology

Access to Document

10.1111/jth.15119Licence: Creative Commons: Attribution (CC BY)

Khan_et_al_2020_Novel_gene_variants_in_patients_Journal_of_Thrombosis_and_HaemostasisFinal published version, 876 KBLicence: Creative Commons: Attribution (CC BY)

Investigating the role of SLFN14 in megakaryocyte and platelet biology
Morgan, N. & Watson, S.
British Heart Foundation
4/06/18 → 3/06/21
Project: Research
Functional investigation of SLFN14 in megakaryocyte and platelet biology
Morgan, N. & Gough, R.
British Heart Foundation
22/08/17 → 20/02/20
Project: Research
Molecular Genetic Investigation of Patients with Congenital Thrombocytopenias
Morgan, N., Harrison, P., Lowe, G. & Watson, S.
British Heart Foundation
18/11/13 → 17/11/16
Project: Research

Cite this

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title = "Novel gene variants in patients with platelet-based bleeding using combined exome sequencing and RNAseq murine expression data",

abstract = "Essentials Identifying genetic variants in platelet disorders is challenging due to its heterogenous nature. We combine WES, RNAseq, and python-based bioinformatics to identify novel gene variants. We find novel candidates in patient data by cross-referencing against a murine RNAseq model of thrombopoiesis. This innovative combined bioinformatic approach provides novel data for future research in the field. Abstract: Background The UK Genotyping and Phenotyping of Platelets study has recruited and analyzed 129 patients with suspected heritable bleeding. Previously, 55 individuals had a definitive genetic diagnosis based on whole exome sequencing (WES) and platelet morphological and functional testing. A significant challenge in this field is defining filtering criteria to identify the most likely candidate mutations for diagnosis and further study. Objective Identify candidate gene mutations for the remaining 74 patients with platelet-based bleeding with unknown genetic cause, forming the basis of future re-recruitment and further functional testing and assessment. Methods Using python-based data frame indexing, we first identify and filter all novel and rare variants using a panel of 116 genes known to cause bleeding across the full cohort of WES data. This identified new variants not previously reported in this cohort. We then index the remaining patients, with rare or novel variants in known bleeding genes against a murine RNA sequencing dataset that models proplatelet-forming megakaryocytes. Results Filtering against known genes identified candidate variants in 59 individuals, including novel variants in several known genes. In the remaining cohort of “unknown” patients, indexing against differentially expressed genes revealed candidate gene variants in several novel unreported genes, focusing on 14 patients with a severe clinical presentation. Conclusions We identified candidate mutations in a cohort of patients with no previous genetic diagnosis. This work involves innovative coupling of RNA sequencing and WES to identify candidate variants forming the basis of future study in a significant number of undiagnosed patients.",

keywords = "RNAseq, bleeding, genetics, megakaryocytes, platelets",

author = "{UK GAPP Study Group} and Abdullah Khan and Rachel Stapley and Jeremy Pike and Susanne Wijesinghe and Jasmeet Reyat and Almazni, {Ibrahim Abdullah F} and Kellie Machlus and Neil Morgan",

note = "Funding Information: The work in the authors' laboratories is supported by the British Heart Foundation (PG/13/36/30275; FS/15/18/31317; PG/16/103/32650; FS/18/11/33443) (N.V.M.) and the Saudi Arabia Cultural Bureau in London (I.A.). A.O.K. is a Wellcome‐funded Sir Henry Wellcome Fellow (218649/Z/19/Z). K.R.M. is supported by the National Institute of Diabetes and Digestive and Kidney Diseases (K01DK111515) at the National Institutes of Health, and is an American Society of Hematology Scholar. Publisher Copyright: {\textcopyright} 2020 The Authors. Journal of Thrombosis and Haemostasis published by Wiley Periodicals LLC on behalf of International Society on Thrombosis and Haemostasis",

year = "2021",

month = jan,

doi = "10.1111/jth.15119",

language = "English",

volume = "19",

pages = "262--268",

journal = "Journal of Thrombosis and Haemostasis",

issn = "1538-7933",

publisher = "Wiley",

number = "1",

}

TY - JOUR

T1 - Novel gene variants in patients with platelet-based bleeding using combined exome sequencing and RNAseq murine expression data

AU - UK GAPP Study Group

AU - Khan, Abdullah

AU - Stapley, Rachel

AU - Pike, Jeremy

AU - Wijesinghe, Susanne

AU - Reyat, Jasmeet

AU - Almazni, Ibrahim Abdullah F

AU - Machlus, Kellie

AU - Morgan, Neil

N1 - Funding Information: The work in the authors' laboratories is supported by the British Heart Foundation (PG/13/36/30275; FS/15/18/31317; PG/16/103/32650; FS/18/11/33443) (N.V.M.) and the Saudi Arabia Cultural Bureau in London (I.A.). A.O.K. is a Wellcome‐funded Sir Henry Wellcome Fellow (218649/Z/19/Z). K.R.M. is supported by the National Institute of Diabetes and Digestive and Kidney Diseases (K01DK111515) at the National Institutes of Health, and is an American Society of Hematology Scholar. Publisher Copyright: © 2020 The Authors. Journal of Thrombosis and Haemostasis published by Wiley Periodicals LLC on behalf of International Society on Thrombosis and Haemostasis

PY - 2021/1

Y1 - 2021/1

N2 - Essentials Identifying genetic variants in platelet disorders is challenging due to its heterogenous nature. We combine WES, RNAseq, and python-based bioinformatics to identify novel gene variants. We find novel candidates in patient data by cross-referencing against a murine RNAseq model of thrombopoiesis. This innovative combined bioinformatic approach provides novel data for future research in the field. Abstract: Background The UK Genotyping and Phenotyping of Platelets study has recruited and analyzed 129 patients with suspected heritable bleeding. Previously, 55 individuals had a definitive genetic diagnosis based on whole exome sequencing (WES) and platelet morphological and functional testing. A significant challenge in this field is defining filtering criteria to identify the most likely candidate mutations for diagnosis and further study. Objective Identify candidate gene mutations for the remaining 74 patients with platelet-based bleeding with unknown genetic cause, forming the basis of future re-recruitment and further functional testing and assessment. Methods Using python-based data frame indexing, we first identify and filter all novel and rare variants using a panel of 116 genes known to cause bleeding across the full cohort of WES data. This identified new variants not previously reported in this cohort. We then index the remaining patients, with rare or novel variants in known bleeding genes against a murine RNA sequencing dataset that models proplatelet-forming megakaryocytes. Results Filtering against known genes identified candidate variants in 59 individuals, including novel variants in several known genes. In the remaining cohort of “unknown” patients, indexing against differentially expressed genes revealed candidate gene variants in several novel unreported genes, focusing on 14 patients with a severe clinical presentation. Conclusions We identified candidate mutations in a cohort of patients with no previous genetic diagnosis. This work involves innovative coupling of RNA sequencing and WES to identify candidate variants forming the basis of future study in a significant number of undiagnosed patients.

AB - Essentials Identifying genetic variants in platelet disorders is challenging due to its heterogenous nature. We combine WES, RNAseq, and python-based bioinformatics to identify novel gene variants. We find novel candidates in patient data by cross-referencing against a murine RNAseq model of thrombopoiesis. This innovative combined bioinformatic approach provides novel data for future research in the field. Abstract: Background The UK Genotyping and Phenotyping of Platelets study has recruited and analyzed 129 patients with suspected heritable bleeding. Previously, 55 individuals had a definitive genetic diagnosis based on whole exome sequencing (WES) and platelet morphological and functional testing. A significant challenge in this field is defining filtering criteria to identify the most likely candidate mutations for diagnosis and further study. Objective Identify candidate gene mutations for the remaining 74 patients with platelet-based bleeding with unknown genetic cause, forming the basis of future re-recruitment and further functional testing and assessment. Methods Using python-based data frame indexing, we first identify and filter all novel and rare variants using a panel of 116 genes known to cause bleeding across the full cohort of WES data. This identified new variants not previously reported in this cohort. We then index the remaining patients, with rare or novel variants in known bleeding genes against a murine RNA sequencing dataset that models proplatelet-forming megakaryocytes. Results Filtering against known genes identified candidate variants in 59 individuals, including novel variants in several known genes. In the remaining cohort of “unknown” patients, indexing against differentially expressed genes revealed candidate gene variants in several novel unreported genes, focusing on 14 patients with a severe clinical presentation. Conclusions We identified candidate mutations in a cohort of patients with no previous genetic diagnosis. This work involves innovative coupling of RNA sequencing and WES to identify candidate variants forming the basis of future study in a significant number of undiagnosed patients.

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Novel gene variants in patients with platelet-based bleeding using combined exome sequencing and RNAseq murine expression data

Abstract

Bibliographical note

Keywords

ASJC Scopus subject areas

Access to Document

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Projects

Investigating the role of SLFN14 in megakaryocyte and platelet biology

Functional investigation of SLFN14 in megakaryocyte and platelet biology

Molecular Genetic Investigation of Patients with Congenital Thrombocytopenias

Cite this