Bone marrow failure unresponsive to bone marrow transplant is caused by mutations in thrombopoietin

Aaron Seo; Miri Ben-Harosh; Mehtap Sirin; Jerry Stein; Orly Dgany; Joseph Kaplelushnik; Manfred Hoenig; Ulrich Pannicke; Myriam Lorenz; Klaus Schwarz; Clemens Stockklausner; Tom Walsh; Suleyman Gulsuner; Ming K. Lee; Anoop Sendamarai; Marilyn Sanchez-Bonilla; Mary Claire King; Holger Cario; Andreas E. Kulozik; Klaus Michael Debatin; Ansgar Schulz; Hannah Tamary; Akiko Shimamura

doi:10.1182/blood-2017-02-768036

Bone marrow failure unresponsive to bone marrow transplant is caused by mutations in thrombopoietin

Aaron Seo, Miri Ben-Harosh, Mehtap Sirin, Jerry Stein, Orly Dgany, Joseph Kaplelushnik, Manfred Hoenig, Ulrich Pannicke, Myriam Lorenz, Klaus Schwarz, Clemens Stockklausner, Tom Walsh, Suleyman Gulsuner, Ming K. Lee, Anoop Sendamarai, Marilyn Sanchez-Bonilla, Mary Claire King, Holger Cario, Andreas E. Kulozik, Klaus Michael DebatinAnsgar Schulz, Hannah Tamary, Akiko Shimamura^*

^*Corresponding author for this work

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

48 Scopus citations

Abstract

We report 5 individuals in 3 unrelated families with severe thrombocytopenia progressing to trilineage bone marrow failure (BMF). Four of the children received hematopoietic stem cell transplants and all showed poor graft function with persistent severe cytopenias even after repeated transplants with different donors. Exome and targeted sequencing identified mutations in the gene encoding thrombopoietin (THPO): THPO R99W, homozygous in affected children in 2 families, and THPO R157X, homozygous in the affected child in the third family. Both mutations result in a lack of THPO in the patients’ serum. For the 2 surviving patients, improvement in trilineage hematopoiesis was achieved following treatment with a THPO receptor agonist. These studies demonstrate that biallelic loss-of-function mutations in THPO cause BMF, which is unresponsive to transplant due to a hematopoietic cell-extrinsic mechanism. These studies provide further support for the critical role of the MPL-THPO pathway in hematopoiesis and highlight the importance of accurate genetic diagnosis to inform treatment decisions for BMF.

Original language	English
Pages (from-to)	875-880
Number of pages	6
Journal	Blood
Volume	130
Issue number	7
DOIs	https://doi.org/10.1182/blood-2017-02-768036
State	Published - 17 Aug 2017

Funding

Funders	Funder number
Ghiglione Aplastic Anemia Fund
NIH National Institute of General Medical Sciences
National Health and Medical Research Council of Australia
National Institutes of Health
National Institute of General Medical Sciences	T32GM007266
National Institute of Diabetes and Digestive and Kidney Diseases	R24DK099808, F30DK103462
Achievement Rewards for College Scientists Foundation
Eunice Kennedy Shriver National Institute of Child Health and Human Development	T32HD007183
Seattle Children’s Hospital
Australian National University
Israel Cancer Association

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Seo, A., Ben-Harosh, M., Sirin, M., Stein, J., Dgany, O., Kaplelushnik, J., Hoenig, M., Pannicke, U., Lorenz, M., Schwarz, K., Stockklausner, C., Walsh, T., Gulsuner, S., Lee, M. K., Sendamarai, A., Sanchez-Bonilla, M., King, M. C., Cario, H., Kulozik, A. E., ... Shimamura, A. (2017). Bone marrow failure unresponsive to bone marrow transplant is caused by mutations in thrombopoietin. Blood, 130(7), 875-880. https://doi.org/10.1182/blood-2017-02-768036

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title = "Bone marrow failure unresponsive to bone marrow transplant is caused by mutations in thrombopoietin",

abstract = "We report 5 individuals in 3 unrelated families with severe thrombocytopenia progressing to trilineage bone marrow failure (BMF). Four of the children received hematopoietic stem cell transplants and all showed poor graft function with persistent severe cytopenias even after repeated transplants with different donors. Exome and targeted sequencing identified mutations in the gene encoding thrombopoietin (THPO): THPO R99W, homozygous in affected children in 2 families, and THPO R157X, homozygous in the affected child in the third family. Both mutations result in a lack of THPO in the patients{\textquoteright} serum. For the 2 surviving patients, improvement in trilineage hematopoiesis was achieved following treatment with a THPO receptor agonist. These studies demonstrate that biallelic loss-of-function mutations in THPO cause BMF, which is unresponsive to transplant due to a hematopoietic cell-extrinsic mechanism. These studies provide further support for the critical role of the MPL-THPO pathway in hematopoiesis and highlight the importance of accurate genetic diagnosis to inform treatment decisions for BMF.",

author = "Aaron Seo and Miri Ben-Harosh and Mehtap Sirin and Jerry Stein and Orly Dgany and Joseph Kaplelushnik and Manfred Hoenig and Ulrich Pannicke and Myriam Lorenz and Klaus Schwarz and Clemens Stockklausner and Tom Walsh and Suleyman Gulsuner and Lee, {Ming K.} and Anoop Sendamarai and Marilyn Sanchez-Bonilla and King, {Mary Claire} and Holger Cario and Kulozik, {Andreas E.} and Debatin, {Klaus Michael} and Ansgar Schulz and Hannah Tamary and Akiko Shimamura",

note = "Publisher Copyright: {\textcopyright} 2017 by The American Society of Hematology.",

year = "2017",

month = aug,

day = "17",

doi = "10.1182/blood-2017-02-768036",

language = "אנגלית",

volume = "130",

pages = "875--880",

journal = "Blood",

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publisher = "Elsevier B.V.",

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Seo, A, Ben-Harosh, M, Sirin, M, Stein, J, Dgany, O, Kaplelushnik, J, Hoenig, M, Pannicke, U, Lorenz, M, Schwarz, K, Stockklausner, C, Walsh, T, Gulsuner, S, Lee, MK, Sendamarai, A, Sanchez-Bonilla, M, King, MC, Cario, H, Kulozik, AE, Debatin, KM, Schulz, A, Tamary, H & Shimamura, A 2017, 'Bone marrow failure unresponsive to bone marrow transplant is caused by mutations in thrombopoietin', Blood, vol. 130, no. 7, pp. 875-880. https://doi.org/10.1182/blood-2017-02-768036

TY - JOUR

T1 - Bone marrow failure unresponsive to bone marrow transplant is caused by mutations in thrombopoietin

AU - Seo, Aaron

AU - Ben-Harosh, Miri

AU - Sirin, Mehtap

AU - Stein, Jerry

AU - Dgany, Orly

AU - Kaplelushnik, Joseph

AU - Hoenig, Manfred

AU - Pannicke, Ulrich

AU - Lorenz, Myriam

AU - Schwarz, Klaus

AU - Stockklausner, Clemens

AU - Walsh, Tom

AU - Gulsuner, Suleyman

AU - Lee, Ming K.

AU - Sendamarai, Anoop

AU - Sanchez-Bonilla, Marilyn

AU - King, Mary Claire

AU - Cario, Holger

AU - Kulozik, Andreas E.

AU - Debatin, Klaus Michael

AU - Schulz, Ansgar

AU - Tamary, Hannah

AU - Shimamura, Akiko

PY - 2017/8/17

Y1 - 2017/8/17

N2 - We report 5 individuals in 3 unrelated families with severe thrombocytopenia progressing to trilineage bone marrow failure (BMF). Four of the children received hematopoietic stem cell transplants and all showed poor graft function with persistent severe cytopenias even after repeated transplants with different donors. Exome and targeted sequencing identified mutations in the gene encoding thrombopoietin (THPO): THPO R99W, homozygous in affected children in 2 families, and THPO R157X, homozygous in the affected child in the third family. Both mutations result in a lack of THPO in the patients’ serum. For the 2 surviving patients, improvement in trilineage hematopoiesis was achieved following treatment with a THPO receptor agonist. These studies demonstrate that biallelic loss-of-function mutations in THPO cause BMF, which is unresponsive to transplant due to a hematopoietic cell-extrinsic mechanism. These studies provide further support for the critical role of the MPL-THPO pathway in hematopoiesis and highlight the importance of accurate genetic diagnosis to inform treatment decisions for BMF.

AB - We report 5 individuals in 3 unrelated families with severe thrombocytopenia progressing to trilineage bone marrow failure (BMF). Four of the children received hematopoietic stem cell transplants and all showed poor graft function with persistent severe cytopenias even after repeated transplants with different donors. Exome and targeted sequencing identified mutations in the gene encoding thrombopoietin (THPO): THPO R99W, homozygous in affected children in 2 families, and THPO R157X, homozygous in the affected child in the third family. Both mutations result in a lack of THPO in the patients’ serum. For the 2 surviving patients, improvement in trilineage hematopoiesis was achieved following treatment with a THPO receptor agonist. These studies demonstrate that biallelic loss-of-function mutations in THPO cause BMF, which is unresponsive to transplant due to a hematopoietic cell-extrinsic mechanism. These studies provide further support for the critical role of the MPL-THPO pathway in hematopoiesis and highlight the importance of accurate genetic diagnosis to inform treatment decisions for BMF.

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DO - 10.1182/blood-2017-02-768036

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C2 - 28559357

AN - SCOPUS:85027871624

SN - 0006-4971

VL - 130

SP - 875

EP - 880

JO - Blood

JF - Blood

IS - 7

ER -

Bone marrow failure unresponsive to bone marrow transplant is caused by mutations in thrombopoietin

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