Spectrum of hematological malignancies, clonal evolution and outcomes in 144 Mayo Clinic patients with germline predisposition syndromes

Emma St Martin; Alejandro Ferrer; Abhishek A. Mangaonkar; Shakila P. Khan; Mira A. Kohorst; Avni Y. Joshi; William J. Hogan; Horatiu Olteanu; Ann M. Moyer; Aref Al-Kali; Ayalew Tefferi; Dong Chen; Kitsada Wudhikarn; Ronald Go; David Viswanatha; Rong He; Rhett Ketterling; Phuong L. Nguyen; Jennifer L. Oliveira; Naseema Gangat; Terra Lasho; Mrinal M. Patnaik

doi:10.1002/ajh.26321

Spectrum of hematological malignancies, clonal evolution and outcomes in 144 Mayo Clinic patients with germline predisposition syndromes

Emma St Martin, Alejandro Ferrer, Abhishek A. Mangaonkar, Shakila P. Khan, Mira A. Kohorst, Avni Y. Joshi, William J. Hogan, Horatiu Olteanu, Ann M. Moyer, Aref Al-Kali, Ayalew Tefferi, Dong Chen, Kitsada Wudhikarn, Ronald Go, David Viswanatha, Rong He, Rhett Ketterling, Phuong L. Nguyen, Jennifer L. Oliveira, Naseema GangatTerra Lasho, Mrinal M. Patnaik

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

Abstract

Germline predisposition syndromes (GPS) result from constitutional aberrations in tumor suppressive and homeostatic genes, increasing risk for neoplasia in affected kindred. In this study, we present clinical and genomic data on 144 Mayo Clinic patients with GPS; 59 evaluated prospectively using an algorithm-based diagnostic approach in the setting of a dedicated GPS/ inherited bone marrow failure syndrome (IBMFS) clinic. Seventy-two (50%) patients had IBMFS (telomere biology disorders-32,Fanconi anemia-18, Diamond Blackfan Anemia – 11, congenital neutropenia–5, Schwachman-Diamond Syndrome-5 and Bloom Syndrome-1), 27 (19%) had GPS with antecedent thrombocytopenia (RUNX1-FPD-15, ANKRD26-6, ETV6-2, GATA1-1, MPL-3), 28 (19%) had GPS without antecedent thrombocytopenia (GATA2 haploinsufficiency-16, DDX41-10, CBL-1 and CEBPA-1) and 17 (12%) had general cancer predisposition syndromes (ataxia telangiectasia-7, heterozygous ATM variants-3, CHEK2-2, TP53-2, CDK2NA-1, NF1-1 and Nijmegen Breakage Syndrome-1). Homozygous and heterozygous ATM pathogenic variants were exclusively associated with lymphoproliferative disorders (LPD), while DDX41 GPS was associated with LPD and myeloid neoplasms. The use of somatic NGS-testing identified clonal evolution in GPS patients, with ASXL1, RAS pathway genes, SRSF2 and TET2 being most frequently mutated. Fifty-two (91%) of 59 prospectively identified GPS patients had a change in their management approach, including additional GPS-related screening in 42 (71%), referral for allogenic HSCT workup and screening of related donors in 16 (27%), medication initiation and selection of specific conditioning regimens in 14 (24%), and genetic counseling with specific intent of fertility preservation and preconceptual counseling in 10 (17%) patients; highlighting the importance of dedicated GPS screening, detection and management programs for patients with hematological neoplasms.

Original language	English (US)
Pages (from-to)	1450-1460
Number of pages	11
Journal	American journal of hematology
Volume	96
Issue number	11
DOIs	https://doi.org/10.1002/ajh.26321
State	Published - Nov 1 2021

ASJC Scopus subject areas

Hematology

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Martin, E. S., Ferrer, A., Mangaonkar, A. A., Khan, S. P., Kohorst, M. A., Joshi, A. Y., Hogan, W. J., Olteanu, H., Moyer, A. M., Al-Kali, A., Tefferi, A., Chen, D., Wudhikarn, K., Go, R., Viswanatha, D., He, R., Ketterling, R., Nguyen, P. L., Oliveira, J. L., ... Patnaik, M. M. (2021). Spectrum of hematological malignancies, clonal evolution and outcomes in 144 Mayo Clinic patients with germline predisposition syndromes. American journal of hematology, 96(11), 1450-1460. https://doi.org/10.1002/ajh.26321

Martin, ES, Ferrer, A, Mangaonkar, AA, Khan, SP, Kohorst, MA, Joshi, AY, Hogan, WJ, Olteanu, H, Moyer, AM, Al-Kali, A, Tefferi, A, Chen, D, Wudhikarn, K, Go, R, Viswanatha, D, He, R, Ketterling, R, Nguyen, PL, Oliveira, JL, Gangat, N, Lasho, T & Patnaik, MM 2021, 'Spectrum of hematological malignancies, clonal evolution and outcomes in 144 Mayo Clinic patients with germline predisposition syndromes', American journal of hematology, vol. 96, no. 11, pp. 1450-1460. https://doi.org/10.1002/ajh.26321

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title = "Spectrum of hematological malignancies, clonal evolution and outcomes in 144 Mayo Clinic patients with germline predisposition syndromes",

abstract = "Germline predisposition syndromes (GPS) result from constitutional aberrations in tumor suppressive and homeostatic genes, increasing risk for neoplasia in affected kindred. In this study, we present clinical and genomic data on 144 Mayo Clinic patients with GPS; 59 evaluated prospectively using an algorithm-based diagnostic approach in the setting of a dedicated GPS/ inherited bone marrow failure syndrome (IBMFS) clinic. Seventy-two (50%) patients had IBMFS (telomere biology disorders-32,Fanconi anemia-18, Diamond Blackfan Anemia – 11, congenital neutropenia–5, Schwachman-Diamond Syndrome-5 and Bloom Syndrome-1), 27 (19%) had GPS with antecedent thrombocytopenia (RUNX1-FPD-15, ANKRD26-6, ETV6-2, GATA1-1, MPL-3), 28 (19%) had GPS without antecedent thrombocytopenia (GATA2 haploinsufficiency-16, DDX41-10, CBL-1 and CEBPA-1) and 17 (12%) had general cancer predisposition syndromes (ataxia telangiectasia-7, heterozygous ATM variants-3, CHEK2-2, TP53-2, CDK2NA-1, NF1-1 and Nijmegen Breakage Syndrome-1). Homozygous and heterozygous ATM pathogenic variants were exclusively associated with lymphoproliferative disorders (LPD), while DDX41 GPS was associated with LPD and myeloid neoplasms. The use of somatic NGS-testing identified clonal evolution in GPS patients, with ASXL1, RAS pathway genes, SRSF2 and TET2 being most frequently mutated. Fifty-two (91%) of 59 prospectively identified GPS patients had a change in their management approach, including additional GPS-related screening in 42 (71%), referral for allogenic HSCT workup and screening of related donors in 16 (27%), medication initiation and selection of specific conditioning regimens in 14 (24%), and genetic counseling with specific intent of fertility preservation and preconceptual counseling in 10 (17%) patients; highlighting the importance of dedicated GPS screening, detection and management programs for patients with hematological neoplasms.",

author = "Martin, {Emma St} and Alejandro Ferrer and Mangaonkar, {Abhishek A.} and Khan, {Shakila P.} and Kohorst, {Mira A.} and Joshi, {Avni Y.} and Hogan, {William J.} and Horatiu Olteanu and Moyer, {Ann M.} and Aref Al-Kali and Ayalew Tefferi and Dong Chen and Kitsada Wudhikarn and Ronald Go and David Viswanatha and Rong He and Rhett Ketterling and Nguyen, {Phuong L.} and Oliveira, {Jennifer L.} and Naseema Gangat and Terra Lasho and Patnaik, {Mrinal M.}",

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year = "2021",

month = nov,

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doi = "10.1002/ajh.26321",

language = "English (US)",

volume = "96",

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T1 - Spectrum of hematological malignancies, clonal evolution and outcomes in 144 Mayo Clinic patients with germline predisposition syndromes

AU - Martin, Emma St

AU - Ferrer, Alejandro

AU - Mangaonkar, Abhishek A.

AU - Khan, Shakila P.

AU - Kohorst, Mira A.

AU - Joshi, Avni Y.

AU - Hogan, William J.

AU - Olteanu, Horatiu

AU - Moyer, Ann M.

AU - Al-Kali, Aref

AU - Tefferi, Ayalew

AU - Chen, Dong

AU - Wudhikarn, Kitsada

AU - Go, Ronald

AU - Viswanatha, David

AU - He, Rong

AU - Ketterling, Rhett

AU - Nguyen, Phuong L.

AU - Oliveira, Jennifer L.

AU - Gangat, Naseema

AU - Lasho, Terra

AU - Patnaik, Mrinal M.

PY - 2021/11/1

Y1 - 2021/11/1

N2 - Germline predisposition syndromes (GPS) result from constitutional aberrations in tumor suppressive and homeostatic genes, increasing risk for neoplasia in affected kindred. In this study, we present clinical and genomic data on 144 Mayo Clinic patients with GPS; 59 evaluated prospectively using an algorithm-based diagnostic approach in the setting of a dedicated GPS/ inherited bone marrow failure syndrome (IBMFS) clinic. Seventy-two (50%) patients had IBMFS (telomere biology disorders-32,Fanconi anemia-18, Diamond Blackfan Anemia – 11, congenital neutropenia–5, Schwachman-Diamond Syndrome-5 and Bloom Syndrome-1), 27 (19%) had GPS with antecedent thrombocytopenia (RUNX1-FPD-15, ANKRD26-6, ETV6-2, GATA1-1, MPL-3), 28 (19%) had GPS without antecedent thrombocytopenia (GATA2 haploinsufficiency-16, DDX41-10, CBL-1 and CEBPA-1) and 17 (12%) had general cancer predisposition syndromes (ataxia telangiectasia-7, heterozygous ATM variants-3, CHEK2-2, TP53-2, CDK2NA-1, NF1-1 and Nijmegen Breakage Syndrome-1). Homozygous and heterozygous ATM pathogenic variants were exclusively associated with lymphoproliferative disorders (LPD), while DDX41 GPS was associated with LPD and myeloid neoplasms. The use of somatic NGS-testing identified clonal evolution in GPS patients, with ASXL1, RAS pathway genes, SRSF2 and TET2 being most frequently mutated. Fifty-two (91%) of 59 prospectively identified GPS patients had a change in their management approach, including additional GPS-related screening in 42 (71%), referral for allogenic HSCT workup and screening of related donors in 16 (27%), medication initiation and selection of specific conditioning regimens in 14 (24%), and genetic counseling with specific intent of fertility preservation and preconceptual counseling in 10 (17%) patients; highlighting the importance of dedicated GPS screening, detection and management programs for patients with hematological neoplasms.

AB - Germline predisposition syndromes (GPS) result from constitutional aberrations in tumor suppressive and homeostatic genes, increasing risk for neoplasia in affected kindred. In this study, we present clinical and genomic data on 144 Mayo Clinic patients with GPS; 59 evaluated prospectively using an algorithm-based diagnostic approach in the setting of a dedicated GPS/ inherited bone marrow failure syndrome (IBMFS) clinic. Seventy-two (50%) patients had IBMFS (telomere biology disorders-32,Fanconi anemia-18, Diamond Blackfan Anemia – 11, congenital neutropenia–5, Schwachman-Diamond Syndrome-5 and Bloom Syndrome-1), 27 (19%) had GPS with antecedent thrombocytopenia (RUNX1-FPD-15, ANKRD26-6, ETV6-2, GATA1-1, MPL-3), 28 (19%) had GPS without antecedent thrombocytopenia (GATA2 haploinsufficiency-16, DDX41-10, CBL-1 and CEBPA-1) and 17 (12%) had general cancer predisposition syndromes (ataxia telangiectasia-7, heterozygous ATM variants-3, CHEK2-2, TP53-2, CDK2NA-1, NF1-1 and Nijmegen Breakage Syndrome-1). Homozygous and heterozygous ATM pathogenic variants were exclusively associated with lymphoproliferative disorders (LPD), while DDX41 GPS was associated with LPD and myeloid neoplasms. The use of somatic NGS-testing identified clonal evolution in GPS patients, with ASXL1, RAS pathway genes, SRSF2 and TET2 being most frequently mutated. Fifty-two (91%) of 59 prospectively identified GPS patients had a change in their management approach, including additional GPS-related screening in 42 (71%), referral for allogenic HSCT workup and screening of related donors in 16 (27%), medication initiation and selection of specific conditioning regimens in 14 (24%), and genetic counseling with specific intent of fertility preservation and preconceptual counseling in 10 (17%) patients; highlighting the importance of dedicated GPS screening, detection and management programs for patients with hematological neoplasms.

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Spectrum of hematological malignancies, clonal evolution and outcomes in 144 Mayo Clinic patients with germline predisposition syndromes

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