Somatic mutations and progressive monosomy modify SAMD9-related phenotypes in humans

Buonocore, Federica; Kühnen, Peter; Suntharalingham, Jenifer P.; Valle, Ignacio del; Digweed, Martin; Stachelscheid, Harald; Khajavi, Noushafarin; Didi, Mohammed; Brady, Angela; Blankenstein, Oliver; Procter, Annie; Dimitri, Paul; Wales, Jerry; Ghirri, Paolo; Knöbl, Dieter; Strahm, Brigitte; Erlacher, Miriam; Wlodarski, Marcin W.; Chen, Wei; Kokai, George; Anderson, Glenn; Morrogh, Deborah; Moulding, Dale; McKee, Shane; Niemeyer, Charlotte M.; Grüters, Annette; Achermann, John C.

doi:10.1172/jci91913

Cited by 136 publications

(224 citation statements)

References 32 publications

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“…In the report by Buonocore et al , two out of four patients with two mutations died very early, and the remaining two patients developed myelodysplastic syndrome with monosomy 7 3. Probably due to these reasons, the proportion of the revertant cells did not reach to 100% 3. Hence, the two patients described in this study are the first patients who achieved complete haematological reversion.…”

Section: Discussionmentioning

confidence: 55%

“…For patient 2, although we could not test whether p.Gln39* was a somatic mutation since the patient has already died, skewed X chromosome inactivation in leucocytes was shown, indicating their monoclonality. Simultaneous detection of one activating and another inactivating SAMD9 mutation in MIRAGE syndrome have already been reported by Buonocore et al ,3 although colocalisation of two mutations on the same allele was not confirmed. In the report by Buonocore et al , two out of four patients with two mutations died very early, and the remaining two patients developed myelodysplastic syndrome with monosomy 7 3.…”

Section: Discussionmentioning

confidence: 88%

“…Simultaneous detection of one activating and another inactivating SAMD9 mutation in MIRAGE syndrome have already been reported by Buonocore et al ,3 although colocalisation of two mutations on the same allele was not confirmed. In the report by Buonocore et al , two out of four patients with two mutations died very early, and the remaining two patients developed myelodysplastic syndrome with monosomy 7 3. Probably due to these reasons, the proportion of the revertant cells did not reach to 100% 3.…”

Section: Discussionmentioning

confidence: 88%

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Two patients with MIRAGE syndrome lacking haematological features: role of somatic second-site reversion SAMD9 mutations

et al. 2017

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Section: Discussionmentioning

confidence: 55%

Section: Discussionmentioning

confidence: 88%

Section: Discussionmentioning

confidence: 88%

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Two patients with MIRAGE syndrome lacking haematological features: role of somatic second-site reversion SAMD9 mutations

et al. 2017

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“…Schwartz et al [42] identified these mutations in 17% of pediatric MDS patients. Germline variants in SAMD9 and SAMD9L have been associated with multisystem disorders with a range of systemic abnormalities, including cytopenia, infection, intrauterine restriction of growth, adrenal hypoplasia, abnormal genital phenotypes, progressive cerebellar dysfunction, and enteropathy [43][44][45][46]. To date, there are no reports of expected BM morphology in mutation carriers.…”

Section: Other Recently Described Myeloid Neoplasms With Germline Prementioning

confidence: 99%

Myeloid Neoplasms with Germline Predisposition

Geyer¹

2018

Pathobiology

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The updated 2016 WHO classification of hematopoietic tumors has a new category: “myeloid neoplasms with germline predisposition.” These entities are rare, but are also currently underdiagnosed and underreported. Recognition is critical for appropriate clinical evaluation and therapy, with potential implications for the patient’s entire family. The WHO includes 3 categories of myeloid neoplasms with germline predisposition: neoplasms without preexisting conditions, neoplasms with a history of thrombocytopenia, and neoplasms with other organ dysfunction. Specialized molecular testing is frequently necessary to make the diagnosis, as the presence of one of the implicated mutations is not sufficient for diagnosis and should be confirmed with germline DNA evaluation. Many families have unique mutations that are not detected by targeted sequencing panels. Periodic bone marrow (BM) examinations are recommended to assess patients’ baseline morphology and rule out evidence of disease progression. Thus, accurate diagnosis requires a careful recording of clinical history, a BM morphology evaluation, and advanced molecular testing.

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“…The genes implicated are diverse, including well-known hematopoietic transcription factors such as CEBPA, GATA2, and RUNX1 as well as genes such as BRCA1 and MSH6 , more traditionally thought of as solid tumor risk genes [10]. The most recently identified genes, DDX41, SAMD9 and SAMD9L , are revealing novel pathways involved in leukemogenesis and deepening our understanding of the basic biology of MDS/AML [11–13]. In recognition of the impact of this growing field on clinical care, the World Health Organization, European Leukemia Net, and National Comprehensive Cancer Network have all recently incorporated consideration of MDS/AML germ line predisposition syndromes into MDS/AML classification and clinical management guidelines, making knowledge of these syndromes now essential for clinicians and pathologists alike [14–16].…”

Section: Inherited Genetics In Myelodysplastic Syndrome and Acute Myementioning

confidence: 99%

Familial myelodysplastic syndrome/acute myeloid leukemia

Churpek

2017

Best Practice & Research Clinical Haematology

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A growing number of inherited genetic loci that contribute to myelodysplastic syndrome/acute myeloid leukemia (MDS/AML) development in both children as well as adults are rapidly being identified. In recognition of the clinical impact of this emerging field, the World Health Organization, National Comprehensive Cancer Network, and European LeukemiaNet have all added consideration of inherited predisposition to MDS/AML classification and management. Study of these disorders is providing unique insight into the biology of both sporadic and familial MDS/AML. International collaborative efforts to store germline tissue, document family histories, and pool data are essential to progress in diagnosing and treating both hereditary and sporadic forms of MDS/AML.

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Somatic mutations and progressive monosomy modify SAMD9-related phenotypes in humans

Cited by 136 publications

References 32 publications

Two patients with MIRAGE syndrome lacking haematological features: role of somatic second-site reversion SAMD9 mutations

Two patients with MIRAGE syndrome lacking haematological features: role of somatic second-site reversion SAMD9 mutations

Myeloid Neoplasms with Germline Predisposition

Familial myelodysplastic syndrome/acute myeloid leukemia

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