Hematopoietic stem cell and progenitor cell mechanisms in myelodysplastic syndromes

Pang, Wendy W.; Pluvinage, John V.; Price, Elizabeth; Sridhar, Kunju; Arber, Daniel A.; Greenberg, Peter L.; Schrier, Stanley L.; Park, Christopher Y.; Weissman, Irving L.

doi:10.1073/pnas.1222861110

Cited by 234 publications

(281 citation statements)

References 39 publications

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“…We recently showed that the HSCs in MDS that show a clonal pathogenic chromosomal event such as 5q-or monosomy 7 expand at the expense of normal HSCs, just as we had shown in CML (240). But the progeny of these hypercompetitive HSCs produce progenitors that are phagocytosed, likely to be responsible for the loss in blood of red blood cells and/or granulocytes and/or platelets (240). So MDS is a prototype of preleukemic progression wherein the successful clone has blocked programmed cell death, but its oligolineage progeny, also highly viable, can, in a stage-specific manner, express cell surface calreticulin and are phagocytosed in a calreticulin-dependent event (240).…”

Section: Cancer Stem Cells and The Therapeutics That Come From Them: mentioning

confidence: 59%

“…Now we knew that it was the "eat me" signal that was expressed on the surface of all AML cells. We showed later that calreticulin was expressed on the surface of the GMP and erythrocyte progenitor cells in the marrow of patients with myelodysplastic syndrome (MDS), and we showed that, as a consequence, their frequency relative to other marrow cells was significantly diminished (240). We recently showed that the HSCs in MDS that show a clonal pathogenic chromosomal event such as 5q-or monosomy 7 expand at the expense of normal HSCs, just as we had shown in CML (240).…”

Section: Cancer Stem Cells and The Therapeutics That Come From Them: mentioning

confidence: 68%

“…We showed later that calreticulin was expressed on the surface of the GMP and erythrocyte progenitor cells in the marrow of patients with myelodysplastic syndrome (MDS), and we showed that, as a consequence, their frequency relative to other marrow cells was significantly diminished (240). We recently showed that the HSCs in MDS that show a clonal pathogenic chromosomal event such as 5q-or monosomy 7 expand at the expense of normal HSCs, just as we had shown in CML (240). But the progeny of these hypercompetitive HSCs produce progenitors that are phagocytosed, likely to be responsible for the loss in blood of red blood cells and/or granulocytes and/or platelets (240).…”

Section: Cancer Stem Cells and The Therapeutics That Come From Them: mentioning

confidence: 95%

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How One Thing Led to Another

Weissman

2016

Annu. Rev. Immunol.

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I started research in high school, experimenting on immunological tolerance to transplantation antigens. This led to studies of the thymus as the site of maturation of T cells, which led to the discovery, isolation, and clinical transplantation of purified hematopoietic stem cells (HSCs). The induction of immune tolerance with HSCs has led to isolation of other tissue-specific stem cells for regenerative medicine. Our studies of circulating competing germline stem cells in colonial protochordates led us to document competing HSCs. In human acute myelogenous leukemia we showed that all preleukemic mutations occur in HSCs, and determined their order; the final mutations occur in a multipotent progenitor derived from the preleukemic HSC clone. With these, we discovered that CD47 is an upregulated gene in all human cancers and is a “don't eat me” signal; blocking it with antibodies leads to cancer cell phagocytosis. CD47 is the first known gene common to all cancers and is a target for cancer immunotherapy.

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Section: Cancer Stem Cells and The Therapeutics That Come From Them: mentioning

confidence: 59%

Section: Cancer Stem Cells and The Therapeutics That Come From Them: mentioning

confidence: 68%

Section: Cancer Stem Cells and The Therapeutics That Come From Them: mentioning

confidence: 95%

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How One Thing Led to Another

Weissman

2016

Annu. Rev. Immunol.

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“…[1][2][3] Despite their genetic heterogeneity, they share common phenotypic features including low peripheral blood counts (cytopenias) in spite of a hypercellular bone marrow (ineffective hematopoiesis), dysplasia and a variable propensity for transformation to acute myeloid leukemia (AML). 4 Programmed cell death or apoptosis of white blood cells is a common feature, and is thought to contribute to the cytopenias particularly in early stages of the disease.…”

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confidence: 99%

PUMA promotes apoptosis of hematopoietic progenitors driving leukemic progression in a mouse model of myelodysplasia

et al. 2016

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Myelodysplastic syndrome (MDS) is characterized by ineffective hematopoiesis with resultant cytopenias. Increased apoptosis and aberrantly functioning progenitors are thought to contribute to this phenotype. As is the case for other malignancies, overcoming apoptosis is believed to be important in progression toward acute myeloid leukemia (AML). Using the NUP98-HOXD13 (NHD13) transgenic mouse model of MDS, we previously reported that overexpression of the anti-apoptotic protein BCL2, blocked apoptosis and improved cytopenias, paradoxically, delaying leukemic progression. To further understand this surprising result, we examined the role of p53 and its pro-apoptotic effectors, PUMA and NOXA in NHD13 mice. The absence of p53 or PUMA but not NOXA reduced apoptosis and expanded the numbers of MDS-repopulating cells. Despite a similar effect on apoptosis and cell numbers, the absence of p53 and PUMA had diametrically opposed effects on progression to AML: absence of p53 accelerated leukemic progression, while absence of PUMA significantly delayed progression. This may be explained in part by differences in cellular responses to DNA damage. The absence of p53 led to higher levels of γ-H2AX (indicative of persistent DNA lesions) while PUMA-deficient NHD13 progenitors resolved DNA lesions in a manner comparable to wild-type cells. These results suggest that targeting PUMA may improve the cytopenias of MDS without a detrimental effect on leukemic progression thus warranting further investigation. Cell Death and Differentiation (2016) 23, 1049-1059 doi:10.1038/cdd.2015; published online 8 January 2016Myelodysplastic syndromes (MDS) are a genetically and clonally heterogeneous group of myeloid malignancies, likely arising from the hematopoietic stem cell. 1-3 Despite their genetic heterogeneity, they share common phenotypic features including low peripheral blood counts (cytopenias) in spite of a hypercellular bone marrow (ineffective hematopoiesis), dysplasia and a variable propensity for transformation to acute myeloid leukemia (AML). 4 Programmed cell death or apoptosis of white blood cells is a common feature, and is thought to contribute to the cytopenias particularly in early stages of the disease. The basis of ineffective hematopoiesis in MDS may also lie in the dysfunction of hematopoietic progenitors and their inability to support adequate bone marrow function. Apoptosis can be triggered by extrinsic factors, such as FAS ligand or TNF-α, or by cell-intrinsic factors such as ribosomal stress or increased reactive oxygen species. A cell extrinsic mechanism for apoptosis in MDS has been favored for many years; 5 however, recent evidence suggests a cell-intrinsic trigger, especially in del(5q) MDS for which there is evidence for activation of the tumor suppressor p53 by ribosomal dysfunction. 6,7 More aggressive stages of MDS have less apoptosis than earlier stages, 8 supporting the paradigm that acquired resistance to apoptosis of malignant progenitors is an important step in cancer progression. 9 Among hematological...

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“…Deren genetische Instabilität ist die Grundlage für den Erwerb einer Vielzahl weiterer Mutationen, die mit dem Verlust der normalen Differenzierungskapazität schließlich funktionell zu einer dysplastischen und ineffektiven Hämatopoese führen [2]. Allerdings findet sich in Kollektiven älterer (>70 Jahre), asymptomatischer Personen bei einem Anteil von bis zu 10 % der Nachweis einer klonal veränderten Hämatopoese, deren klinische Bedeutung gegenwärtig unklar ist [3].…”

Section: » Klinische Hauptphänomene Sind Anämie Erhöhte Blutungsbereunclassified