Clinton J. V. Campbell scite author profile

Acute myeloid leukaemia (AML) is distinguished by the generation of dysfunctional leukaemic blasts, and patients characteristically suffer from fatal infections and anaemia due to insufficient normal myelo-erythropoiesis. Direct physical crowding of bone marrow (BM) by accumulating leukaemic cells does not fully account for this haematopoietic failure. Here, analyses from AML patients were applied to both in vitro co-culture platforms and in vivo xenograft modelling, revealing that human AML disease specifically disrupts the adipocytic niche in BM. Leukaemic suppression of BM adipocytes led to imbalanced regulation of endogenous haematopoietic stem and progenitor cells, resulting in impaired myelo-erythroid maturation. In vivo administration of PPARγ agonists induced BM adipogenesis, which rescued healthy haematopoietic maturation while repressing leukaemic growth. Our study identifies a previously unappreciated axis between BM adipogenesis and normal myelo-erythroid maturation that is therapeutically accessible to improve symptoms of BM failure in AML via non-cell autonomous targeting of the niche.

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tBid Undergoes Multiple Conformational Changes at the Membrane Required for Bax Activation

Shamas‐Din¹,

Bindner²,

Zhu³

et al. 2013

Journal of Biological Chemistry

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Background: tBid is a Bcl-2 family protein that promotes apoptosis at the mitochondria. Results: tBid undergoes a reversible conformational change at membranes before activation that is accelerated by Mtch2. Conclusion: The Mtch2 accelerated conformational change in membrane-bound tBid enables it to activate Bax. Significance: The conformational change in tBid is a novel potential site of apoptosis regulation.

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Regional Localization within the Bone Marrow Influences the Functional Capacity of Human HSCs

et al. 2013

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Numerous studies have shown that the bone marrow (BM) niche plays a key role in mouse hematopoietic stem cell (HSC) function and involves contributions from a broad array of cell types. However, the composition and role of the human BM HSC niche have not been investigated. Here, using human bone biopsy specimens, we provide evidence of HSC propensity to localize to endosteal regions of the trabecular bone area (TBA). Through functional xenograft transplantation, we found that human HSCs localizing to the TBA have superior regenerative and self-renewal capacity and are molecularly distinct from those localizing to the long bone area (LBA). In addition, osteoblasts in the TBA possess unique characteristics and express a key network of factors that regulate TBA- versus LBA-localized human HSCs in vivo. Our study reveals that BM localization and architecture play a critical role in defining the functional and molecular properties of human HSCs.

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Fine-Tuning and training of densenet for histopathology image representation using TCGA diagnostic slides

Riasatian

Babaie

Maleki

et al. 2021

Medical Image Analysis

125

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Yottixel – An Image Search Engine for Large Archives of Histopathology Whole Slide Images

Kalra

Tizhoosh

Choi

et al. 2020

Medical Image Analysis

106

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