Publications by authors named "R Hurren"

ClpXP is a two-component mitochondrial matrix protease. The caseinolytic mitochondrial matrix peptidase chaperone subunit X (ClpX) recognizes and translocates protein substrates into the degradation chamber of the caseinolytic protease P (ClpP) for proteolysis. ClpXP degrades damaged respiratory chain proteins and is necessary for cancer cell survival.

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Resistance to chemotherapy remains a major hurdle to the cure of Acute Myeloid Leukemia (AML) patients. Recent studies indicate a minority of malignant cells, termed drug-tolerant persisters (DTPs), stochastically upregulate stress pathways to evade cell death upon acute exposure to chemotherapy without acquiring new genetic mutations. This chemoresistant state is transient and the cells return to baseline after removal of chemotherapy.

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Micronuclei (MN) are induced by various genotoxic stressors and amass nuclear- and cytoplasmic-resident proteins, priming the cell for MN-driven signaling cascades. Here, we measured the proteome of micronuclear, cytoplasmic, and nuclear fractions from human cells exposed to a panel of six genotoxins, comprehensively profiling their MN protein landscape. We find that MN assemble a proteome distinct from both surrounding cytoplasm and parental nuclei, depleted of spliceosome and DNA damage repair components while enriched for a subset of the replisome.

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Article Synopsis
  • Mitochondrial metabolite hexokinase 2 (HK2) is found in the nucleus of both leukaemic and normal haematopoietic stem cells, affecting their functions.
  • Overexpressing HK2 in the nucleus enhances leukaemic stem cell traits and inhibits differentiation, while reducing HK2 promotes differentiation and reduces stem cell properties.
  • HK2's nuclear presence relies on phosphorylation and specific transport mechanisms, impacting DNA repair and chemoresistance without its enzymatic function, highlighting a novel role for mitochondrial enzymes in regulating stem cells.
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