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10.18632/oncotarget.15181

http://scihub22266oqcxt.onion/10.18632/oncotarget.15181
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C5369962!5369962!28187445
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suck abstract from ncbi


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pmid28187445      Oncotarget 2017 ; 8 (10): 16275-92
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  • In vivo histone H1 migration from necrotic to viable tissue #MMPMID28187445
  • Luhrs KA; Pink D; Schulte W; Zijlstra A; Lewis JD; Parseghian MH
  • Oncotarget 2017[Mar]; 8 (10): 16275-92 PMID28187445show ga
  • Necrosis is induced by ischemic conditions within the core of many solid tumors. Using fluorescent fusion proteins, we provide in vivo evidence of histone trafficking among cancer cells in implanted tumors. In particular, the most abundant H1 isoform (H1.2) was found to be transported from necrotic tumor cells into surrounding viable cells where histones are selectively taken up by energy-dependent endocytosis. We propose that intercellular histone trafficking could function as a target for drug delivery. This concept was validated using an anti-histone antibody that was co-internalized with histones from dead cells into viable ones surrounding the necrotic regions of a tumor, where some of the most chemoresistant cells reside. These findings demonstrate that cellular translocation of conjugated drugs using anti-histone antibodies is a promising strategy for targeted drug delivery to chemoresistant tumors.
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