| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 2107090 | Cancer Cell | 2014 | 17 Pages |
•CQ reduces cancer cell invasion and metastasis•CQ induces tumor vessel normalization and improves drug delivery and response•CQ-mediated vessel normalization is autophagy independent•Vessel normalization by CQ relies on increased endothelial Notch1 signaling
SummaryChloroquine (CQ) has been evaluated as an autophagy blocker for cancer treatment, but it is unknown if it acts solely by inhibiting cancer cell autophagy. We report that CQ reduced tumor growth but improved the tumor milieu. By normalizing tumor vessel structure and function and increasing perfusion, CQ reduced hypoxia, cancer cell invasion, and metastasis, while improving chemotherapy delivery and response. Inhibiting autophagy in cancer cells or endothelial cells (ECs) failed to induce such effects. CQ’s vessel normalization activity relied mainly on alterations of endosomal Notch1 trafficking and signaling in ECs and was abrogated by Notch1 deletion in ECs in vivo. Thus, autophagy-independent vessel normalization by CQ restrains tumor invasion and metastasis while improving chemotherapy, supporting the use of CQ for anticancer treatment.
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