An integrin β3–KRAS–RalB complex drives tumour stemness and resistance to EGFR inhibition

Seguin, Laetitia; Kato, Shumei; Franovic, Aleksandra; Camargo, M. Fernanda; Lesperance, Jacqueline; Elliott, Kathryn C.; Yebra, Mayra; Mielgo, Ainhoa; Lowy, Andrew M.; Husain, Hatim; Cascone, Tina; Li, Diao; Wang, Jing; Wistuba, Ignacio I.; Heymach, John V.; Lippman, Scott M.; Desgrosellier, Jay S.; Anand, Sudarshan; Weis, Sara M.; Cheresh, David A.

doi:10.1038/ncb2953

Cited by 322 publications

(355 citation statements)

References 58 publications

(64 reference statements)

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“…Integrin a v b 3 -expressing tumor-initiating cells from breast, lung, and pancreatic carcinomas are resistant to EGFR inhibitors [53]. NF-kB activation contributes to this phenotype because integrin a v b 3 drives tumor stemness and resistance to EGFR inhibitors by interacting with Kirsten rat sarcoma viral oncogene homolog GTPase (KRAS) through galectin-3 to promote the sequential activation of both GTPase v-Ral simian leukemia oncogene homolog B GTPase (RALB) and TANK-binding kinase-1 (TBK1), which then targets c-Rel, a NF-kB protein [53]. Interestingly, this pathway does not require the binding of any ligand to integrin a v b 3 , demonstrating that resistance to EGFR inhibitors can be cell autonomous.…”

Section: Reviewmentioning

confidence: 99%

EGFR and NF-κB: partners in cancer

Shostak

Chariot

2015

Trends in Molecular Medicine

184

160

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Section: Reviewmentioning

confidence: 99%

EGFR and NF-κB: partners in cancer

Shostak

Chariot

2015

Trends in Molecular Medicine

184

160

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“…While it is speculated that single targeted therapies may not be enough to surmount the dynamic nature and adaptive capacity of tumor cells [57], rational combinatorial therapies have the potential to overcome these resistance mechanisms with additional advantages such as blocking multiple survival pathways. It was recently found that as drug resistance occurs, tumor cells acquire stem cell-like properties giving them the capacity to survive throughout the body and essentially ignore the drugs [58]. In a study on acquisition of resistance against tyrosine kinase inhibitors (TKIs), the molecular pathway that facilitates pluripotency of tumor cells and drug resistance was delineated, and existing drugs that exploit this pathway (e.g., bortezomid) were identified.…”

Section: Challenge: Drug Resistance and The Role Of Tumor Genetic DIVmentioning

confidence: 99%

“Combo” nanomedicine: Co-delivery of multi-modal therapeutics for efficient, targeted, and safe cancer therapy

Kemp

Shim

Heo

et al. 2016

Advanced Drug Delivery Reviews

416

259

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a b s t r a c t a r t i c l e i n f oThe dynamic and versatile nature of diseases such as cancer has been a pivotal challenge for developing efficient and safe therapies. Cancer treatments using a single therapeutic agent often result in limited clinical outcomes due to tumor heterogeneity and drug resistance. Combination therapies using multiple therapeutic modalities can synergistically elevate anti-cancer activity while lowering doses of each agent, hence, reducing side effects. Co-administration of multiple therapeutic agents requires a delivery platform that can normalize pharmacokinetics and pharmacodynamics of the agents, prolong circulation, selectively accumulate, specifically bind to the target, and enable controlled release in target site. Nanomaterials, such as polymeric nanoparticles, gold nanoparticles/cages/shells, and carbon nanomaterials, have the desired properties, and they can mediate therapeutic effects different from those generated by small molecule drugs (e.g., gene therapy, photothermal therapy, photodynamic therapy, and radiotherapy). This review aims to provide an overview of developing multi-modal therapies using nanomaterials ("combo" nanomedicine) along with the rationale, up-to-date progress, further considerations, and the crucial roles of interdisciplinary approaches.

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“…Specifically, we found that while GPBAR1 activation reduced the expression of MMP7 and MMP13 genes, the expression of two other metalloproteinases MMP3 and MMP10 was robustly enhanced by all there agonists [31][32][33]. Further on, all three GPBAR1 ligands were effective in inducing the expression of ITGB3 [34], a integrin beta-chain subunit coded by a serotoninrelated gene on chromosome 17, that has been reported to be associated with the risk of several human cancers, including colorectal cancer. The ITGB3 family includes αIIb β3 and αvβ3.…”

Section: Discussionmentioning

confidence: 70%