Lysosomal Sequestration of Sunitinib: A Novel Mechanism of Drug Resistance

Gotink, Kristy J.; Broxterman, Henk J.; Labots, Mariëtte; Haas, Richard R. de; Dekker, Henk; Honeywell, Richard J.; Rudek, Michelle A.; Beerepoot, Laurens V.; Musters, René J. P.; Jansen, Gerrit; Griffioen, Arjan W.; Assaraf, Yehuda G.; Пили, Роберто; Peters, Godefridus J.; Verheul, Henk M.W.

doi:10.1158/1078-0432.ccr-11-1667

Cited by 296 publications

(328 citation statements)

References 34 publications

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“…In addition, cimetidine had a similar effect as desipramine on crizotinib mass transport. The higher sunitinib and crizotinib accumulation in the Caco-2 intestinal monolayer after the incubation of verapamil and cimetidine is probably masked by lysosomal accumulation [22,39]. Just like sunitinib, sorafenib does not seem to be dependent on hOCT transport from apical to basolateral side.…”

Section: Discussionmentioning

confidence: 86%

“…These drugs are also not a highaffinity substrate for the ABC-family transporters, which is in agreement with the data reported by this study. However, passive transport can be masked by the lysosomal uptake leading to more accumulation in the cell at 37 °C as seen with sunitinib [22,39].…”

Section: Discussionmentioning

confidence: 99%

“…At later time-points the pattern changes, erlotinib accumulation at 4 °C continued to increase, but at 37 °C the accumulation decreased (Figure 2A), indicating an active efflux process. Sunitinib accumulation at 37 °C continued to increase, possibly due to a lysosomal accumulation ( Figure 2C) [22,39]. For crizotinib, the accumulation continued to increase under both conditions ( Figure 2E), but for sorafenib no change was observed ( Figure 2D).…”

Section: Temperature Dependent Accumulation In Caco-2 Cellsmentioning

confidence: 93%

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Transport of six tyrosine kinase inhibitors: active or passive?

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Section: Discussionmentioning

confidence: 86%

Section: Discussionmentioning

confidence: 99%

Section: Temperature Dependent Accumulation In Caco-2 Cellsmentioning

confidence: 93%

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Transport of six tyrosine kinase inhibitors: active or passive?

Honeywell¹,

Hitzerd²,

Kathmann³

et al. 2016

ADMET DMPK

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“…L'autophagie permet ainsi aux cellules de survivre avant l'induction de l'angiogenèse, en dégradant les protéines et les organites qui ne leur sont pas essentiels. La séquestration dans des lysosomes de cellules tumorales, de l'inhibiteur sunitinib, constitue ainsi un mécanisme de résistance au traitement [33]. Les cellules inflammatoires, nerveuses et endothé- SYNTHÈSE REVUES concentration plasmatique des facteurs de l'angiogenèse comme le VEGF, le PlGF, le FGF-2 ou l'IL-8, qui est le reflet d'une résistance ayant pour origine une néoangiogenèse, est considérée comme un marqueur de mauvais pronostic.…”

Section: Les éChanges De Microparticules Et La Présence De Pompes à Eunclassified

La résistance aux traitements antiangiogéniques

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Boisson-Vidal

et al. 2016

Med Sci (Paris)

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“…In Phase II trials, a heterogeneous response to sunitinib was noted in both docetaxel-resistant and chemotherapy naïve patients with a significant proportion of tumors demonstrating at least a partial radiographic response. In the most recent study of subjects with docetaxel-resistant CRPC, 11.1% of patients demonstrated 30% tumor reduction by Response Evaluation Criteria In Solid Tumors (RECIST) criteria. Another 44.4% of patients had quantifiable but less significant tumor response (5).…”

Section: Introductionmentioning

confidence: 99%

974 Modulation of Akt/Mtor Signaling Overcomes Sunitinib Resistance in Renal and Prostate Cancer Cells

et al. 2012

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Tyrosine kinase inhibitors (TKIs) exhibit impressive activity against advanced renal cell carcinoma. However, recent clinical studies have demonstrated an equivocal response to sunitinib in patients with castration-resistant prostate cancer. The tumor suppressor phosphatase and tensin homolog (PTEN) acts as a gatekeeper of the PI3K/Akt/mTOR cell-survival pathway. Our experiments demonstrate that PTEN expression inversely correlates with sunitinib resistance in renal and prostate cancer cells. Restoration of PTEN expression markedly increases sensitivity of tumor cells to sunitinib both in vitro and in vivo. In addition, pharmacologic manipulation of PI3K/Akt/mTOR signaling with PI3K/mTOR inhibitor, GDC-0980, mTOR inhibitor, temsirolimus, or pan-Akt inhibitor, GSK690693, was able to overcome sunitinib resistance in cancer cells. Our findings underscore the importance of PTEN expression in relation to sunitinib resistance and imply a direct cytotoxic effect by sunitinib on tumor cells in addition to its antiangiogenic actions.

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Lysosomal Sequestration of Sunitinib: A Novel Mechanism of Drug Resistance

Cited by 296 publications

References 34 publications

Transport of six tyrosine kinase inhibitors: active or passive?

Transport of six tyrosine kinase inhibitors: active or passive?

La résistance aux traitements antiangiogéniques

974 Modulation of Akt/Mtor Signaling Overcomes Sunitinib Resistance in Renal and Prostate Cancer Cells

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