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Literature DB >> 21470103

Looking beyond inhibition of VEGF/mTOR: emerging targets for renal cell carcinoma drug development.

Abstract

The incidence rates of renal cell carcinoma (RCC) have continued to rise with 58,000 new cases in the United States. RCC has notoriously been refractory to traditional chemotherapeutic including radiation and cytokine therapies. The advent of the use of molecularly targeted therapies for RCC has significantly improved the standard of care. Yet, there still remains room for improvement as many of the current therapies are limited by acquired resistance and dosing restrictions due to toxicity. In this review we discuss many potential therapeutic targets that have been suggested for development as advancements are made in discovering the underlying molecular biology of RCC. Among the targets that discussed are additional targets within the well-established VHL/HIF axis, the PI3K/AKT/mTOR pathway, independent targets, and those identified by synthetic lethality screens.

Entities: Disease Gene

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Year: 2011 PMID： 21470103 DOI： 10.2174/157488411797189389

Source DB: PubMed Journal: Curr Clin Pharmacol ISSN： 1574-8847

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Cited

10 in total

1. Resistance to the mTOR inhibitor temsirolimus alters adhesion and migration behavior of renal cell carcinoma cells through an integrin α5- and integrin β3-dependent mechanism.

Authors: Eva Juengel; Jasmina Makarević; Michael Reiter; Jens Mani; Igor Tsaur; Georg Bartsch; Axel Haferkamp; Roman A Blaheta
Journal: Neoplasia Date: 2014-04 Impact factor: 5.715

Review 2. Resistance to Targeted Therapies in Renal Cancer: The Importance of Changing the Mechanism of Action.

Authors: I Duran; J Lambea; P Maroto; J L González-Larriba; Luis Flores; S Granados-Principal; M Graupera; B Sáez; A Vivancos; O Casanovas
Journal: Target Oncol Date: 2017-02 Impact factor: 4.493

3. Heteronemin, a Spongean Sesterterpene, Induces Cell Apoptosis and Autophagy in Human Renal Carcinoma Cells.

Authors: Szu-Ying Wu; Ping-Jyun Sung; Ya-Ling Chang; Shiow-Lin Pan; Che-Ming Teng
Journal: Biomed Res Int Date: 2015-05-18 Impact factor: 3.411

4. Racial difference in histologic subtype of renal cell carcinoma.

Authors: Andrew F Olshan; Tzy-Mey Kuo; Anne-Marie Meyer; Matthew E Nielsen; Mark P Purdue; W Kimryn Rathmell
Journal: Cancer Med Date: 2013-08-06 Impact factor: 4.452

5. Reduced E-cadherin facilitates renal cell carcinoma progression by WNT/β-catenin signaling activation.

Authors: Xinqi Zhang; Mingxi Yang; Hua Shi; Jianxin Hu; Yuanlin Wang; Zhaolin Sun; Shuxiong Xu
Journal: Oncotarget Date: 2017-03-21

6. MET expression and copy number status in clear-cell renal cell carcinoma: prognostic value and potential predictive marker.

Authors: Stephan Macher-Goeppinger; Martina Keith; Volker Endris; Roland Penzel; Katrin E Tagscherer; Sascha Pahernik; Markus Hohenfellner; Humphrey Gardner; Carsten Grüllich; Peter Schirmacher; Wilfried Roth
Journal: Oncotarget Date: 2017-01-03

Looking beyond inhibition of VEGF/mTOR: emerging targets for renal cell carcinoma drug development.

1. Resistance to the mTOR inhibitor temsirolimus alters adhesion and migration behavior of renal cell carcinoma cells through an integrin α5- and integrin β3-dependent mechanism.

Review 2. Resistance to Targeted Therapies in Renal Cancer: The Importance of Changing the Mechanism of Action.

3. Heteronemin, a Spongean Sesterterpene, Induces Cell Apoptosis and Autophagy in Human Renal Carcinoma Cells.

4. Racial difference in histologic subtype of renal cell carcinoma.

5. Reduced E-cadherin facilitates renal cell carcinoma progression by WNT/β-catenin signaling activation.

6. MET expression and copy number status in clear-cell renal cell carcinoma: prognostic value and potential predictive marker.

7. Tumor treating fields inhibit glioblastoma cell migration, invasion and angiogenesis.

8. HAX1 maintains the glioma progression in hypoxia through promoting mitochondrial fission.

Review 9. Prognostic markers in renal cell carcinoma: A focus on the 'mammalian target of rapamycin' pathway.

10. Cross-communication between histone H3 and H4 acetylation and Akt-mTOR signalling in prostate cancer cells.