VEGF-targeted agents consist of the monoclonal antibody bevacizumab which neutra

VEGF-targeted agents incorporate the monoclonal antibody bevacizumab which neutralizes VEGF itself, and receptor tyrosine kinase inhibitors just like sorafenib, sunitinib, pazopanib, and axitinib. These agents target the VEGFRs, as do further TKIs in ongoing clinical development, with effects that extend beyond the VEGFRs . The new wave of US Food and Drug Administration? approved molecularly targeted antiangiogenic agents has largely supplanted cytokines as first- and second-line therapy for metastatic RCC . Second-generation molecularly targeted selleck product therapies in development incorporate axitinib ; tivozanib and cediranib ; brivanib ; motesanib ; XL184 ; and VEGF TRAP . Timely and proper management of treatmentrelated toxicities is vital in an effort to deliver therapy safely and optimally. This assessment describes and compares the toxicity profiles of antiangiogenic agents utilised in mRCC. Specific interest is devoted to axitinib, an antiangiogenic multi-targeted TKI in active clinical development for mRCC. Guidelines for preventing and managing treatment-related toxicities of axitinib are presented, which also have general relevance to all the small-molecule angiogenesis inhibitors. Efficacy of new antiangiogenic agents in pivotal clinical trials Findings from important clinical trials of approved antiangiogenic agents in advanced RCC have reported consistent prolongation of progression-free survival and, in some instances, general survival in both treatment-na?ve and previously treated patients .
The newer agent, axitinib, is often a potent, selective, secondgeneration inhibitor of VEGFR-1, 2, and three with clinical antitumor activity inside a number of solid tumors . Within a current pivotal randomized phase III trial, axitinib demonstrated statistically superior PFS compared with sorafenib, also as being a greater response rate . Though a lot of from the toxicities of axitinib are shared with these in the other TKIs, there can be essential differences, most notably an apparent higher incidence of hypertension. Moreover, the safety profile Erlotinib for axitinib is distinct from that of sorafenib. Typical adverse events much more frequent with sorafenib versus axitinib had been hand-foot syndrome , rash, alopecia, anemia, hypophosphatemia, hypocalcemia, and elevated lipase whereas the predominant toxicities with axitinib were hypertension, fatigue, nausea, vomiting, and hypothyroidism . Axitinib 1st demonstrated clinical activity in patients with refractory advanced RCC within a phase II study , in which 52 individuals with cytokine-refractory mRCC and clear-cell histology received axitinib 5 mg twice everyday . An all round response rate of 44% was reported with a median duration of response of 23.0 months . Median time to progression was 15.7 months and median OS was 29.9 months . Within a second phase II trial , patients with sorafenib-refractory mRCC received axitinib at a starting dose of five mg BID.

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