4 2 2 p53-based drug therapy Several drugs have been investigated

4.2.2 p53-based drug therapy Several drugs have been investigated to target p53 via different mechanisms. One class of drugs are small molecules that can restore mutated p53 back to their wild-type functions. For example, Phikan083, a small molecule and carbazole derivative, has been shown to bind to and restore mutant p53 [77]. Another small molecule, CP-31398, has been found to intercalate with DNA and alter and destabilise the DNA-p53 core domain complex, resulting selleck in the restoration of unstable p53 mutants [78]. Other drugs that have been used to target p53 include the nutlins, MI-219 and the tenovins.

Nutlins are analogues of cis-imidazoline, which inhibit the MSM2-p53 interaction, stabilise p53 and selectively induce senescence

in cancer cells [79] while MI-219 was reported to disrupt the MDM2-p53 interaction, resulting in inhibition of cell proliferation, selective apoptosis in tumour cells and complete tumour growth inhibition [80]. The tenovins, on the other hand, are small molecule p53 activators, which have been shown to decrease tumour growth in vivo [81]. 4.2.3 p53-based immunotherapy Several clinical trials have been carried out using p53 vaccines. In a clinical trial by Kuball et al, six patients with advanced-stage cancer were given vaccine containing a recombinant replication-defective adenoviral vector with human wild-type p53. When followed up at 3 months post immunisation, four out of the six patients had stable disease. However, CH5424802 clinical trial only one patient had stable disease from 7 months onwards [82]. Other than viral-based vaccines, dendritic-cell based vaccines have also been attempted in clinical trials. Svane et al tested the use of p53 peptide pulsed dendritic cells in a phase I clinical trial and reported a clinical Evodiamine response in two out of six patients and p53-specific T cell responses in three out of six patients [83]. Other vaccines

that have been used including short peptide-based and long peptide-based vaccines (reviewed by Vermeij R et al., 2011 [84]). 4.3 Targeting the IAPs 4.3.1 Targeting XIAP When designing novel drugs for cancers, the IAPs are attractive molecular targets. So far, XIAP has been reported to be the most potent inhibitor of apoptosis among all the IAPs. It effectively inhibits the intrinsic as well as extrinsic pathways of apoptosis and it does so by binding and inhibiting upstream caspase-9 and the downstream caspases-3 and -7 [85]. Some novel therapy targeting XIAP include antisense strategies and short interfering RNA (siRNA) molecules. Using the antisense approach, inhibition of XIAP has been reported to result in an improved in vivo tumour control by radiotherapy [86]. When used together with anticancer drugs XIAP antisense oligonucleotides have been demonstrated to exhibit enhanced chemotherapeutic activity in lung cancer cells in vitro and in vivo [87].

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