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Journal ArticleDOI

Kinase Inhibitors in Multitargeted Cancer Therapy.

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TLDR
The present review reports on the most widely FDA-approved multitargeted drugs, discussing about their mechanism of action and outlining the clinical trials that have brought them to approval.
Abstract
The old-fashioned anticancer approaches, aiming at arresting cancer cell proliferation interfering with non-specific targets (e.g. DNA), have been replaced, in the last decades, by more specific target oriented ones. Nonetheless, single-target approaches have not always led to optimal outcomes because, for its complexity, cancer needs to be tackled at various levels by modulation of several targets. Although at present, combinations of individual singletarget drugs represent the most clinically practiced therapeutic approaches, the modulation of multiple proteins by a single drug, in accordance with the polypharmacological strategy, has become more and more appealing. In the perspective of a multi-target approach, the closely related evolutionary members of the tyrosine kinase family are ideal candidates. Indeed, tyrosine kinase activities are not only critical in tumor phenotype maintenance, but also modulate several functions in the tumor microenvironment. Consequently, several multikinase inhibitors were approved in the last decade, and many new molecules are currently in preclinical or clinical development. In the present review we report on the most widely FDA-approved multitargeted drugs, discussing about their mechanism of action and outlining the clinical trials that have brought them to approval.

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G-quadruplex, Friend or Foe: The Role of the G-quartet in Anticancer Strategies.

TL;DR: The latest achievements and breakthroughs in the use of G4 nucleic acids as both therapeutic tools and targets for anticancer drugs and targets, particularly using aptamers and quadruplex-targeted ligands, respectively are summarized.
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Systemic Treatments for Metastatic Cutaneous Melanoma

TL;DR: A network meta-analysis approach was implemented to make indirect comparisons and rank treatments according to their effectiveness and harm and found that the combination of multiple chemotherapeutic agents (polychemotherapy) did not translate into significantly better survival.
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The power of combining phenotypic and target-focused drug discovery.

TL;DR: Despite the panoply of available in vitro TD methods, the task of matching a phenotypically active compound with a biomolecular target remains challenging and this review details the latest developments of in silico techniques that expedite TD.
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Genome-wide identification and analysis of prognostic features in human cancers

TL;DR: In this paper , a pan-cancer analysis identifies genomic biomarkers linked with patient outcome and demonstrates that these genomic features can predict patient outcomes in clinically ambiguous situations, while adverse biomarkers are commonly believed to represent cancer driver genes and promising therapeutic targets.
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Genome-wide identification and analysis of prognostic features in human cancers

TL;DR: In this paper, the authors constructed genome-wide survival models using gene expression, copy number, methylation, and mutation data from 10,884 patients with known clinical outcomes and identified more than 100,000 significant prognostic biomarkers and demonstrated that these genomic features can predict patient outcomes in clinically-ambiguous situations.
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