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Review
. 2014 Mar;18(3):277-92.
doi: 10.1517/14728222.2014.867946. Epub 2014 Jan 6.

Therapeutic targets for neuroblastomas

Garrett M Brodeur  1 Radhika IyerJamie L CroucherTiangang ZhuangMayumi HigashiVenkatadri Kolla
Affiliations
Review

Therapeutic targets for neuroblastomas

Garrett M Brodeur et al. Expert Opin Ther Targets. 2014 Mar.

Abstract

Introduction: Neuroblastoma (NB) is the most common and deadly solid tumor in children. Despite recent improvements, the long-term outlook for high-risk NB is still < 50%. Further, there is considerable short- and long-term toxicity. More effective, less toxic therapy is needed, and the development of targeted therapies offers great promise.

Areas covered: Relevant literature was reviewed to identify current and future therapeutic targets that are critical to malignant transformation and progression of NB. The potential or actual NB therapeutic targets are classified into four categories: i) genes activated by amplification, mutation, translocation or autocrine overexpression; ii) genes inactivated by deletion, mutation or epigenetic silencing; iii) membrane-associated genes expressed on most NBs but few other tissues; or iv) common target genes relevant to NB as well as other tumors.

Expert opinion: Therapeutic approaches have been developed to some of these targets, but many remain untargeted at the present time. It is unlikely that single targeted agents will be sufficient for long-term cure, at least for high-risk NBs. The challenge will be how to integrate targeted agents with each other and with conventional therapy to enhance their efficacy, while simultaneously reducing systemic toxicity.

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Figures

Figure 1
Figure 1. Diagrammatic representation and intracellular location of therapeutic targets of NB
Activated genes and their encoded proteins are shown in red; inactivated genes/proteins are shown in green; selectively expressed membrane proteins (e.g., NET, GD2) are shown in burgundy; and common targets relevant to NBs and other cancers are shown in blue.
See this image and copyright information in PMC

References

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