Literature DB >> 25046202

Personalized oncology: genomic screening in phase 1.

Ida Viller Tuxen1, Lars Jønson, Eric Santoni-Rugiu, Jane Preuss Hasselby, Finn Cilius Nielsen, Ulrik Lassen.   

Abstract

Improvements in cancer genomics and tumor biology have reinforced the evidence of cancer development driven by numerous genomic alterations. Advanced genomics technology can be used to characterize genomic alterations that potentially drive tumor growth. With the possibility of screening thousands of genes simultaneously, personalized molecular medicine has become an option. New treatments are being investigated in phase 1 trials around the world. Traditionally, the goal of phase 1 studies was to determine the optimal dose and assess dose-limiting toxicity of a potential new experimental drug. Only a limited number of patients will benefit from the treatment. However, introducing genomic mapping to select patients for early clinical trials with targeted molecular therapy according to the genomic findings, may lead to a better outcome for the patient, an enrichment of phase 1 trials, and thereby accelerated drug development. The overall advantage is to determine which mutation profiles correlate with sensitivity or lack of resistance to specific targeted therapies. The utility and current limitations of genomic screening to guide selection to Phase 1 clinical trial will be discussed.
© 2014 APMIS. Published by John Wiley & Sons Ltd.

Entities:  

Keywords:  Personalized medicine; cancer; next generation sequencing; phase 1; targeted treatment

Mesh:

Substances:

Year:  2014        PMID: 25046202     DOI: 10.1111/apm.12293

Source DB:  PubMed          Journal:  APMIS        ISSN: 0903-4641            Impact factor:   3.205


  10 in total

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Review 2.  Fast renal decline to end-stage renal disease: an unrecognized feature of nephropathy in diabetes.

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Review 3.  Global trends in the distribution of cancer types among patients in oncology phase I trials, 1991-2015.

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7.  Detection of copy number alterations in cell-free tumor DNA from plasma.

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8.  Application of cell-free DNA for genomic tumor profiling: a feasibility study.

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Journal:  Oncotarget       Date:  2019-02-15

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10.  Circulating tumor DNA as a marker of treatment response in BRAF V600E mutated non-melanoma solid tumors.

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  10 in total

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