TY - JOUR
T1 - Personalized oncology
T2 - genomic screening in phase 1
AU - Tuxen, Ida Elisabeth Viller
AU - Jønson, Lars
AU - Santoni-Rugiu, Eric
AU - Hasselby, Jane Preuss
AU - Nielsen, Finn Cilius
AU - Lassen, Ulrik
N1 - © 2014 APMIS. Published by John Wiley & Sons Ltd.
PY - 2014/8
Y1 - 2014/8
N2 - 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.
AB - 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.
KW - Chromosome Mapping
KW - Clinical Trials, Phase I as Topic
KW - DNA Mutational Analysis
KW - Genetic Testing
KW - Genetic Variation
KW - Genomics
KW - Humans
KW - Individualized Medicine
KW - Molecular Targeted Therapy
KW - Neoplasms
KW - Patient Selection
KW - Tumor Markers, Biological
U2 - 10.1111/apm.12293
DO - 10.1111/apm.12293
M3 - Journal article
C2 - 25046202
SN - 0903-4641
VL - 122
SP - 723
EP - 733
JO - APMIS : acta pathologica, microbiologica, et immunologica Scandinavica
JF - APMIS : acta pathologica, microbiologica, et immunologica Scandinavica
IS - 8
ER -