TY - JOUR
T1 - Approaching the increasing complexity of non-small cell lung cancer taxonomy
AU - Maugeri-Saccà, Marcello
AU - Bartucci, Monica
AU - Pagliuca, Alfredo
AU - Patrizii, Michele
AU - Signore, Michele
AU - De Maria Marchiano, Ruggero
PY - 2014
Y1 - 2014
N2 - The advent of molecular targeted agents is changing the treatment of solid tumors. In non-small-cell lung cancer, compounds directed against oncogenic proteins offer novel therapeutic opportunities for a fraction of patients whose tumors harbor specific genetic defects. With the increased level of resolution achieved by high-throughput technologies, the taxonomy of lung cancer is rapidly changing. For instance, by cataloguing genetic abnormalities in squamous cell lung cancer the Cancer Genome Atlas Network revealed the existence of multiple molecular entities, each one characterized by specific molecular abnormalities, and by a different spectrum of activated/inactivated molecular networks. Although this increased complexity could be perceived as a further drawback in effective antican-cer therapy, on the other hand the combined interrogation of genomic and proteomic data is expected to provide the whole molecular map of each tumor, and to determine the information flow in the explored biological system. In particular, novel genetic and proteomic approaches are offering the opportunity for matching specific genetic defects and aberrant protein-protein interactions with active pathway-targeted inhibitors. Moreover, the isolation and characterization of a cellular pool endowed with stem-like traits, and able to recapitulate the parental disease in animals, is enabling investigators to recreate the individual patient tumor in the laboratory. In this article, we discuss how novel technologies and cellular and animal models, applied to lung cancer research, hold the potential to foster a new wave of biomarker-driven clinical trials. © 2014 Bentham Science Publishers.
AB - The advent of molecular targeted agents is changing the treatment of solid tumors. In non-small-cell lung cancer, compounds directed against oncogenic proteins offer novel therapeutic opportunities for a fraction of patients whose tumors harbor specific genetic defects. With the increased level of resolution achieved by high-throughput technologies, the taxonomy of lung cancer is rapidly changing. For instance, by cataloguing genetic abnormalities in squamous cell lung cancer the Cancer Genome Atlas Network revealed the existence of multiple molecular entities, each one characterized by specific molecular abnormalities, and by a different spectrum of activated/inactivated molecular networks. Although this increased complexity could be perceived as a further drawback in effective antican-cer therapy, on the other hand the combined interrogation of genomic and proteomic data is expected to provide the whole molecular map of each tumor, and to determine the information flow in the explored biological system. In particular, novel genetic and proteomic approaches are offering the opportunity for matching specific genetic defects and aberrant protein-protein interactions with active pathway-targeted inhibitors. Moreover, the isolation and characterization of a cellular pool endowed with stem-like traits, and able to recapitulate the parental disease in animals, is enabling investigators to recreate the individual patient tumor in the laboratory. In this article, we discuss how novel technologies and cellular and animal models, applied to lung cancer research, hold the potential to foster a new wave of biomarker-driven clinical trials. © 2014 Bentham Science Publishers.
KW - Cancer stem cells
KW - Drug Discovery3003 Pharmaceutical Science
KW - Loss-of-function genetic screens
KW - Medicine (all)
KW - Molecular targeted agents
KW - Non-small-cell lung cancer
KW - Pharmacology
KW - Reverse-phase protein arrays
KW - Cancer stem cells
KW - Drug Discovery3003 Pharmaceutical Science
KW - Loss-of-function genetic screens
KW - Medicine (all)
KW - Molecular targeted agents
KW - Non-small-cell lung cancer
KW - Pharmacology
KW - Reverse-phase protein arrays
UR - http://hdl.handle.net/10807/112079
UR - http://www.ingentaconnect.com/content/ben/cpd
U2 - 10.2174/13816128113196660759
DO - 10.2174/13816128113196660759
M3 - Article
SN - 1381-6128
VL - 20
SP - 3973
EP - 3981
JO - Current Pharmaceutical Design
JF - Current Pharmaceutical Design
ER -