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Brief overview of selected approaches in targeting pancreatic adenocarcinoma
Abstract: Introduction: Pancreatic adenocarcinoma (PDAC) has the worst prognosis of any major malignancy, with 5-year survival painfully inadequate at under 5%. Investigators have struggled to target and exploit PDAC unique biology, failing to bring meaningful results from bench to bedside. Nonetheless, in recent years, several promising targets have emerged.

Areas covered: This review will discuss novel drug approaches in development for use in PDAC. The authors examine the continued efforts to target Kirsten rat sarcoma viral oncogene homolog (KRas), which have recently been successfully abated using novel small interfering RNA (siRNA) eluting devices. The authors also discuss other targets relevant to PDAC including those downstream of mutated KRas, such as MAPK kinase and phosphatidylinositol 3-kinase.

Expert opinion: Although studies into novel biomarkers and advanced imaging have highlighted the potential new avenues toward discovering localized tumors earlier, the current therapeutic options highlight the fact that PDAC is a highly metastatic and chemoresistant cancer that often must be fought with virulent, systemic therapies. Several newer approaches, including siRNA targeting of mutated KRas and enzymatic depletion of hyaluronan with PEGylated hyaluronidase are particularly exciting given their early stage results. Further research should help in elucidating their potential impact as therapeutic options.
Keywords:AKT inhibitors  apricoxib  cabozantinib  celecoxib  c-Met  cyclooxygenase-2  crizotinib  cytidine deaminase  delta-like ligand 4  demcizumab  desmoplasia  γ-secretase inhibitors  gemcitabine  histone deacetylases  hyaluronan  KRas  local drug eluter  MAPK kinase inhibitors  MRK-003  MS-275  notch signaling  pancreatic adenocarcinoma  PEGylated hyaluronidase  PF-03084014  Ras  Sonic hedgehog  urokinase  urokinase plasminogen activator receptor  vorinostat
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