AI Article Synopsis

  • Uveal melanoma (UM) is the most common primary eye cancer in adults, but it often spreads to the liver, where current treatments are ineffective and prognosis is poor.
  • Researchers developed two mouse models to study UM liver metastasis: one using direct liver implantation and another using splenic implantation.
  • The findings showed that the direct model produced localized liver tumors while the splenic model led to multiple liver metastases, mirroring human disease, providing valuable insights for future UM research.

Article Abstract

Uveal melanoma (UM) is a rare type of melanoma, although it is the most common primary ocular malignant tumor in adults. Nearly one-half the patients with primary UM subsequently develop systemic metastasis, preferentially to the liver. Currently, no treatment is effective for UM hepatic metastasis, and the prognosis is universally poor. The main challenge in designing a treatment strategy for UM hepatic metastasis is the lack of suitable animal models. We developed two orthotopic mouse models for human UM hepatic metastases: direct hepatic implantation model (intrahepatic dissemination model) and splenic-implantation model (hematogenous dissemination model) and investigated the tumorgenesis in the liver. A human UM cell line, established from a hepatic metastasis and nonobese diabetic severe combined immunodeficient γ mice, were used for development of in vivo tumor models. In the direct hepatic implantation model, a localized tumor developed in the liver in all cases and intrahepatic dissemination was subsequently seen in about one-half of cases. However, in the splenic implantation model, multiple hepatic metastases were observed after splenic implantation. Hepatic tumors subsequently seeded intra-abdominal metastasis; however, lung metastases were not seen. These findings are consistent with those observed in human UM hepatic metastases. These orthotopic mouse models offer useful tools to investigate the biological behavior of human UM cells in the liver.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4715216PMC
http://dx.doi.org/10.1016/j.ajpath.2015.09.011DOI Listing

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