Novel human melanoma brain metastasis models in athymic nude fox1nu mice: Site‐specific metastasis patterns reflecting their clinical origin

Henrik A. Svendsen; Torstein R. Meling; Vigdis Nygaard; Stein Waagene; Hege Russnes; Siri Juell; Siril G. Rogne; Jens Pahnke; Eirik Helseth; Øystein Fodstad; Gunhild M. Mælandsmo

doi:10.1002/cam4.4334

Cancer Medicine (Dec 2021)

Novel human melanoma brain metastasis models in athymic nude fox1nu mice: Site‐specific metastasis patterns reflecting their clinical origin

Henrik A. Svendsen,
Torstein R. Meling,
Vigdis Nygaard,
Stein Waagene,
Hege Russnes,
Siri Juell,
Siril G. Rogne,
Jens Pahnke,
Eirik Helseth,
Øystein Fodstad,
Gunhild M. Mælandsmo

Affiliations

Henrik A. Svendsen: Institute of Clinical Medicine Faculty of Medicine University of Oslo Oslo Norway
Torstein R. Meling: Institute of Clinical Medicine Faculty of Medicine University of Oslo Oslo Norway
Vigdis Nygaard: Department of Tumor Biology Institute for Cancer Research Oslo University Hospital‐Radiumhospitalet Oslo Norway
Stein Waagene: Department of Tumor Biology Institute for Cancer Research Oslo University Hospital‐Radiumhospitalet Oslo Norway
Hege Russnes: Department of Pathology Oslo University Hospital Oslo Norway
Siri Juell: Department of Tumor Biology Institute for Cancer Research Oslo University Hospital‐Radiumhospitalet Oslo Norway
Siril G. Rogne: Department of Neurosurgery Oslo University Hospital Oslo Norway
Jens Pahnke: Institute of Clinical Medicine Faculty of Medicine University of Oslo Oslo Norway
Eirik Helseth: Institute of Clinical Medicine Faculty of Medicine University of Oslo Oslo Norway
Øystein Fodstad: Institute of Clinical Medicine Faculty of Medicine University of Oslo Oslo Norway
Gunhild M. Mælandsmo: Department of Tumor Biology Institute for Cancer Research Oslo University Hospital‐Radiumhospitalet Oslo Norway

DOI: https://doi.org/10.1002/cam4.4334
Journal volume & issue: Vol. 10, no. 23
pp. 8604 – 8613

Abstract

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Abstract Background Malignant melanomas frequently metastasize to the brain, but metastases in the cerebellum are underrepresented compared with metastases in the cerebrum. Methods We established animal models by injecting intracardially in athymic nude fox1nu mice two human melanoma cell lines, originating from a cerebral metastasis (HM19) and a cerebellar metastasis (HM86). Results Using magnetic resonance imaging (MRI), metastases were first detected after a mean of 34.5 days. Mean survival time was 59.6 days for the mice in the HM86 group and significantly shorter (43.7 days) for HM19‐injected animals (p < 0.001). In the HM86 group, the first detectable metastasis was located in the cerebellum in 15/55 (29%) mice compared with none in the HM19 group (p < 0.001). At sacrifice, cerebellar metastases were found in 34/55 (63%) HM86‐injected mice compared with 1/53 (2%) in the HM19‐injected (p < 0.001) mice. At that time, all mice in both groups had detectable metastases in the cerebrum. Comparing macroscopic and histologic appearances of the brain metastases with their clinical counterparts, the cell line‐based tumors had kept their original morphologic characteristics. Conclusions The present work demonstrates that human brain‐metastatic melanoma cells injected intracardially in mice had retained inherent characteristics also in reproducing interaction with subtle microenvironmental brain tissue compartment‐specific features. The models offer new possibilities for investigating tumor‐ and host‐associated factors involved in determining tissue specificity of brain metastasis.

Published in Cancer Medicine

ISSN: 2045-7634 (Online)
Publisher: Wiley
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine: Neoplasms. Tumors. Oncology. Including cancer and carcinogens
Website: https://onlinelibrary.wiley.com/journal/20457634

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