Carcinogenic effect of human tumor-derived cell-free filtrates in nude mice
Jorge Berlanga-Acosta, Ernesto Arteaga-Hernandez, Ariana Garcia-Ojalvo, Dayanis Duvergel-Calderin, Marisol Rodriguez-Touseiro, Laura Lopez-Marin, Jose Suarez-Alba, Dasha Fuentes-Morales, Osmany Mendoza-Fuentes, Sheyla Fernández-Puentes, Yanier Nuñez-Figueredo

TL;DR
This study shows that tumor-derived cell-free filtrates can cause cancer in healthy mice, suggesting the presence of 'malignancy drivers' in these extracts.
Contribution
The study demonstrates that tumor homogenates can act as vectors for carcinogenesis in healthy mice, extending prior findings.
Findings
Mammary carcinoma homogenates induced lung adenocarcinomas and small cell-like carcinomas in mice.
Pancreatic and melanoma homogenates caused deterioration in mouse health and specific tumor formations.
Zebrafish embryos exposed to breast tumor homogenates showed increased c-Myc and HER-2 expression.
Abstract
Cancer remains a worldwide cause of morbidity and mortality. Investigational research efforts have included the administration of tumor-derived extracts to healthy animals. Having previously demonstrated that the administration of non-transmissible, human cancer-derived homogenates induced malignant tumors in mice, here, we examined the consequences of administering 50 or 100 µg of protein of crude homogenates from mammary carcinoma, pancreatic adenocarcinoma, and melanoma samples in 6 inoculations per week during 2 months. The concurrent control mice received homogenates of healthy donor-skin cosmetic surgery fragments. Mammary carcinoma homogenate administration did not provoke the deterioration or mortality of the animals. Multiple foci of lung adenocarcinomas with a broad expression of malignity histomarkers coexisting with small cell-like carcinomas were found. Disseminated cells,…
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Taxonomy
TopicsCancer Cells and Metastasis · Mesenchymal stem cell research · Cancer Research and Treatments
