ASPIC

Authors and Affiliations:

Sara Silva ^1 2 3, Cláudia Alves ⁴, Diana Duarte ^1 2, Ana Costa ^5 6, Bruno Sarmento ^5 6 7 8, António J Almeida ³, Paula Gomes ⁴, Nuno Vale ^1 9

¹ OncoPharma Research Group, Center for Health Technology and Services Research (CINTESIS), Rua Dr. Plácido da Costa, 4200-450 Porto, Portugal.

We have established a in vivo limiting dilution assay (LDA) using the chick embryo chorioallantoic membrane (CAM), using a metastatic breast cancer cell model previously shown to be enriched for cancer stem cell (CSC) properties. This new tool was able to reproduce the same results found in mice, which is the gold standard method to evaluate CSC enrichment. Importantly, the chick model has several advantages, namely its easy handling, accessibility, rapid growth, lower costs and the absence of ethical and regulatory constraints.

Estabelecemos um ensaio de diluições limitantes utilizando a membrana corioalantóide do embrião da galinha (CAM), usando um modelo metastático de cancro da mama, no qual já foi demonstrado um enriquecimento em células com potencial estaminal. Com este novo ensaio  foi possível reproduzir os mesmos resultados encontrados no ratinho, o modelo  animal standard para a avaliação do enriquecimento estaminal em cancro.

Researchers from two Groups of Research Center IPO Porto Cancer: Biology & Epigenetics Group and Medical Physics, Radiobiology and Radiological Protection, recently published a study in the international journal Cell Death & Disease entitled: “JmjC-KDMs KMD3A and KDM6B modulate radioresistance under hypoxic conditions in esophageal squamous cell carcinoma”. This work highlights the role of lysine demethylases (KDMs), in particular KDM3A, in radioresistant behavior of esophageal squamous cell carcinoma cells, under hypoxia.

Investigadores do Grupo de Epigénetica e Biologia do Cancro e do Grupo de Física Médica, Radiobiologia e Protecção Radiológica do Centro de Investigação do IPO do Porto, publicaram recentemente na revista internacional Cell Death & Disease um trabalho desenvolvido no âmbito do Projecto ESTIMA (NORTE-01-0145-FEDER-000027) intitulado: “JmjC-KDMs KMD3A and KDM6B modulate radioresistance under hypoxic conditions in esophageal squamous cell carcinoma”.

Authors and affiliations:
Eduardo Costa ^1,2,3,4, Tânia Ferreira-Gonçalves ³, Miguel Cardoso ^2,5,6,7, João M. P. Coelho ⁸, Maria Manuela Gaspar ³, Pedro Faísca ⁹, Lia Ascensão ¹⁰, António S. Cabrita ², Catarina Pinto Reis ^3,8,* and Isabel V. Figueiredo ^1,7,*

¹ Pharmacology and Pharmaceutical Care Laboratory, Faculty of Pharmacy, University of Coimbra, Azinhaga de Santa Comba, 3000-548 Coimbra, Portugal;

The presence of polymorphic gene variants in the human genome provides extensive genetic (and eventually phenotypic) variation affecting both normal physiological mechanisms and cancer pathogenesis. Functional genetic polymorphisms might have predictive and/or prognostic value in lung cancer, opening novel opportunities to improve prediction and guide clinical reasoning and therapeutics in lung cancer patients.