| Literature DB >> 31015588 |
Nobuyuki Tanaka1,2, Shigeaki Kanatani1, Raju Tomer3, Cecilia Sahlgren4,5, Pauliina Kronqvist6, Dagmara Kaczynska1, Lauri Louhivuori1, Lorand Kis7,8, Claes Lindh7,8, Przemysław Mitura9, Andrzej Stepulak10, Sara Corvigno7, Johan Hartman7,8, Patrick Micke11, Artur Mezheyeuski7, Carina Strell7, Joseph W Carlson7,8, Carlos Fernández Moro12,13, Hanna Dahlstrand7,11,14, Arne Östman7, Kazuhiro Matsumoto2, Peter Wiklund15,16, Mototsugu Oya2, Ayako Miyakawa1,15,16, Karl Deisseroth17,18,19, Per Uhlén20.
Abstract
Intratumoral heterogeneity is a critical factor when diagnosing and treating patients with cancer. Marked differences in the genetic and epigenetic backgrounds of cancer cells have been revealed by advances in genome sequencing, yet little is known about the phenotypic landscape and the spatial distribution of intratumoral heterogeneity within solid tumours. Here, we show that three-dimensional light-sheet microscopy of cleared solid tumours can identify unique patterns of phenotypic heterogeneity, in the epithelial-to-mesenchymal transition and in angiogenesis, at single-cell resolution in whole formalin-fixed paraffin-embedded (FFPE) biopsy samples. We also show that cleared FFPE samples can be re-embedded in paraffin after examination for future use, and that our tumour-phenotyping pipeline can determine tumour stage and stratify patient prognosis from clinical samples with higher accuracy than current diagnostic methods, thus facilitating the design of more efficient cancer therapies.Entities:
Year: 2017 PMID: 31015588 DOI: 10.1038/s41551-017-0139-0
Source DB: PubMed Journal: Nat Biomed Eng ISSN: 2157-846X Impact factor: 25.671