Single-Cell Epigenomics In Cancer Research     
Yazarlar (2)
Dr. Öğr. Üyesi Çağlar BERKEL Tokat Gaziosmanpaşa Üniversitesi, Türkiye
Prof. Dr. Ercan ÇAÇAN Tokat Gaziosmanpaşa Üniversitesi, Türkiye
Makale Türü Diğer (Teknik, not, yorum, vaka takdimi, editöre mektup, özet, kitap krıtiği, araştırma notu, bilirkişi raporu ve benzeri)
Makale Alt Türü Diğer hakemli uluslararası dergilerde yayınlanan teknik not, editöre mektup, tartışma, vaka takdimi ve özet türünden makale
Dergi Adı Biomedical Journal of Scientific Technical Research
Dergi ISSN 2574-1241
Dergi Tarandığı Indeksler Crossref
Makale Dili İngilizce
Basım Tarihi 09-2019
Cilt No 21
Sayı 3
DOI Numarası 10.26717/BJSTR.2019.21.003619
Makale Linki https://biomedres.us/fulltexts/BJSTR.MS.ID.003619.php
Özet
A single tumor mass is comprised of many different subpopulations of cells. During evolutionary trajectory of a tumor, cells with different molecular features are likely to evolve and interactions between these heterogenous cell subpopulations in tumor are highly dynamic [1]. This intratumoral heterogeneity (ITH) is regulated in multiple levels and each cell subpopulation in a particular tumor can have distinct genomic, epigenomic, transcriptomic and spatial characteristics, effecting their metastatic potential and chemoresistance [2]. How the complex contributions of each subgroup in a complete population of cells in tumor affects the clinical progression of the disease is not completely understood. This is mostly due to the fact that cancer research previously has been limited to the analysis of bulk cells without dissecting heterogenous cell populations into subgroups with similar molecular features, therefore these studies have only reflected average profile of complex subgroups of cells, called subclones.
Anahtar Kelimeler
BM Sürdürülebilir Kalkınma Amaçları
Atıf Sayıları
Google Scholar 4
Single-Cell Epigenomics In Cancer Research

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