AI Article Synopsis

  • Self-renewal is a critical characteristic of cancer that can be evaluated through cell transplantation in zebrafish, a model that previously lacked the necessary tools for such studies.
  • Myc-induced T-cell acute lymphoblastic leukemias (T-ALLs) can be effectively created in zebrafish and transplanted into genetically similar siblings without immune suppression, revealing that self-renewing cells make up a significant portion of T-ALL mass.
  • The research introduces high-throughput imaging techniques to facilitate the study of numerous transgenic zebrafish, allowing for extensive analysis of the gene pathways related to cancer self-renewal and the tumor-initiating potential of leukemias.

Article Abstract

Self-renewal is a feature of cancer and can be assessed by cell transplantation into immune-compromised or immune-matched animals. However, studies in zebrafish have been severely limited by lack of these reagents. Here, Myc-induced T-cell acute lymphoblastic leukemias (T-ALLs) have been made in syngeneic, clonal zebrafish and can be transplanted into sibling animals without the need for immune suppression. These studies show that self-renewing cells are abundant in T-ALL and comprise 0.1% to 15.9% of the T-ALL mass. Large-scale single-cell transplantation experiments established that T-ALLs can be initiated from a single cell and that leukemias exhibit wide differences in tumor-initiating potential. T-ALLs also can be introduced into clonal-outcrossed animals, and T-ALLs arising in mixed genetic backgrounds can be transplanted into clonal recipients without the need for major histocompatibility complex matching. Finally, high-throughput imaging methods are described that allow large numbers of fluorescent transgenic animals to be imaged simultaneously, facilitating the rapid screening of engrafted animals. Our experiments highlight the large numbers of zebrafish that can be experimentally assessed by cell transplantation and establish new high-throughput methods to functionally interrogate gene pathways involved in cancer self-renewal.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2858492PMC
http://dx.doi.org/10.1182/blood-2009-10-246488DOI Listing

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