| Literature DB >> 33602908 |
Pin Lu1, Shengchun Wang1,2, Carrie A Franzen3, Girish Venkataraman3, Rebecca McClure4, Lei Li3, Wenjun Wu1, Nifang Niu3, Madina Sukhanova5, Jianming Pei1, Donald A Baldwin1, Reza Nejati1, Mariusz A Wasik1, Nadia Khan1, Yifan Tu6, Juehua Gao5, Yihua Chen5, Shuo Ma5, Richard A Larson3, Y Lynn Wang7,8.
Abstract
Ibrutinib inhibits Bruton tyrosine kinase while venetoclax is a specific inhibitor of the anti-apoptotic protein BCL2. Both drugs are highly effective as monotherapy against chronic lymphocytic leukemia (CLL), and clinical trials using the combination therapy have produced remarkable results in terms of rate of complete remission and frequency of undetectable minimal residual disease. However, the laboratory rationale behind the success of the drug combination is still lacking. A better understanding of how these two drugs synergize would eventually help develop other rational combination strategies. Using an ex vivo model that promotes CLL proliferation, we show that modeled ibrutinib proliferative responses, but not viability responses, correlate well with patients' actual clinical responses. Importantly, we demonstrate for the first time that ibrutinib and venetoclax act on distinct CLL subpopulations that have different proliferative capacities. While the dividing subpopulation of CLL responds to ibrutinib, the resting subpopulation preferentially responds to venetoclax. The combination of these targeted therapies effectively reduced both the resting and dividing subpopulations in most cases. Our laboratory findings help explain several clinical observations and contribute to the understanding of tumor dynamics. Additionally, our proliferation model may be used to identify novel drug combinations with the potential of eradicating residual disease.Entities:
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Year: 2021 PMID: 33602908 PMCID: PMC7893066 DOI: 10.1038/s41408-021-00429-z
Source DB: PubMed Journal: Blood Cancer J ISSN: 2044-5385 Impact factor: 9.812