Lisa Sprinzen scite author profile

Lisa Sprinzen

3Publications

56Citation Statements Received

122Citation Statements Given

How they've been cited

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118

Affiliations

Cancer Genetics (United States), Columbia University

Publications

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Kinase-dead ATM protein is highly oncogenic and can be preferentially targeted by Topo-isomerase I inhibitors

Yamamoto

Wang

Sprinzen

et al. 2016

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Missense mutations in ATM kinase, a master regulator of DNA damage responses, are found in many cancers, but their impact on ATM function and implications for cancer therapy are largely unknown. Here we report that 72% of cancer-associated ATM mutations are missense mutations that are enriched around the kinase domain. Expression of kinase-dead ATM (AtmKD/-) is more oncogenic than loss of ATM (Atm-/-) in mouse models, leading to earlier and more frequent lymphomas with Pten deletions. Kinase-dead ATM protein (Atm-KD), but not loss of ATM (Atm-null), prevents replication-dependent removal of Topo-isomerase I-DNA adducts at the step of strand cleavage, leading to severe genomic instability and hypersensitivity to Topo-isomerase I inhibitors. Correspondingly, Topo-isomerase I inhibitors effectively and preferentially eliminate AtmKD/-, but not Atm-proficientor Atm-/- leukemia in animal models. These findings identify ATM kinase-domain missense mutations as a potent oncogenic event and a biomarker for Topo-isomerase I inhibitor based therapy.DOI: http://dx.doi.org/10.7554/eLife.14709.001

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Author response: Kinase-dead ATM protein is highly oncogenic and can be preferentially targeted by Topo-isomerase I inhibitors

Yamamoto

Wang

Sprinzen

et al. 2016

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P3‐415: Testing of Innate Immunity Stimulation via Tlr9 on Cerebral Amyloid Angiopathy Using Non‐human Primates

Scholtzova

Nehete²,

Nehete³

et al. 2014

Alzheimer's & Dementia

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Lisa Sprinzen

Kinase-dead ATM protein is highly oncogenic and can be preferentially targeted by Topo-isomerase I inhibitors

Author response: Kinase-dead ATM protein is highly oncogenic and can be preferentially targeted by Topo-isomerase I inhibitors

P3‐415: Testing of Innate Immunity Stimulation via Tlr9 on Cerebral Amyloid Angiopathy Using Non‐human Primates

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