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Synthetic lethal therapies for cancer: what’s next after PARP inhibitors?
by
Ashworth, Alan
, Lord, Christopher J
in
BRCA1 protein
/ BRCA2 protein
/ Breast cancer
/ Computer applications
/ CRISPR
/ Lethality
/ Mutagenesis
/ Ovarian cancer
/ Patients
/ Poly(ADP-ribose)
/ Poly(ADP-ribose) polymerase
/ Prostate cancer
/ Ribose
/ Targeted cancer therapy
2018
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Synthetic lethal therapies for cancer: what’s next after PARP inhibitors?
by
Ashworth, Alan
, Lord, Christopher J
in
BRCA1 protein
/ BRCA2 protein
/ Breast cancer
/ Computer applications
/ CRISPR
/ Lethality
/ Mutagenesis
/ Ovarian cancer
/ Patients
/ Poly(ADP-ribose)
/ Poly(ADP-ribose) polymerase
/ Prostate cancer
/ Ribose
/ Targeted cancer therapy
2018
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While trying to remove the title from your shelf something went wrong :( Kindly try again later!
Do you wish to request the book?
Synthetic lethal therapies for cancer: what’s next after PARP inhibitors?
by
Ashworth, Alan
, Lord, Christopher J
in
BRCA1 protein
/ BRCA2 protein
/ Breast cancer
/ Computer applications
/ CRISPR
/ Lethality
/ Mutagenesis
/ Ovarian cancer
/ Patients
/ Poly(ADP-ribose)
/ Poly(ADP-ribose) polymerase
/ Prostate cancer
/ Ribose
/ Targeted cancer therapy
2018
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Synthetic lethal therapies for cancer: what’s next after PARP inhibitors?
Journal Article
Synthetic lethal therapies for cancer: what’s next after PARP inhibitors?
2018
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Overview
The genetic concept of synthetic lethality has now been validated clinically through the demonstrated efficacy of poly(ADP-ribose) polymerase (PARP) inhibitors for the treatment of cancers in individuals with germline loss-of-function mutations in either BRCA1 or BRCA2. Three different PARP inhibitors have now been approved for the treatment of patients with BRCA-mutant ovarian cancer and one for those with BRCA-mutant breast cancer; these agents have also shown promising results in patients with BRCA-mutant prostate cancer. Here, we describe a number of other synthetic lethal interactions that have been discovered in cancer. We discuss some of the underlying principles that might increase the likelihood of clinical efficacy and how new computational and experimental approaches are now facilitating the discovery and validation of synthetic lethal interactions. Finally, we make suggestions on possible future directions and challenges facing researchers in this field.
Publisher
Nature Publishing Group
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