Publications by authors named "Andrea Ciamarone"
Article Synopsis
- Synthetic lethality is emerging as a key strategy for anticancer therapies, expanding beyond just PARP inhibitors for BRCA1/2-defective tumors.
- New molecular targets, particularly in DNA damage response, are quickly progressing to clinical trials, showcasing the growing interest in synthetic lethal approaches.
- The article highlights the latest developments in synthetic lethal targets, discusses their design and therapeutic strategies, and ends with an exploration of the challenges and opportunities for future research in this area.
The BRCA2-RAD51 interaction remains an intriguing target for cancer drug discovery due to its vital role in DNA damage repair mechanisms, which cancer cells become particularly reliant on. Moreover, RAD51 has many synthetically lethal partners, including PARP1-2, which can be exploited to induce synthetic lethality in cancer. In this study, we established a F-NMR-fragment based approach to identify RAD51 binders, leading to two initial hits.
View Article and Find Full Text PDFIn recent years, the RAD52 protein has been highlighted as a mediator of many DNA repair mechanisms. While RAD52 was initially considered to be a non-essential auxiliary factor, its inhibition has more recently been demonstrated to be synthetically lethal in cancer cells bearing mutations and inactivation of specific intracellular pathways, such as homologous recombination. RAD52 is now recognized as a novel and critical pharmacological target.
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