Publications by authors named "Lauren Bradshaw"

PRMT5, a type 2 arginine methyltransferase, has a critical role in regulating cell growth and survival in cancer. With the aim of developing MTA-cooperative PRMT5 inhibitors suitable for MTAP-deficient cancers, herein we report our efforts to develop novel "MTA-cooperative" compounds identified through a high-throughput biochemical screening approach. Optimization of hits was achieved through structure-based design with a focus on improvement of oral drug-like properties.

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Article Synopsis
  • The Phase III CAPItello-291 trial showed that combining capivasertib (an AKT inhibitor) and fulvestrant (a SERD) improved progression-free survival for HR+ breast cancer patients after aromatase inhibitors, but prior treatment with CDK4/6 inhibitors may lessen the effectiveness of future endocrine therapies.
  • Researchers examined how CDK4/6 inhibitors affect the function of estrogen receptor-positive (ER+) breast cancer cells and their responses to fulvestrant and capivasertib, finding varied gene expression and signaling alterations in resistant cell lines.
  • Despite reduced efficacy and changes in cellular signaling in both RB+ and RB- resistant models, the combination therapy was still effective in reducing cell cycle activity
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Alzheimer's disease (AD) is associated with the intracellular aggregation of hyperphosphorylated tau and the accumulation of β-amyloid in the neocortex. We use transgenic mice harboring human tau (rTg4510) and amyloid precursor protein (J20) mutations to investigate transcriptional changes associated with the progression of tau and amyloid pathology. rTg4510 mice are characterized by widespread transcriptional differences in the entorhinal cortex with changes paralleling neuropathological burden across multiple brain regions.

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Recent data suggest that the adhesion docking protein NEDD9/HEF1/Cas-L is a critical regulator of adhesion-dependent signalling pathways during mammary tumour development. Multiple phosphorylation modifications of NEDD9 regulate interaction with downstream protein partners, thus the regulation of NEDD9 phospho-forms is an important point of control for NEDD9 function. As estradiol (E2) plays a central role in the development and progression of breast cancer, we have investigated NEDD9 phospho-form regulation in MCF-7 estrogen receptor (ER)-positive breast cancer cells in response to estrogen.

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