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Metabolism of 2022 FDA approved small molecule drugs PART 2

Metabolite Tales Blog

Metabolism of 2022 FDA approved small molecule drugs part 2 Mixing it Up By Julia Shanu-Wilson In Part 1 of this topic we looked at metabolism of the small molecule drugs approved by the FDA in 2022 that were mediated by CYP3A4. We hope it was a useful two-parter! We’re looking forward to the next crop! Br J Pharmacol.

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Looking beyond traditional oncogenic pathways to break cancer resistance

Drug Target Review

Applying our technology has enabled us to develop a new small molecule, TT125-802, and to assign a new role to the epigenetic regulator CBP/p300 as a novel master regulator of non-oncogene resistance. This orally available small molecule binds to the bromodomain of CBP/p300 in a highly specific manner. Bell CC, Gilan O.

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ATUZAGINSTAT

New Drug Approvals

link] 01 Aug 2022 Cortexyme is now called Quince Therapeutics You need to be a logged in or subscribed to view this content This small molecule is an orally available protease inhibitor targeting the lysine proteases of the periodontal pathogen Porphyromonas gingivalis. In the same study, they show that in mice, oral P.

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Antibody-drug conjugates payloads: then, now and next

Drug Target Review

Groundbreaking strategies like proteolysis-targeting chimeric molecules (PROTACs) are also being explored. 6 Combining the effect of payloads with different mechanisms of action – an approach that revolutionised small molecule chemotherapy – also holds the promise of enhanced therapeutic activity for ADCs. 1 , 33–43 (2018).

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Steep FY2025 PDUFA Fee Increase: Ways to Reduce the Full Fee Rate for Repurposed Drugs

The Premier Consulting Blog

For example, pharmacokinetic (PK) data from a comparative BA study and PK modeling approaches (e.g., October 2019. [iv] patients with renal, hepatic, or cardiovascular concerns). July 28, 2023. iii] US Food and Drug Administration. Prescription Drug User Fee Act Waivers, Reductions, and Refunds for Drug and Biological Products.

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New molecular insights on medical cannabis

Drug Target Review

2,8-10 However, the number of compounds with satisfying pharmacokinetic parameters (PKD) are limited, with most unable to cross the blood-brain barrier or go sufficiently deep into a malignant tumour. He previously obtained a PharmD and a MSc degree from Grenoble Alpes University in 2019. J Med Chem. 2017 Mar 9;60(5):2006–17.

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The new approach in cancer therapy with innovative mechanism-of-action for ferroptosis induction

The Pharma Data

To this end, the team carefully evaluated hits from a screen of around ten thousand small molecule compounds and identified icFSP1 as a new in vivo effective drug. Although FSP1 has been considered as an attractive drug target for cancer therapy, in vivo efficacious FSP1 inhibitors have been lacking.