Journal
BIOORGANIC & MEDICINAL CHEMISTRY
Volume 65, Issue -, Pages -Publisher
PERGAMON-ELSEVIER SCIENCE LTD
DOI: 10.1016/j.bmc.2022.116785
Keywords
Protein phosphatase-1; PP1-disrupting peptides; Peptide pharmacophore; High throughput screening; Virtual screening; Rational peptide design; Structure-activity relationship study
Funding
- ALMF at EMBL [336567, 865119]
- ALMF at EMBL
- LIC at the University of Freiburg
- European Research Council (ERC) [336567, 865119]
- European Research Council (ERC) [336567, 865119] Funding Source: European Research Council (ERC)
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This study presents the sequence optimization of a 23mer PDP to a 5mer peptide, providing a lead structure for targeting PP1 in therapy or for its use in phosphatase-recruiting chimeras in the future.
PP1 is a major phosphoserine/threonine-specific phosphatase that is involved in diseases such as heart insufficiency and diabetes. PP1-disrupting peptides (PDPs) are selective modulators of PP1 activity that release its catalytic subunit, which then dephosphorylates nearby substrates. Recently, PDPs enabled the creation of phosphatase-recruiting chimeras, which are bifunctional molecules that guide PP1 to a kinase to dephosphorylate and inactivate it. However, PDPs are 23mer peptides, which is not optimal for their use in therapy due to potential stability and immunogenicity issues. Therefore, we present here the sequence optimization of the 23mer PDP to a 5mer peptide, involving several attempts considering structure-based virtual screening, high throughput screening and peptide sequence optimization. We provide here a strong pharmacophore as lead structure to enable PP1 targeting in therapy or its use in phosphatase-recruiting chimeras in the future.
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