Small molecule antagonists of PTPmu identified by artificial intelligence-based computational screening block glioma cell migration and growth

Molyneaux, Kathleen; Laggner, Christian; Vincent, Jason; Brady‐Kalnay, Susann M.

doi:10.1371/journal.pone.0288980

Cited by 2 publications

(1 citation statement)

References 64 publications

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“…The AtomNet technology was also successfully used to identify ligands for very different protein families, for example, Miro1 261 as well as PTPmu. 262 The work proposing AttentionSiteDTI 219 also prospectively validated their approach, by predicting the binding interaction of seven compounds toward the Spike (ACE2) protein of SARS-CoV-2 where five out of seven were classified correctly.…”

Section: Applicationsmentioning

confidence: 99%

Modern machine‐learning for binding affinity estimation of protein–ligand complexes: Progress, opportunities, and challenges

Harren,

Gutermuth,

Grebner

et al. 2024

WIREs Comput Mol Sci

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Structure‐based drug design is a widely applied approach in the discovery of new lead compounds for known therapeutic targets. In most structure‐based drug design applications, the docking procedure is considered the crucial step. Here, a potential ligand is fitted into the binding site, and a scoring function assesses its binding capability. With the rise of modern machine‐learning in drug discovery, novel scoring functions using machine‐learning techniques achieved significant performance gains in virtual screening and ligand optimization tasks on retrospective data. However, real‐world applications of these methods are still limited. Missing success stories in prospective applications are one reason for this. Additionally, the fast‐evolving nature of the field makes it challenging to assess the advantages of each individual method. This review will highlight recent strides toward improved real world applicability of machine‐learning based scoring, enabling a better understanding of the potential benefits and pitfalls of these functions on a project. Furthermore, a systematic way of classifying machine‐learning based scoring that facilitates comparisons will be presented.This article is categorized under: Data Science > Chemoinformatics Data Science > Artificial Intelligence/Machine Learning Software > Molecular Modeling

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Section: Applicationsmentioning

confidence: 99%

Modern machine‐learning for binding affinity estimation of protein–ligand complexes: Progress, opportunities, and challenges

Harren,

Gutermuth,

Grebner

et al. 2024

WIREs Comput Mol Sci

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A novel binding pocket in the D2 domain of protein tyrosine phosphatase mu (PTPmu) guides AI screen to identify small molecules that modulate tumour cell adhesion, growth and migration

Molyneaux,

Laggner,

Brady‐Kalnay

2023

J Cellular Molecular Medi

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Approximately 40% of people will get cancer in their lifetime in the US, and 20% are predicted to die from the condition when it is invasive and metastatic. Targeted screening for drugs that interact with proteins that drive cancer cell growth and migration can lead to new therapies. We screened molecular libraries with the AtomNet® AI‐based drug design tool to identify compounds predicted to interact with the cytoplasmic domain of protein tyrosine phosphatase mu. Protein tyrosine phosphatase mu (PTPmu) is proteolytically downregulated in cancers such as glioblastoma generating fragments that stimulate cell survival and migration. Aberrant nuclear localization of PTPmu intracellular fragments drives cancer progression, so we targeted a predicted drug‐binding site between the two cytoplasmic phosphatase domains we termed a D2 binding pocket. The function of the D2 domain is controversial with various proposed regulatory functions, making the D2 domain an attractive target for the development of allosteric drugs. Seventy‐five of the best‐scoring and chemically diverse computational hits predicted to interact with the D2 binding pocket were screened for effects on tumour cell motility and growth in 3D culture as well as in a direct assay for PTPmu‐dependent adhesion. We identified two high‐priority hits that inhibited the migration and glioma cell sphere formation of multiple glioma tumour cell lines as well as aggregation. We also identified one activator of PTPmu‐dependent aggregation, which was able to stimulate cell migration. We propose that the PTPmu D2 binding pocket represents a novel regulatory site and that inhibitors targeting this region may have therapeutic potential for treating cancer.

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Small molecule antagonists of PTPmu identified by artificial intelligence-based computational screening block glioma cell migration and growth

Cited by 2 publications

References 64 publications

Modern machine‐learning for binding affinity estimation of protein–ligand complexes: Progress, opportunities, and challenges

Modern machine‐learning for binding affinity estimation of protein–ligand complexes: Progress, opportunities, and challenges

A novel binding pocket in the D2 domain of protein tyrosine phosphatase mu (PTPmu) guides AI screen to identify small molecules that modulate tumour cell adhesion, growth and migration

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