Cloning and functional complementation of ten Schistosoma mansoni phosphodiesterases expressed in the mammalian host stages

Munday, Jane C.; Kunz, Stefan; Kalejaiye, Titilola D.; Siderius, Marco; Schroeder, Susanne; Paape, Daniel; Al-Ghamdi, Ali; Abbasi, Zainab; Huang, Sheng Xiang; Donachie, Anne M.; William, Samia; Sabra, Abdel Nasser A.; Sterk, Geert Jan; Botros, Sanaa S.; Brown, David G.; Hoffman, Charles S.; Leurs, Rob; Koning, Harry P. de

doi:10.1371/journal.pntd.0008447

Cited by 2 publications

(4 citation statements)

References 92 publications

(155 reference statements)

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“…After cloning the SmPDE4a gene [ 26 ], we set out to characterize this parasite PDE biochemically, pharmacologically, as well as structurally to enable a structure-based drug design program aiming to target SmPDE4A. To this end, two 6×His-tagged SmPDE4a constructs were generated, PCR amplified and cloned into pOPINF encoding a cleavable N -terminal 6×His tag.…”

Section: Resultsmentioning

confidence: 99%

“…Within the EU-funded consortium PDE4NPD aiming at investigating the potential of parasite PDEs as drug targets, we decided at its start in 2014 to embark on a PDE target discovery program for S. mansoni [ 25 ]. Munday et al [ 26 ] identified 11 different PDE open reading frames in the S. mansoni genome and cloned 10 of these SmPDEs (ranging from 517 to 1081 amino acids) from cDNA. Moreover, using different expression systems (yeast, T. brucei ), enzymatic activity was documented for six of the SmPDEs [ 26 ], making these parasite PDEs attractive new drug targets.…”

Section: Introductionmentioning

confidence: 99%

“…Munday et al [ 26 ] identified 11 different PDE open reading frames in the S. mansoni genome and cloned 10 of these SmPDEs (ranging from 517 to 1081 amino acids) from cDNA. Moreover, using different expression systems (yeast, T. brucei ), enzymatic activity was documented for six of the SmPDEs [ 26 ], making these parasite PDEs attractive new drug targets.…”

Section: Introductionmentioning

confidence: 99%

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To Target or Not to Target Schistosoma mansoni Cyclic Nucleotide Phosphodiesterase 4A?

Zheng

Schroeder

Kanev

et al. 2023

IJMS

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Schistosomiasis is a neglected tropical disease with high morbidity. Recently, the Schistosoma mansoni phosphodiesterase SmPDE4A was suggested as a putative new drug target. To support SmPDE4A targeted drug discovery, we cloned, isolated, and biochemically characterized the full-length and catalytic domains of SmPDE4A. The enzymatically active catalytic domain was crystallized in the apo-form (PDB code: 6FG5) and in the cAMP- and AMP-bound states (PDB code: 6EZU). The SmPDE4A catalytic domain resembles human PDE4 more than parasite PDEs because it lacks the parasite PDE-specific P-pocket. Purified SmPDE4A proteins (full-length and catalytic domain) were used to profile an in-house library of PDE inhibitors (PDE4NPD toolbox). This screening identified tetrahydrophthalazinones and benzamides as potential hits. The PDE inhibitor NPD-0001 was the most active tetrahydrophthalazinone, whereas the approved human PDE4 inhibitors roflumilast and piclamilast were the most potent benzamides. As a follow-up, 83 benzamide analogs were prepared, but the inhibitory potency of the initial hits was not improved. Finally, NPD-0001 and roflumilast were evaluated in an in vitro anti-S. mansoni assay. Unfortunately, both SmPDE4A inhibitors were not effective in worm killing and only weakly affected the egg-laying at high micromolar concentrations. Consequently, the results with these SmPDE4A inhibitors strongly suggest that SmPDE4A is not a suitable target for anti-schistosomiasis therapy.

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Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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To Target or Not to Target Schistosoma mansoni Cyclic Nucleotide Phosphodiesterase 4A?

Zheng

Schroeder

Kanev

et al. 2023

IJMS

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“…Previously, we expressed in S. pombe PDE4, PDE8, and PDE11 family members from the blood fluke Schistosoma mansoni , whose genome includes members of all 11 Class I PDE families ( Vyas et al, 2021 ). 5FOA growth assays were used to determine the relative ability of these enzymes to hydrolyze cAMP and cGMP as shown by an increase in amount of exogenous cNMP required to confer 5FOA R growth ( Munday et al, 2020 ). However, an even more fertile area of research could involve the treatment of infections by parasitic nematodes due to the existence of the well-established model organism nematode Caenorhabditis elegans ( Corsi et al, 2015 ), whose genome includes only six Class I PDE genes.…”

Section: Targeting Parasitic Nematode Pdesmentioning

confidence: 99%

Use of a Fission Yeast Platform to Identify and Characterize Small Molecule PDE Inhibitors

Hoffman

2022

Front. Pharmacol.

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Cyclic nucleotide phosphodiesterases (PDEs) have been proven to be targets for which highly selective and potent drugs can be developed. Mammalian genomes possess 21 genes whose products are pharmacologically grouped into 11 families; however related genes from pathogenic organisms display sufficient divergence from the mammalian homologs such that PDE inhibitors to these enzymes could be used to treat parasitic infections without acting on the related human PDEs. We have developed a platform for expressing cloned PDEs in the fission yeast Schizosaccharomyces pombe, allowing for inexpensive, but robust screening for small molecule inhibitors that are cell permeable. Such compounds typically display the expected biological activity when tested in cell culture, including anti-inflammatory properties for PDE4 and PDE7 inhibitors. The genetic pliability of S. pombe also allows for molecular genetic screens to identify mutations in target PDE genes that confer some resistance to these inhibitors as a way of investigating the PDE-inhibitor interaction. This screening method is readily accessible to academic laboratories as it does not require the purification of large quantities of a target protein. This allows for the discovery and profiling of PDE inhibitors to treat inflammation or of inhibitors of targets such as pathogen PDEs for which there may not be a sufficient financial motivation for pharmaceutical companies to identify selective PDE inhibitors using more traditional in vitro enzyme-based screening methods.

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Cloning and functional complementation of ten Schistosoma mansoni phosphodiesterases expressed in the mammalian host stages

Cited by 2 publications

References 92 publications

To Target or Not to Target Schistosoma mansoni Cyclic Nucleotide Phosphodiesterase 4A?

To Target or Not to Target Schistosoma mansoni Cyclic Nucleotide Phosphodiesterase 4A?

Use of a Fission Yeast Platform to Identify and Characterize Small Molecule PDE Inhibitors

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