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      The Roles of Pseudophosphatases in Disease

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          Abstract

          The pseudophosphatases, atypical members of the protein tyrosine phosphatase family, have emerged as bona fide signaling regulators within the past two decades. Their roles as regulators have led to a renaissance of the pseudophosphatase and pseudoenyme fields, catapulting interest from a mere curiosity to intriguing and relevant proteins to investigate. Pseudophosphatases make up approximately fourteen percent of the phosphatase family, and are conserved throughout evolution. Pseudophosphatases, along with pseudokinases, are important players in physiology and pathophysiology. These atypical members of the protein tyrosine phosphatase and protein tyrosine kinase superfamily, respectively, are rendered catalytically inactive through mutations within their catalytic active signature motif and/or other important domains required for catalysis. This new interest in the pursuit of the relevant functions of these proteins has resulted in an elucidation of their roles in signaling cascades and diseases. There is a rapid accumulation of knowledge of diseases linked to their dysregulation, such as neuropathies and various cancers. This review analyzes the involvement of pseudophosphatases in diseases, highlighting the function of various role(s) of pseudophosphatases involvement in pathologies, and thus providing a platform to strongly consider them as key therapeutic drug targets.

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          Differential regulation of MAP kinase signalling by dual-specificity protein phosphatases.

          D. Owens, S Keyse (2007)
          The regulated dephosphorylation of mitogen-activated protein kinases (MAPKs) plays a key role in determining the magnitude and duration of kinase activation and hence the physiological outcome of signalling. In mammalian cells, an important component of this control is mediated by the differential expression and activities of a family of 10 dual-specificity (Thr/Tyr) MAPK phosphatases (MKPs). These enzymes share a common structure in which MAPK substrate recognition is determined by sequences within an amino-terminal non-catalytic domain whereas MAPK binding often leads to a conformational change within the C-terminal catalytic domain resulting in increased enzyme activity. MKPs can either recognize and inactivate a single class of MAP kinase, as in the specific inactivation of extracellular signal regulated kinase (ERK) by the cytoplasmic phosphatase DUSP6/MKP-3 or can regulate more than one MAPK pathway as illustrated by the ability of DUSP1/MKP-1 to dephosphorylate ERK, c-Jun amino-terminal kinase and p38 in the cell nucleus. These properties, coupled with transcriptional regulation of MKP expression in response to stimuli that activate MAPK signalling, suggest a complex negative regulatory network in which individual MAPK activities can be subject to negative feedback control, but also raise the possibility that signalling through multiple MAPK pathways may be integrated at the level of regulation by MKPs.
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            PTEN.

            Carolyn A. Worby, Jack Dixon (2014)
            The importance of PTEN in cellular function is underscored by the frequency of its deregulation in cancer. PTEN tumor-suppressor activity depends largely on its lipid phosphatase activity, which opposes PI3K/AKT activation. As such, PTEN regulates many cellular processes, including proliferation, survival, energy metabolism, cellular architecture, and motility. More than a decade of research has expanded our knowledge about how PTEN is controlled at the transcriptional level as well as by numerous posttranscriptional modifications that regulate its enzymatic activity, protein stability, and cellular location. Although the role of PTEN in cancers has long been appreciated, it is also emerging as an important factor in other diseases, such as diabetes and autism spectrum disorders. Our understanding of PTEN function and regulation will hopefully translate into improved prognosis and treatment for patients suffering from these ailments.
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              The lipid phosphatase activity of PTEN is critical for its tumor supressor function.

              M P Myers, I. PASS, I Batty (1998)
              Since their discovery, protein tyrosine phosphatases have been speculated to play a role in tumor suppression because of their ability to antagonize the growth-promoting protein tyrosine kinases. Recently, a tumor suppressor from human chromosome 10q23, called PTEN or MMAC1, has been identified that shares homology with the protein tyrosine phosphatase family. Germ-line mutations in PTEN give rise to several related neoplastic disorders, including Cowden disease. A key step in understanding the function of PTEN as a tumor suppressor is to identify its physiological substrates. Here we report that a missense mutation in PTEN, PTEN-G129E, which is observed in two Cowden disease kindreds, specifically ablates the ability of PTEN to recognize inositol phospholipids as a substrate, suggesting that loss of the lipid phosphatase activity is responsible for the etiology of the disease. Furthermore, expression of wild-type or substrate-trapping forms of PTEN in HEK293 cells altered the levels of the phospholipid products of phosphatidylinositol 3-kinase and ectopic expression of the phosphatase in PTEN-deficient tumor cell lines resulted in the inhibition of protein kinase (PK) B/Akt and regulation of cell survival.
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                Author and article information

                Contributors
                Marta Vicente-Rodríguez: Role: Academic Editor
                Journal
                Journal ID (nlm-ta): Int J Mol Sci
                Journal ID (iso-abbrev): Int J Mol Sci
                Journal ID (publisher-id): ijms
                Title: International Journal of Molecular Sciences
                Publisher: MDPI
                ISSN (Electronic): 1422-0067
                Publication date (Electronic): 28 June 2021
                Publication date Collection: July 2021
                Volume: 22
                Issue: 13
                Electronic Location Identifier: 6924
                Affiliations
                Integrated Science Center, Department of Biology, College of William and Mary, Williamsburg, VA 23185, USA; ammattei@ 123456email.wm.edu (A.M.M.); jdsmailys@ 123456email.wm.edu (J.D.S.); ewhepworth@ 123456email.wm.edu (E.M.W.H.)
                Author notes
                [* ]Correspondence: sdhinton@ 123456wm.edu ; Tel.: +1-757-221-2587; Fax: +1-757-221-6483
                Article
                Publisher ID: ijms-22-06924
                DOI: 10.3390/ijms22136924
                PMC ID: 8269279
                PubMed ID: 34203203
                SO-VID: 694f2b91-93aa-49d5-aab6-afbe603d11ec
                Copyright © © 2021 by the authors.
                License:

                Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license ( https://creativecommons.org/licenses/by/4.0/).

                History
                Date received : 30 April 2021
                Date accepted : 24 June 2021
                Categories
                Subject: Review

                ScienceOpen disciplines: Molecular biology
                Keywords: pseudoenzymes,pseudophosphatases,protein tyrosine phosphatases (ptps),dual specificity phosphatases (dusps),myotubularin phosphatases (mtms),styx (phosphoserine/threonine/tyrosine-interacting protein),mk-styx (mapk (mitogen-activated protein kinase) phosphoserine/threonine/tyrosine-binding protein),tensin,disease
                Data availability:
                ScienceOpen disciplines: Molecular biology
                Keywords: pseudoenzymes, pseudophosphatases, protein tyrosine phosphatases (ptps), dual specificity phosphatases (dusps), myotubularin phosphatases (mtms), styx (phosphoserine/threonine/tyrosine-interacting protein), mk-styx (mapk (mitogen-activated protein kinase) phosphoserine/threonine/tyrosine-binding protein), tensin, disease

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