Your search keyword '"Melissa R. Pitman"' showing total 44 results

1. Resensitising proteasome inhibitor-resistant myeloma with sphingosine kinase 2 inhibition

Author

Melissa K. Bennett, Manjun Li, Melinda N. Tea, Melissa R. Pitman, John Toubia, Paul P.-S. Wang, Dovile Anderson, Darren J. Creek, Robert Z. Orlowski, Briony L. Gliddon, Jason A. Powell, Craig T. Wallington-Beddoe, and Stuart M. Pitson

Subjects

Myeloma, Bortezomib, Resistance, Sphingolipid, Unfolded protein response, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

The introduction of the proteasome inhibitor bortezomib into treatment regimens for myeloma has led to substantial improvement in patient survival. However, whilst bortezomib elicits initial responses in many myeloma patients, this haematological malignancy remains incurable due to the development of acquired bortezomib resistance. With other patients presenting with disease that is intrinsically bortezomib resistant, it is clear that new therapeutic approaches are desperately required to target bortezomib-resistant myeloma. We have previously shown that targeting sphingolipid metabolism with the sphingosine kinase 2 (SK2) inhibitor K145 in combination with bortezomib induces synergistic death of bortezomib-naïve myeloma. In the current study, we have demonstrated that targeting sphingolipid metabolism with K145 synergises with bortezomib and effectively resensitises bortezomib-resistant myeloma to this proteasome inhibitor. Notably, these effects were dependent on enhanced activation of the unfolded protein response, and were observed in numerous separate myeloma models that appear to have different mechanisms of bortezomib resistance, including a new bortezomib-resistant myeloma model we describe which possesses a clinically relevant proteasome mutation. Furthermore, K145 also displayed synergy with the next-generation proteasome inhibitor carfilzomib in bortezomib-resistant and carfilzomib-resistant myeloma cells. Together, these findings indicate that targeting sphingolipid metabolism via SK2 inhibition may be effective in combination with a broad spectrum of proteasome inhibitors in the proteasome inhibitor resistant setting, and is an approach worth clinical exploration.

Published

2022

2. The sphingosine 1-phosphate receptor 2/4 antagonist JTE-013 elicits off-target effects on sphingolipid metabolism

Author

Melissa R. Pitman, Alexander C. Lewis, Lorena T. Davies, Paul A. B. Moretti, Dovile Anderson, Darren J. Creek, Jason A. Powell, and Stuart M. Pitson

Subjects

Medicine, Science

Abstract

Abstract Sphingosine 1-phosphate (S1P) is a signaling lipid that has broad roles, working either intracellularly through various protein targets, or extracellularly via a family of five G-protein coupled receptors. Agents that selectively and specifically target each of the S1P receptors have been sought as both biological tools and potential therapeutics. JTE-013, a small molecule antagonist of S1P receptors 2 and 4 (S1P2 and S1P4) has been widely used in defining the roles of these receptors in various biological processes. Indeed, our previous studies showed that JTE-013 had anti-acute myeloid leukaemia (AML) activity, supporting a role for S1P2 in the biology and therapeutic targeting of AML. Here we examined this further and describe lipidomic analysis of AML cells that revealed JTE-013 caused alterations in sphingolipid metabolism, increasing cellular ceramides, dihydroceramides, sphingosine and dihydrosphingosine. Further examination of the mechanisms behind these observations showed that JTE-013, at concentrations frequently used in the literature to target S1P2/4, inhibits several sphingolipid metabolic enzymes, including dihydroceramide desaturase 1 and both sphingosine kinases. Collectively, these findings demonstrate that JTE-013 can have broad off-target effects on sphingolipid metabolism and highlight that caution must be employed in interpreting the use of this reagent in defining the roles of S1P2/4.

Published

2022

3. Resensitising proteasome inhibitor-resistant myeloma with sphingosine kinase 2 inhibition

Author

Briony L. Gliddon, Craig T. Wallington-Beddoe, Manjun Li, Darren J. Creek, Melissa R. Pitman, Melinda N. Tea, Paul Wang, Dovile Anderson, John Toubia, Melissa K. Bennett, Robert Z. Orlowski, Stuart M. Pitson, Jason A. Powell, Bennett, Melissa K, Li, Manjun, Tea, Melinda N, Pitman, Melissa R, Toubia, John, Wang, Paul PS, Anderson, Dovile, Creek, Darren J, Orlowski, Robert Z, Gliddon, Briony L, Powell, Jason A, Wallington-Beddoe, Craig T, and Pitson, Stuart M

Subjects

Cancer Research, ATF4, activating transcription factor 4, Resistance, Myeloma, medicine.disease_cause, Sphingolipid, Bortezomib, Unfolded protein response, Gene Knockout Techniques, Mice, chemistry.chemical_compound, UPR, unfolded protein response, GSEA, gene set enrichment analysis, immune system diseases, hemic and lymphatic diseases, Enzyme Inhibitors, RC254-282, Mutation, bortezomib, Sphingosine Kinase 2, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, unfolded protein response, BR, bortezomib resistant, Phosphotransferases (Alcohol Group Acceptor), myeloma, S1P, sphingosine 1-phosphate, Multiple Myeloma, Proteasome Inhibitors, medicine.drug, wt, wild-type, Original article, ATF6, activating transcription factor 6, Cell Survival, IRE1, inositol-requiring enzyme 1, Antineoplastic Agents, resistance, ER, endoplasmic reticulum, Structure-Activity Relationship, Cell Line, Tumor, medicine, Animals, Humans, cardiovascular diseases, neoplasms, SK2, sphingosine kinase 2, Dose-Response Relationship, Drug, business.industry, PERK, protein kinase R-like ER kinase, XBP1s, X-box binding protein 1s, Xenograft Model Antitumor Assays, Carfilzomib, CR, carfilzomib resistant, Disease Models, Animal, Proteasome, chemistry, Drug Resistance, Neoplasm, Proteasome inhibitor, Cancer research, sphingolipid, business

Abstract

Refereed/Peer-reviewed The introduction of the proteasome inhibitor bortezomib into treatment regimens for myeloma has led to substantial improvement in patient survival. However, whilst bortezomib elicits initial responses in many myeloma patients, this haematological malignancy remains incurable due to the development of acquired bortezomib resistance. With other patients presenting with disease that is intrinsically bortezomib resistant, it is clear that new therapeutic approaches are desperately required to target bortezomib-resistant myeloma. We have previously shown that targeting sphingolipid metabolism with the sphingosine kinase 2 (SK2) inhibitor K145 in combination with bortezomib induces synergistic death of bortezomib-naive myeloma. In the current study, we have demonstrated that targeting sphingolipid metabolism with K145 synergises with bortezomib and effectively resensitises bortezomib-resistant myeloma to this proteasome inhibitor Notably, these effects were dependent on enhanced activation of the unfolded protein response, and were observed in numerous separate myeloma models that appear to have different mechanisms of bortezomib resistance, including a new bortezomib-resistant myeloma model we describe which possesses a clinically relevant proteasome mutation. Furthermore, K145 also displayed synergy with the next-generation proteasome inhibitor carfilzomib in bortezomib-resistant and carfilzomib-resistant myeloma cells. Together, these findings indicate that targeting sphingolipid metabolism via SK2 inhibition may be effective in combination with a broad spectrum of proteasome inhibitors in the proteasome inhibitor resistant setting, and is an approach worth clinical exploration.

Published

2022

4. Data from CIB2 Negatively Regulates Oncogenic Signaling in Ovarian Cancer via Sphingosine Kinase 1

Author

Stuart M. Pitson, Melissa R. Pitman, Martin K. Oehler, Paul A.B. Moretti, Houng Taing, Briony L. Gliddon, Lorena T. Davies, Heidi A. Neubauer, Noor A. Lokman, Kate E. Jarman, and Wenying Zhu

Abstract

Sphingosine kinase 1 (SK1) is a key regulator of the cellular balance between proapoptotic and prosurvival sphingolipids. Oncogenic signaling by SK1 relies on its localization to the plasma membrane, which is mediated by the calcium and integrin binding protein CIB1 via its Ca2+-myristoyl switch function. Here we show that another member of the CIB family, CIB2, plays a surprisingly opposite role to CIB1 in the regulation of SK1 signaling. CIB2 bound SK1 on the same site as CIB1, yet it lacks the Ca2+-myristoyl switch function. As a result, CIB2 blocked translocation of SK1 to the plasma membrane and inhibited its subsequent signaling, which included sensitization to TNFα-induced apoptosis and inhibition of Ras-induced neoplastic transformation. CIB2 was significantly downregulated in ovarian cancer and low CIB2 expression was associated with poor prognosis in ovarian cancer patients. Notably, reintroduction of CIB2 in ovarian cancer cells blocked plasma membrane localization of endogenous SK1, reduced in vitro neoplastic growth and tumor growth in mice, and suppressed cell motility and invasiveness both in vitro and in vivo. Consistent with the in vitro synergistic effects between the SK1-specific inhibitor SK1-I and standard chemotherapeutics, expression of CIB2 also sensitized ovarian cancer cells to carboplatin. Together, these findings identify CIB2 as a novel endogenous suppressor of SK1 signaling and potential prognostic marker and demonstrate the therapeutic potential of SK1 in this gynecologic malignancy. Cancer Res; 77(18); 4823–34. ©2017 AACR.

Published

2023

5. Supplementary Methods, Supplementary Figures 1 through 6, and Supplementary Table 1 from CIB2 Negatively Regulates Oncogenic Signaling in Ovarian Cancer via Sphingosine Kinase 1

Author

Stuart M. Pitson, Melissa R. Pitman, Martin K. Oehler, Paul A.B. Moretti, Houng Taing, Briony L. Gliddon, Lorena T. Davies, Heidi A. Neubauer, Noor A. Lokman, Kate E. Jarman, and Wenying Zhu

Abstract

Supplementary Methods. Supplementary Figure S1. Validation of the physiological interaction between CIB2 and SK1 using proximity ligation assays with different antibody combinations. Supplementary Figure S2. N-myristoylation of CIB2 does not affect its interaction with SK1. Supplementary Figure S3. Over-expression of CIB2 sensitises cells to TNFα-induced caspase 3/7 activation. Supplementary Figure S4. Stratification of CIB2 gene expression in ovarian cancer tissues. Supplementary Figure S5. Gene expression of SK1 in ovarian tissues. Supplementary Figure S6. CIB2 inhibits neoplastic growth and cell migration of OV90 ovarian cancer cells. Supplementary Table S1. Clinical characteristics of the ovarian cancer patient cohort from which ovirian cancer cells were derived.

Published

2023

6. Mitochondrial translocation of TFEB regulates complex I and inflammation

Author

Chiara Calabrese, Hendrik Nolte, Melissa R Pitman, Raja Ganesan, Philipp Lampe, Raymond Laboy, Roberto Ripa, Julia Fischer, Sandhya Chipurupalli, Saray Gutierrez, Ruhi Polara, Daniel Thomas, Stuart M Pitson, Adam Antebi, and Nirmal Robinson

Abstract

TFEB is a master regulator of autophagy, lysosome biogenesis and mitochondrial metabolism that works, and immunity, primarily through transcription controlled by cytosol-to-nuclear translocation. Emerging data indicate additional regulatory interactions at the surface of organelles such as lysosomes. Here we show that TFEB has a non-transcriptional role in mitochondria, regulating the electron transport chain complex I to down-modulate inflammation. Proteomic analysis revealed extensive TFEB co-precipitation with several mitochondrial proteins, whose interactions are disrupted upon infection withS.Typhimurium. Localization of TFEB in the mitochondrial matrix was confirmed by high resolution confocal microscopy and biochemistry with translocation dependent on a conserved N-terminal TOMM20-binding motif enhanced by mTOR inhibition. Within the mitochondria, TFEB and protease LONP1 antagonistically co-regulate complex I, reactive oxygen species and the inflammatory response. Consequently, during infection, lack of TFEB specifically in the mitochondria exacerbates the expression of pro-inflammatory cytokines, contributing to innate immune pathogenesis.

Published

2023

7. Disrupted epithelial/macrophage crosstalk via Spinster homologue 2-mediated S1P signaling may drive defective macrophage phagocytic function in COPD.

Author

Hai B Tran, Hubertus Jersmann, Tung Thanh Truong, Rhys Hamon, Eugene Roscioli, Miranda Ween, Melissa R Pitman, Stuart M Pitson, Greg Hodge, Paul N Reynolds, and Sandra Hodge

Subjects

Medicine, Science

Abstract

We have previously established a link between impaired phagocytic capacity and deregulated S1P signaling in alveolar macrophages from COPD subjects. We hypothesize that this defect may include a disruption of epithelial-macrophage crosstalk via Spns2-mediated intercellular S1P signaling.Primary alveolar macrophages and bronchial epithelial cells from COPD subjects and controls, cell lines, and a mouse model of chronic cigarette smoke exposure were studied. Cells were exposed to 10% cigarette smoke extract, or vehicle control. Spns2 expression and subcellular localization was studied by immunofluorescence, confocal microscopy and RT-PCR. Phagocytosis was assessed by flow-cytometry. Levels of intra- and extracellular S1P were measured by S1P [3H]-labeling.Spns2 expression was significantly increased (p

Published

2017

8. Integrated in silico and experimental assessment of disease relevance of PCDH19 missense variants

Author

Stuart M. Pitson, Mark A. Corbett, Stephen P. Robertson, Rebekah de Nys, Heidi E. Kirsch, Deepak Gill, Melissa R. Pitman, Samuel F. Berkovic, Benjamin J. Halliday, Lachlan A. Jolly, Slavé Petrovski, Jozef Gecz, Kavitha Kothur, Kristy L. Kolc, Brigid M. Regan, Alison Gardner, Duyen H. Pham, Ingrid E. Scheffer, Sulekha Rajagopalan, Raman Kumar, Renèe B. Schulz, Sarah E. Heron, Pham, Duyen H, Pitman, Melissa R, Kumar, Raman, Jolly, Lachlan A, Pitson, Stuart M, and Gecz, Jozef

Subjects

medicine.medical_specialty, PCDH19, In silico, Mutation, Missense, Protocadherin, Disease, Computational biology, Biology, functional test, variant assessment, 03 medical and health sciences, Genetics, medicine, Humans, Missense mutation, Relevance (information retrieval), Genetics (clinical), 030304 developmental biology, 0303 health sciences, Epilepsy, Molecular pathology, 030305 genetics & heredity, Sequence Analysis, DNA, Cadherins, Protocadherins, VUS, epilepsy, Medical genetics, Function (biology)

Abstract

PCDH19 is a nonclustered protocadherin molecule involved in axon bundling, synapse function, and transcriptional coregulation. Pathogenic variants in PCDH19 cause infantile-onset epilepsy known as PCDH19-clustering epilepsy or PCDH19-CE. Recent advances in DNA-sequencing technologies have led to a significant increase in the number of reported PCDH19-CE variants, many of uncertain significance. We aimed to determine the best approaches for assessing the disease relevance of missense variants in PCDH19. The application of the American College of Medical Genetics and Association for Molecular Pathology (ACMG-AMP) guidelines was only 50% accurate. Using a training set of 322 known benign or pathogenic missense variants, we identified MutPred2, MutationAssessor, and GPP as the best performing in silico tools. We generated a protein structural model of the extracellular domain and assessed 24 missense variants. We also assessed 24 variants using an in vitro reporter assay. A combination of these tools was 93% accurate in assessing known pathogenic and benign PCDH19 variants. We increased the accuracy of the ACMG-AMP classification of 45 PCDH19 variants from 50% to 94%, using these tools. In summary, we have developed a robust toolbox for the assessment of PCDH19 variant pathogenicity to improve the accuracy of PCDH19-CE variant classification. Refereed/Peer-reviewed

Published

2021

9. Slit-Robo signalling establishes a Sphingosine-1-phosphate gradient to polarise fin mesenchyme

Author

Harsha Mahabaleshwar, PV Asharani, Tricia Yi Loo, Shze Yung Koh, Melissa R Pitman, Samuel Kwok, Jiajia Ma, Bo Hu, Fang Lin, Xue Li Lok, Stuart M Pitson, Timothy E Saunders, Tom J Carney, Lee Kong Chian School of Medicine (LKCMedicine), Institute of Molecular and Cell Biology (IMCB), A*STAR, Mahabaleshwar, Harsha, Asharani, PV, Loo, Tricia Yi, Koh, Shze Yung, Pitman, Melissa R, Kwok, Samuel, Ma, Jiajia, Hu, Bo, Lin, Fang, Li Lok, Xue, Pitson, Stuart M, Saunders, Timothy E, and Carney, Tom J

Subjects

QL, QH, fin, Intracellular Signaling Peptides and Proteins, Gene Expression Regulation, Developmental, Articles, Robo, Zebrafish Proteins, Biochemistry, Mesoderm, Slit, Sphingosine, Genetics, sphingosine-1-phosphate, Animals, Medicine [Science], Mesenchyme, Lysophospholipids, Molecular Biology, Zebrafish

Abstract

Immigration of mesenchymal cells into the growing fin and limb buds drives distal outgrowth, with subsequent tensile forces between these cells essential for fin and limb morphogenesis. Morphogens derived from the apical domain of the fin, orientate limb mesenchyme cell polarity, migration, division and adhesion. The zebrafish mutant stomp displays defects in fin morphogenesis including blister formation and associated loss of orientation and adhesion of immigrating fin mesenchyme cells. Positional cloning of stomp identifies a mutation in the gene encoding the axon guidance ligand, Slit3. We provide evidence that Slit ligands derived from immigrating mesenchyme act via Robo receptors at the apical ectodermal ridge (AER) to promote release of sphingosine-1-phosphate (S1P). S1P subsequently diffuses back to the mesenchyme to promote their polarisation, orientation, positioning and adhesion to the interstitial matrix of the fin fold. We thus demonstrate the coordination of the Slit-Robo and S1P signalling pathways in fin fold morphogenesis. Our work introduces a mechanism regulating the orientation, positioning and adhesion of its constituent cells. Ministry of Education (MOE) Work in the TJC and TES labs was funded by a Ministry of Education of Singapore AcRF Tier 3 grant (MOE2016-T3-1-005). Work in the FL lab was supported by funding from the National Science Foundation, IOS-1354457. SMP is supported by Senior Research Fellowships (1042589and1156693) from the National Health and Medical Research Council of Australia.

Published

2022

10. Ceramide-induced integrated stress response overcomes Bcl-2 inhibitor resistance in acute myeloid leukemia

Author

Alexander C. Lewis, Victoria S. Pope, Melinda N. Tea, Manjun Li, Gus O. Nwosu, Thao M. Nguyen, Craig T. Wallington-Beddoe, Paul A. B. Moretti, Dovile Anderson, Darren J. Creek, Maurizio Costabile, Saira R. Ali, Chloe A. L. Thompson-Peach, B. Kate Dredge, Andrew G. Bert, Gregory J. Goodall, Paul G. Ekert, Anna L. Brown, Richard D’Andrea, Nirmal Robinson, Melissa R. Pitman, Daniel Thomas, David M. Ross, Briony L. Gliddon, Jason A. Powell, Stuart M. Pitson, Lewis, Alexander C, Pope, Victoria S, Tea, Melinda N, Li, Manjun, Nwosu, Gus O, Nguyen, Thao M, Wallington-Beddoe, Craig T, Moretti, Paul AB, Costabile, Maurizio, Ali, Saira R, Dredge, B Kate, Bert, Andrew G, Goodall, Gregory J, Brown, Anna L, D'Andrea, Richard, Robinson, Nirmal, Pitman, Melissa R, Ross, David M, Gliddon, Briony L, Powell, Jason A, and Pitson, Stuart M

Subjects

AML, hemic and lymphatic diseases, Immunology, protein kinase R, Cell Biology, Hematology, ceramide, acute myeloid leukemia, integrated stress response, ISR, Biochemistry

Abstract

Inducing cell death by the sphingolipid ceramide is a potential anticancer strategy, but the underlying mechanisms remain poorly defined. In this study, triggering an accumulation of ceramide in acute myeloid leukemia (AML) cells by inhibition of sphingosine kinase induced an apoptotic integrated stress response (ISR) through protein kinase R–mediated activation of the master transcription factor ATF4. This effect led to transcription of the BH3-only protein Noxa and degradation of the prosurvival Mcl-1 protein on which AML cells are highly dependent for survival. Targeting this novel ISR pathway, in combination with the Bcl-2 inhibitor venetoclax, synergistically killed primary AML blasts, including those with venetoclax-resistant mutations, as well as immunophenotypic leukemic stem cells, and reduced leukemic engraftment in patient-derived AML xenografts. Collectively, these findings provide mechanistic insight into the anticancer effects of ceramide and preclinical evidence for new approaches to augment Bcl-2 inhibition in the therapy of AML and other cancers with high Mcl-1 dependency.

Published

2022

11. Slit-Robo Signalling Establishes a Sphingosine-1-Phosphate Gradient to Polarise Fin Mesenchyme and Establish Fin Morphology

Author

Harsha Mahabaleshwar, P.V. Asharani, Tricia Loo Yi Jun, Shze Yung Koh, Melissa R. Pitman, Samuel Kwok, Jiajia Ma, Bo Hu, Fang Lin, Xue Li Lok, Stuart M. Pitson, Timothy E. Saunders, and Tom J. Carney

Abstract

SUMMARYImmigration of mesenchymal cells into the growing fin and limb buds drives distal outgrowth, with subsequent tensile forces between these cells essential for fin and limb morphogenesis. Morphogens derived from the apical domain of the fin, orientate limb mesenchyme cell polarity, migration, division and adhesion. The zebrafish mutant stomp displays defects in fin morphogenesis including blister formation and associated loss of orientation and adhesion of immigrating fin mesenchyme cells. Positional cloning of stomp identified a mutation in the gene encoding the axon guidance ligand, Slit3. We provide evidence that Slit ligands derived from immigrating mesenchyme act via Robo receptors at the Apical Ectodermal Ridge (AER) to promote release of sphingosine-1-phosphate (S1P). S1P subsequently diffuses back to the mesenchyme to promote their polarisation, orientation, positioning and adhesion to the interstitial matrix of the fin fold. We thus demonstrate coordination of the Slit-Robo and S1P signalling pathways in fin fold morphogenesis. Our work introduces a mechanism regulating the orientation, positioning and adhesion of its constituent cells.

Published

2021

12. In vitro and in vivo roles of sphingosine kinase 2 during dengue virus infection

Author

Jennifer N. Clarke, Julie K. Calvert, Amanda L. Aloia, Lorena T. Davies, Melissa R. Pitman, Jillian M. Carr, Wisam H. Al-Shujairi, Stuart M. Pitson, Al-Shujairi, Wisam H, Clarke, Jennifer N, Davies, Lorena T, Pitman, Melissa R, Calvert, Julie K, Aloia, Amanda L, Pitson, Stuart M, and Carr, Jillian M

Subjects

0301 basic medicine, Pyridines, sphingosine kinase 2, viruses, 030106 microbiology, Sphingosine kinase, Adamantane, CD8-Positive T-Lymphocytes, Dengue virus, Biology, medicine.disease_cause, Cell Line, Dengue, Mice, 03 medical and health sciences, Sphingosine, In vivo, Cell Line, Tumor, Virology, medicine, Animals, Humans, CXCL10, RNA, Messenger, virus diseases, Sphingosine Kinase 2, Hep G2 Cells, Interferon-beta, Dengue Virus, biochemical phenomena, metabolism, and nutrition, dengue virus infection, dengue, In vitro, Mice, Inbred C57BL, Phosphotransferases (Alcohol Group Acceptor), HEK293 Cells, 030104 developmental biology, sphingosine kinases, Viperin, Thiazolidinediones, Lysophospholipids, CD8

Abstract

There is growing evidence of the influence of sphingosine kinase (SK) enzymes on viral infection. Here, the role of sphingosine kinase 2 (SK2), an isoform of SK prominent in the brain, was defined during dengue virus (DENV) infection. Chemical inhibition of SK2 activity using two different SK2 inhibitors, ABC294640 and K145, had no effect on DENV infection in human cells in vitro. In contrast, DENV infection was restricted in SK2⁻/⁻ immortalized mouse embryonic fibroblasts (iMEFs) with reduced induction of IFN-β mRNA and protein, and mRNA for the IFN-stimulated genes (ISGs) viperin, IFIT1, IRF7 and CXCL10 in DENV-infected SK2⁻/⁻ compared to WT iMEFs. Intracranial (ic) DENV injection in C57BL/6 SK2⁻/⁻mice induced body weight loss earlier than in WT mice but DENV RNA levels were comparable in the brain. Neither SK1 mRNA or sphingosine-1-phosphate (S1P) levels were altered following ic DENV infection in WT or SK2⁻/⁻ mice but brain S1P levels were reduced in all SK2⁻/⁻ mice, independent of DENV infection. CD8 mRNA was induced in the brains of both DENV-infected WT and SK2⁻/⁻ mice, suggesting normal CD8+ T-cell infiltration into the DENV-infected brain independent of SK2 or S1P. Thus, although SK2 may be important for replication of some viruses SK2 activity does not affect DENV infection in vitro and SK2 or S1P levels do not influence DENV infection or T-cell infiltration in the context of infection in the brain. Refereed/Peer-reviewed

Published

2019

13. Mitochondrial Translocation of TFEB Regulates Complex I and Inflammation

Author

Melissa R. Pitman, Adam Antebi, Saray Gutiérrez, Philipp A Lampe, Stuart M. Pitson, Sandhya Chipurupalli, Raja Ganesan, Chiara Calabrese, Nirmal Robinson, Julia Fischer, Hendrik Nolte, Raymond Laboy, and Robeto Ripa

Subjects

medicine.anatomical_structure, Downregulation and upregulation, Mitochondrial matrix, Chemistry, Lysosome, Autophagy, medicine, Transcriptional regulation, TFEB, Mitochondrion, Biogenesis, Cell biology

Abstract

TFEB is an important transcriptional regulator of autophagy, lysosome biogenesis, and immunity, whose activity is regulated by cytosol-to-nuclear translocation through downregulation of the nutrient sensor mTOR. Here we show that TFEB has a non-transcriptional role in mitochondria essential for the regulation of mitochondrial complex I and inflammation. Proteomic analysis revealed that TFEB co-precipitates with several mitochondrial proteins, whose interactions are perturbed in S. Typhimurium infected cells. High resolution microscopy and biochemical experiments further confirmed that TFEB localizes in the mitochondrial matrix. TFEB mitochondrial translocation depends on a conserved TOMM20 binding motif within the protein sequence and is enhanced upon the inhibition of mTOR. Within the mitochondria, TFEB and protease LONP1 antagonistically co-regulate complex I, ROS production and the inflammatory response. Consequently, during S. Typhimurium infection, lack of TFEB specifically in the mitochondria exacerbates the expression of pro-inflammatory cytokines, contributing to pathogenesis.

Published

2021

14. Sphingosine kinase 2 inhibition synergises with bortezomib to target myeloma by enhancing endoplasmic reticulum stress

Author

Craig T. Wallington-Beddoe, Melissa R. Pitman, Melissa K. Bennett, Andrew C.W. Zannettino, Paul A.B. Moretti, Julia R. Zebol, Duncan R. Hewett, Kate Vandyke, Stuart M. Pitson, Lorena T. Davies, Wallington-Beddoe, Craig T, Bennett, Melissa K, Vandyke, Kate, Davies, Lorena, Zebol, Julia R, Moretti, Paul AB, Pitman, Melissa R, Hewett, Duncan R, Zannettino, Andrew CW, and Pitson, Stuart M

Subjects

0301 basic medicine, Sphingosine kinase, Antineoplastic Agents, Apoptosis, Models, Biological, Bortezomib, 03 medical and health sciences, 0302 clinical medicine, immune system diseases, hemic and lymphatic diseases, Cell Line, Tumor, medicine, Animals, Humans, Molecular Targeted Therapy, Cell Death, Dose-Response Relationship, Drug, proteasome inhibitor, Kinase, business.industry, Endoplasmic reticulum, Sphingosine Kinase 2, Drug Synergism, Endoplasmic Reticulum Stress, Xenograft Model Antitumor Assays, Sphingolipid, 3. Good health, Disease Models, Animal, Phosphotransferases (Alcohol Group Acceptor), endoplasmic reticulum, myeloma, 030104 developmental biology, Oncology, sphingosine kinase, 030220 oncology & carcinogenesis, Immunology, Proteasome inhibitor, Unfolded protein response, Cancer research, Multiple Myeloma, business, Proteasome Inhibitors, Priority Research Paper, medicine.drug

Abstract

// Craig T. Wallington-Beddoe 1,2,3 , Melissa K. Bennett 1,2,3 , Kate Vandyke 2,3,4 , Lorena Davies 1,2 , Julia R. Zebol 1,2 , Paul A.B. Moretti 1,2 , Melissa R. Pitman 1,2 , Duncan R. Hewett 3,4 , Andrew C.W. Zannettino 1,2,3,4,* and Stuart M. Pitson 1,2,3,* 1 Center for Cancer Biology, University of South Australia, Adelaide, Australia 2 SA Pathology, Adelaide, Australia 3 School of Medicine, University of Adelaide, Australia 4 South Australian Health and Medical Research Institute, Adelaide, Australia * Co-senior authorship of this article Correspondence to: Andrew C.W. Zannettino, email: // Stuart M. Pitson, email: // Keywords : myeloma, endoplasmic reticulum, proteasome inhibitor, sphingosine kinase Received : March 29, 2017 Accepted : April 04, 2017 Published : April 14, 2017 Abstract The proteasome inhibitor bortezomib has proven to be invaluable in the treatment of myeloma. By exploiting the inherent high immunoglobulin protein production of malignant plasma cells, bortezomib induces endoplasmic reticulum (ER) stress and the unfolded protein response (UPR), resulting in myeloma cell death. In most cases, however, the disease remains incurable highlighting the need for new therapeutic targets. Sphingosine kinase 2 (SK2) has been proposed as one such therapeutic target for myeloma. Our observations that bortezomib and SK2 inhibitors independently elicited induction of ER stress and the UPR prompted us to examine potential synergy between these agents in myeloma. Targeting SK2 synergistically contributed to ER stress and UPR activation induced by bortezomib, as evidenced by activation of the IRE1 pathway and stress kinases JNK and p38MAPK, thereby resulting in potent synergistic myeloma apoptosis in vitro . The combination of bortezomib and SK2 inhibition also exhibited strong in vivo synergy and favourable effects on bone disease. Therefore, our studies suggest that perturbations of sphingolipid signalling can synergistically enhance the effects seen with proteasome inhibition, highlighting the potential for the combination of these two modes of increasing ER stress to be formally evaluated in clinical trials for the treatment of myeloma patients.

Published

2017

15. Targeting sphingosine kinase 1 induces MCL1-dependent cell death in acute myeloid leukemia

Author

Saumya E. Samaraweera, Diana Iarossi, Alexander C. Lewis, Ian D. Lewis, Angel F. Lopez, Melissa R. Pitman, Richard J D'Andrea, Andrew H. Wei, Hayley S. Ramshaw, Craig T. Wallington-Beddoe, John Toubia, Stuart M. Pitson, Jason A. Powell, Wenying Zhu, Nik Cummings, Daniel Thomas, Paul A.B. Moretti, Powell, Jason A, Lewis, Alexander C, Zhu, Wenying, Toubia, John, Pitman, Melissa R, Wallington-Beddoe, Craig T, Moretti, Paul AB, Iarossi, Diana, Samaraweera, Saumya E, Cummings, Nik, Ramshaw, Hayley S, Thomas, Daniel, Wei, Andrew H, Lopez, Angel F, D'Andrea, Richard J, Lewis, Ian D, and Pitson, Stuart M

Subjects

0301 basic medicine, Myeloid, CD34, Biochemistry, myeloid leukemia, Amino Acid Chloromethyl Ketones, Mice, chemistry.chemical_compound, Mice, Inbred NOD, Sphingosine, hemic and lymphatic diseases, Molecular Targeted Therapy, human AML cells, Myeloid Neoplasia, Cell Death, biology, Gene Expression Regulation, Leukemic, Myeloid leukemia, Hematology, Amino Alcohols, Caspase Inhibitors, Leukemia, Myeloid, Acute, Phosphotransferases (Alcohol Group Acceptor), Receptors, Lysosphingolipid, Leukemia, xenografts, medicine.anatomical_structure, Sphingosine kinase 1, Caspases, Neoplastic Stem Cells, Quinolines, Female, Signal Transduction, Immunology, Bone Marrow Cells, SPHK1, 03 medical and health sciences, Cell Line, Tumor, medicine, aspase-dependent cell death, Animals, Humans, Progenitor cell, Protein Kinase Inhibitors, MCL1 degradation, Cell Biology, medicine.disease, Survival Analysis, Xenograft Model Antitumor Assays, Myeloid Cell Leukemia Sequence 1 Protein, 030104 developmental biology, chemistry, Cancer research, biology.protein, Lysophospholipids

Abstract

Acute myeloid leukemia (AML) is an aggressive malignancy where despite improvements in conventional chemotherapy and bone marrow transplantation, overall survival remains poor. Sphingosine kinase 1 (SPHK1) generates the bioactive lipid sphingosine 1- phosphate (S1P) and has established roles in tumor initiation, progression, and chemotherapy resistance in a wide range of cancers. The role and targeting of SPHK1 in primary AML, however, has not been previously investigated. HereweshowthatSPHK1is overexpressed and constitutively activated in primary AML patient blasts but not in normal mononuclear cells. Subsequent targeting of SPHK1 induced caspase-dependent cell death inAMLcell lines, primary AML patient blasts, and isolated AML patient leukemic progenitor/stem cells, with negligible effects on normal bone marrow CD34 + progenitors from healthy donors. Furthermore, administration of SPHK1 inhibitors to orthotopic AML patient-derived xenografts reduced tumor burden and prolonged overall survival without affecting murine hematopoiesis. SPHK1 inhibition was associated with reduced survival signaling from S1P receptor 2, resulting in selective down regulation of the prosurvival protein MCL1. Subsequent analysis showed that the combination of BH3 mimetics with either SPHK1 inhibition or S1P receptor 2 antagonism triggered synergistic AML cell death. These results support the notion that SPHK1 is a bona fide therapeutic target for the treatment of AML. Refereed/Peer-reviewed

Published

2017

16. Kelch-like protein 5-mediated ubiquitination of lysine 183 promotes proteasomal degradation of sphingosine kinase 1

Author

Alexander C. Lewis, Paul A.B. Moretti, Melissa R. Pitman, Stuart M. Pitson, Jason A. Powell, Maurizio Costabile, Julia R. Zebol, Lorena T. Davies, Laura F. Dagley, Andrew I. Webb, Heidi A. Neubauer, Powell, Jason A, Pitman, Melissa R, Zebol, Julia R, Moretti, Paul AB, Neubauer, Heidi A, Davies, Lorena T, Lewis, Alexander C, Dagley, Laura F, Webb, Andrew I, Costabile, Maurizio, and Pitson, Stuart M

Subjects

Proteasome Endopeptidase Complex, Amino Acid Motifs, Sphingosine kinase, Protein degradation, ubiquitin ligase, Biochemistry, chemistry.chemical_compound, Ubiquitin, Humans, Molecular Biology, biology, Sphingosine, protein turnover, Lysine, Microfilament Proteins, Ubiquitination, Cell Biology, Cullin Proteins, Ubiquitin ligase, Cell biology, Phosphotransferases (Alcohol Group Acceptor), proteasome, Sphingosine kinase 1, chemistry, sphingosine kinase, Ubiquitin ligase complex, Proteolysis, protein degradation, biology.protein, Carrier Proteins, Cullin

Abstract

Sphingosine kinase 1 (SK1) is a signalling enzyme that catalyses the phosphorylation of sphingosine to generate the bioactive lipid sphingosine 1-phosphate (S1P). A number of SK1 inhibitors and chemotherapeutics can induce the degradation of SK1, with the loss of this pro-survival enzyme shown to significantly contribute to the anti-cancer properties of these agents. Here we define the mechanistic basis for this degradation of SK1 in response to SK1 inhibitors, chemotherapeutics, and in natural protein turnover. Using an inducible SK1 expression system that enables the degradation of pre-formed SK1 to be assessed independent of transcriptional or translational effects, we found that SK1 was degraded primarily by the proteasome since several proteasome inhibitors blocked SK1 degradation, while lysosome, cathepsin B or pan caspase inhibitors had no effect. Importantly, we demonstrate that this proteasomal degradation of SK1 was enabled by its ubiquitination at Lys183 that appears facilitated by SK1 inhibitor-induced conformational changes in the structure of SK1 around this residue. Furthermore, using yeast two-hybrid screening, we identified Kelch-like protein 5 (KLHL5) as an important protein adaptor linking SK1 to the cullin 3 (Cul3) ubiquitin ligase complex. Notably, knockdown of KLHL5 or Cul3, use of a cullin inhibitor or a dominant-negative Cul3 all attenuated SK1 degradation. Collectively this data demonstrates the KLHL5/Cul3-based E3 ubiquitin ligase complex is important for regulation of SK1 protein stability via Lys183 ubiquitination, in response to SK1 inhibitors, chemotherapy and for normal SK1 protein turnover. Refereed/Peer-reviewed

Published

2019

17. Cytoplasmic dynein regulates the subcellular localization of sphingosine kinase 2 to elicit tumor-suppressive functions in glioblastoma

Author

Cassandra Stefanidis, Claudine S. Bonder, Briony L. Gliddon, Maurizio Costabile, Melinda N. Tea, Melissa R. Pitman, Julia R. Zebol, Paul A.B. Moretti, Heidi A. Neubauer, Brett W. Stringer, Bryan W. Day, Stuart M. Pitson, Jason A. Powell, Jasreen Kular, Michael S. Samuel, Neubauer, Heidi A, Tea, Melinda N, Zebol, Julia R, Gliddon, Briony L, Stefanidis, Cassandra, Moretti, Paul AB, Pitman, Melissa R, Costabile, Maurizio, Kular, Jasreen, Stringer, Brett W, Day, Bryan W, Samuel, Michael S, Bonder, Claudine S, Powell, Jason A, and Pitson, Stuart M

Subjects

0301 basic medicine, Cytoplasmic Dyneins, Cancer Research, Carcinogenesis, Apoptosis, Biology, Article, Cell membrane, 03 medical and health sciences, chemistry.chemical_compound, Mice, 0302 clinical medicine, Sphingosine, Cell Line, Tumor, Genetics, medicine, Animals, Humans, Genes, Tumor Suppressor, Molecular Biology, Cell Proliferation, Kinase, Cell growth, Endoplasmic reticulum, Cell Membrane, Sphingosine Kinase 2, cell signalling, Subcellular localization, Xenograft Model Antitumor Assays, Cell biology, Gene Expression Regulation, Neoplastic, CNS cancer, Phosphotransferases (Alcohol Group Acceptor), 030104 developmental biology, medicine.anatomical_structure, HEK293 Cells, chemistry, Cytoplasm, 030220 oncology & carcinogenesis, Lysophospholipids, Glioblastoma

Abstract

While the two mammalian sphingosine kinases, SK1 and SK2, both catalyze the generation of pro-survival sphingosine 1-phosphate (S1P), their roles vary dependent on their different subcellular localization. SK1 is generally found in the cytoplasm or at the plasma membrane where it can promote cell proliferation and survival. SK2 can be present at the plasma membrane where it appears to have a similar function to SK1, but can also be localized to the nucleus, endoplasmic reticulum or mitochondria where it mediates cell death. Although SK2 has been implicated in cancer initiation and progression, the mechanisms regulating SK2 subcellular localization are undefined. Here, we report that SK2 interacts with the intermediate chain subunits of the retrograde-directed transport motor complex, cytoplasmic dynein 1 (DYNC1I1 and -2), and we show that this interaction, particularly with DYNC1I1, facilitates the transport of SK2 away from the plasma membrane. DYNC1I1 is dramatically downregulated in patient samples of glioblastoma (GBM), where lower expression of DYNC1I1 correlates with poorer patient survival. Notably, low DYNC1I1 expression in GBM cells coincided with more SK2 localized to the plasma membrane, where it has been recently implicated in oncogenesis. Re-expression of DYNC1I1 reduced plasma membrane-localized SK2 and extracellular S1P formation, and decreased GBM tumor growth and tumor-associated angiogenesis in vivo. Consistent with this, chemical inhibition of SK2 reduced the viability of patient-derived GBM cells in vitro and decreased GBM tumor growth in vivo. Thus, these findings demonstrate a tumor-suppressive function of DYNC1I1, and uncover new mechanistic insights into SK2 regulation which may have implications in targeting this enzyme as a therapeutic strategy in GBM. Refereed/Peer-reviewed

Published

2019

18. Proteasomal degradation of sphingosine kinase 1 and inhibition of dihydroceramide desaturase by the sphingosine kinase inhibitors, SKi or ABC294640, induces growth arrest in androgen-independent LNCaP-AI prostate cancer cells

Author

Nigel J. Pyne, Melissa R. Pitman, Melissa McNaughton, Stuart M. Pitson, Susan Pyne, McNaughton, Melissa, Pitman, Melissa, Pitson, Stuart M, Pyne, Nigel J, and Pyne, Susan

Subjects

Male, 0301 basic medicine, Proteasome Endopeptidase Complex, Pyridines, Sphingosine kinase, Adamantane, Antineoplastic Agents, RS, RC0254, 03 medical and health sciences, chemistry.chemical_compound, Prostate cancer, 0302 clinical medicine, Cell Line, Tumor, LNCaP, medicine, Humans, Sphingosine-1-phosphate, sphingosine 1-phosphate, Sphingosine, biology, Cell Cycle Checkpoints, Dihydroceramide desaturase, prostate cancer, medicine.disease, Phosphotransferases (Alcohol Group Acceptor), Prostatic Neoplasms, Castration-Resistant, Thiazoles, growth arrest, 030104 developmental biology, Fenretinide, Oncology, chemistry, Biochemistry, Sphingosine kinase 1, sphingosine kinase, 030220 oncology & carcinogenesis, dihydroceramide desaturase, Cancer research, biology.protein, Oxidoreductases, Research Paper

Abstract

Sphingosine kinases (two isoforms termed SK1 and SK2) catalyse the formation of the bioactive lipid sphingosine 1-phosphate. We demonstrate here that the SK2 inhibitor, ABC294640 (3-(4-chlorophenyl)-adamantane-1-carboxylic acid (pyridin-4-ylmethyl)amide) or the SK1/SK2 inhibitor, SKi (2-(p-hydroxyanilino)-4-(p-chlorophenyl)thiazole)) induce the proteasomal degradation of SK1a (Mr = 42 kDa) and inhibit DNA synthesis in androgen-independent LNCaP-AI prostate cancer cells. These effects are recapitulated by the dihydroceramide desaturase (Des1) inhibitor, fenretinide. Moreover, SKi or ABC294640 reduce Des1 activity in Jurkat cells and ABC294640 induces the proteasomal degradation of Des1 (Mr = 38 kDa) in LNCaP-AI prostate cancer cells. Furthermore, SKi or ABC294640 or fenretinide increase the expression of the senescence markers, p53 and p21 in LNCaP-AI prostate cancer cells. The siRNA knockdown of SK1 or SK2 failed to increase p53 and p21 expression, but the former did reduce DNA synthesis in LNCaP-AI prostate cancer cells. Moreover, N-acetylcysteine (reactive oxygen species scavenger) blocked the SK inhibitor-induced increase in p21 and p53 expression but had no effect on the proteasomal degradation of SK1a. In addition, siRNA knockdown of Des1 increased p53 expression while a combination of Des1/SK1 siRNA increased the expression of p21. Therefore, Des1 and SK1 participate in regulating LNCaP-AI prostate cancer cell growth and this involves p53/p21-dependent and -independent pathways. Therefore, we propose targeting androgen-independent prostate cancer cells with compounds that affect Des1/SK1 to modulate both de novo and sphingolipid rheostat pathways in order to induce growth arrest. Refereed/Peer-reviewed

Published

2016

19. An improved isoform-selective assay for sphingosine kinase 1 activity

Author

Lorena T. Davies, Melissa R. Pitman, Stuart M. Pitson, Pitman, Melissa R, Davies, Lorena T, and Pitson, Stuart M

Subjects

0301 basic medicine, Bligh-dyer extraction, d-erythro-sphingosine, Sphingosine, biology, Kinase, Sphingosine kinase, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, chemistry, Sphingosine kinase 1, Biochemistry, Sphingosine 1-phosphate, Second messenger system, biology.protein, lipids (amino acids, peptides, and proteins), Sphingosine-1-phosphate, Receptor, Cellular localization

Abstract

Sphingosine kinases (SK) are the sole enzymes responsible for the production of sphingosine 1-phosphate (S1P). S1P is a signaling molecule with a plethora of targets, acting as both a second messenger intracellularly and extracellularly via a family of cell surface G-protein-coupled S1P receptors. The two sphingosine kinases, SK1 and SK2, arise from different genes and have some distinct and overlapping cellular functions that are regulated in part by differential cellular localization, developmental expression, and catalytic properties. Here, we describe an improved method for selectively detecting SK1 activity in vitro and cell lysates via the use of the zwitterionic detergent CHAPS, which effectively inhibits SK2 activity and thus allows selective analysis of SK1 activity in a range of cell samples. The assay measures the production of 32 P-labeled S1P following the addition of exogenous sphingosine and [γ 32 P]ATP. The S1P product can be purified by Bligh–Dyer solvent extraction, separated by thin layer chromatography (TLC), and the radiolabeled S1P quantified by exposing the TLC plate to a storage phosphor screen. This sensitive, reproducible assay can be used to selectively detect SK1 activity in tissue, cell, and recombinant protein samples.

Published

2018

20. Differential expression of the S1P transporter, Spinster homologue 2 (Spns2), in airway epithelial cells and macrophages may drive defective macrophage function in COPD

Author

Rhys Hamon, Paul N. Reynolds, Greg Hodge, Miranda P. Ween, Melissa R. Pitman, Stuart M. Pitson, Hubertus Jersmann, Eugene Roscioli, Tung Thanh Truong, Sandra Hodge, and Hai B. Tran

Subjects

medicine.diagnostic_test, business.industry, Cell culture, Cytoplasm, Phagocytosis, Extracellular, medicine, Subcellular localization, Immunofluorescence, business, Nuclear localization sequence, Intracellular, Cell biology

Abstract

We previously established a link between impaired phagocytosis and deregulated S1P signaling in alveolar macrophages in COPD. We hypothesized that this may result from disrupted epithelial-macrophage crosstalk via Spns2-mediated intercellular S1P signaling. Alveolar macrophages and bronchial epithelial cells from COPD subjects and controls, cigarette smoke (CS)-exposed mice, and CS-exposed cell lines were studied. Spns2 expression and subcellular localization was studied by immunofluorescence, confocal microscopy and RT-PCR. Phagocytosis was assessed by flow-cytometry. Levels of intra- and extracellular S1P were measured by S1P [3H]-labeling. In both macrophage and epithelial cells, Spns2 was localized to cytoplasm and nucleus, consistent with predicted bipartile Nuclear Localization Signal at the position aa282 of the human Spns2 sequence. In alveolar macrophages from 4 current-smoker COPD patients, Spns2 expression was significantly increased compared to 7 non-smoker controls. Spns2 was also increased in both human alveolar and THP-1 macrophages exposed to CS. In contrast, a remarkable Spns2 down-regulation was noted in CS-exposed 16HBE epithelial cells (p

Published

2017

21. An Improved Isoform-Selective Assay for Sphingosine Kinase 1 Activity

Author

Melissa R, Pitman, Lorena T, Davies, and Stuart M, Pitson

Subjects

Phosphotransferases (Alcohol Group Acceptor), Sphingosine, Detergents, Animals, Humans, Cholic Acids, Chromatography, Thin Layer, Lysophospholipids, Signal Transduction

Abstract

Sphingosine kinases (SK) are the sole enzymes responsible for the production of sphingosine 1-phosphate (S1P). S1P is a signaling molecule with a plethora of targets, acting as both a second messenger intracellularly and extracellularly via a family of cell surface G-protein-coupled S1P receptors. The two sphingosine kinases, SK1 and SK2, arise from different genes and have some distinct and overlapping cellular functions that are regulated in part by differential cellular localization, developmental expression, and catalytic properties. Here, we describe an improved method for selectively detecting SK1 activity in vitro and cell lysates via the use of the zwitterionic detergent CHAPS, which effectively inhibits SK2 activity and thus allows selective analysis of SK1 activity in a range of cell samples. The assay measures the production of

Published

2017

22. CIB1 contributes to oncogenic signalling by Ras via modulating the subcellular localisation of sphingosine kinase 1

Author

Andrew Ruszkiewicz, Stuart M. Pitson, Jason A. Powell, Briony L. Gliddon, Wenying Zhu, T. Tin, Melissa R. Pitman, Paul A.B. Moretti, Leslie V. Parise, Joanna M. Woodcock, Kate E. Jarman, Zhu, W, Gliddon, BL, Jarman, KE, Moretti, PAB, Tin, T, Parise, LV, Woodcock, JM, Powell, JA, Ruszkiewicz, A, Pitman, MR, and Pitson, SM

Subjects

0301 basic medicine, Cancer Research, Carcinogenesis, Cell Survival, sphingosine kinase 1, Biology, medicine.disease_cause, oncogenic signalling, Article, Proto-Oncogene Proteins p21(ras), 03 medical and health sciences, 0302 clinical medicine, Growth factor receptor, Downregulation and upregulation, Cell Line, Tumor, Neoplasms, Genetics, medicine, Humans, Neoplastic transformation, HRAS, Molecular Biology, Integrin binding, Calcium-Binding Proteins, Cell Membrane, Cell biology, CIB1, Gene Expression Regulation, Neoplastic, Phosphotransferases (Alcohol Group Acceptor), 030104 developmental biology, Sphingosine kinase 1, sphingosine kinase, 030220 oncology & carcinogenesis, Cancer research, biology.protein, Calcium, Ectopic expression, plasma membrane localisation, Ras

Abstract

CIB1 (calcium and integrin binding protein 1) is a small intracellular protein with numerous interacting partners, and hence has been implicated in various cellular functions. Recent studies have revealed emerging roles of CIB1 in regulating cancer cell survival and angiogenesis, although the mechanisms involved have remained largely undefined. In investigating the oncogenic function of CIB1, we initially found that CIB1 is widely up-regulated across a diverse range of cancers, with this upregulation frequently correlating with oncogenic mutations of KRas. Consistent with this, we found that ectopic expression of oncogenic KRas and HRas in cells resulted in elevated CIB1 expression. We previously described the Ca2+-myristoyl switch function of CIB1, and its ability to facilitate agonist-induced plasma membrane localisation of sphingosine kinase 1 (SK1), a location where SK1 is known to elicit oncogenic signalling. Thus, we examined the role this may play in oncogenesis. Consistent with these findings, we demonstrated here that over-expression of CIB1 by itself is sufficient to drive localisation of SK1 to the plasma membrane and enhance the membrane-associated enzymatic activity of SK1, as well as its oncogenic signalling. We subsequently demonstrated that elevated levels of CIB1 resulted in full neoplastic transformation, in a manner dependent on SK1. In agreement with our previous findings that SK1 is a downstream mediator of oncogenic signalling by Ras, we found that targeting CIB1 also inhibited neoplastic growth of cells induced by oncogenic Ras, suggesting an important pro-tumorigenic role for CIB1. Thus, we have demonstrated for the first time a role for CIB1 in neoplastic transformation, and revealed a novel mechanism facilitating oncogenic signalling by Ras and SK1 Refereed/Peer-reviewed

Published

2017

23. CIB2 negatively regulates oncogenic signaling in ovarian cancer via sphingosine kinase 1

Author

Noor A. Lokman, Paul A.B. Moretti, Stuart M. Pitson, Wenying Zhu, Briony L. Gliddon, Melissa R. Pitman, Heidi A. Neubauer, Kate E. Jarman, Martin K. Oehler, Lorena T. Davies, Houng Taing, Zhu, Wenying, Jarman, Kate E, Lokman, Noor A, Neubauer, Heidi A, Davies, Lorena T, Gliddon, Briony L, Taing, Houng, Moretti, Paul AB, Oehler, Martin K, Pitman, Melissa R, and Pitson, Stuart M

Subjects

0301 basic medicine, Cancer Research, Apoptosis, Mice, SCID, Mice, 03 medical and health sciences, Cell Movement, Mice, Inbred NOD, Biomarkers, Tumor, Tumor Cells, Cultured, medicine, Animals, Humans, Neoplasm Invasiveness, Neoplastic transformation, Cell Proliferation, Neoplasm Staging, Integrin binding, Ovarian Neoplasms, biology, Cell growth, Calcium-Binding Proteins, Cancer, Prognosis, medicine.disease, Xenograft Model Antitumor Assays, Sphingolipid, Cell biology, Gene Expression Regulation, Neoplastic, Phosphotransferases (Alcohol Group Acceptor), 030104 developmental biology, Oncology, Sphingosine kinase 1, biology.protein, Female, Ovarian cancer

Abstract

Sphingosine kinase 1 (SK1) is a key regulator of the cellular balance between proapoptotic and prosurvival sphingolipids. Oncogenic signaling by SK1 relies on its localization to the plasma membrane, which is mediated by the calcium and integrin binding protein CIB1 via its Ca2+-myristoyl switch function. Here we show that another member of the CIB family, CIB2, plays a surprisingly opposite role to CIB1 in the regulation of SK1 signaling. CIB2 bound SK1 on the same site as CIB1, yet it lacks the Ca2+-myristoyl switch function. As a result, CIB2 blocked translocation of SK1 to the plasma membrane and inhibited its subsequent signaling, which included sensitization to TNFα-induced apoptosis and inhibition of Ras-induced neoplastic transformation. CIB2 was significantly downregulated in ovarian cancer and low CIB2 expression was associated with poor prognosis in ovarian cancer patients. Notably, reintroduction of CIB2 in ovarian cancer cells blocked plasma membrane localization of endogenous SK1, reduced in vitro neoplastic growth and tumor growth in mice, and suppressed cell motility and invasiveness both in vitro and in vivo. Consistent with the in vitro synergistic effects between the SK1-specific inhibitor SK1-I and standard chemotherapeutics, expression of CIB2 also sensitized ovarian cancer cells to carboplatin. Together, these findings identify CIB2 as a novel endogenous suppressor of SK1 signaling and potential prognostic marker and demonstrate the therapeutic potential of SK1 in this gynecologic malignancy. Cancer Res; 77(18); 4823–34. ©2017 AACR.

Published

2017

24. Disrupted epithelial/macrophage crosstalk via Spinster homologue 2-mediated S1P signaling may drive defective macrophage phagocytic function in COPD

Author

Hubertus Jersmann, Melissa R. Pitman, Rhys Hamon, Tung Thanh Truong, Stuart M. Pitson, Eugene Roscioli, Miranda P. Ween, Hai B. Tran, Sandra Hodge, Greg Hodge, Paul N. Reynolds, Tran, Hai B, Jersmann, Hubertus, Truong, Tung Thanh, Hamon, Rhys, Roscioli, Eugene, Ween, Miranda, Pitman, Melissa R, Pitson, Stuart M, Hodge, Greg, Reynolds, Paul N, and Hodge, Sandra

Subjects

0301 basic medicine, Pulmonology, Immunofluorescence, lcsh:Medicine, Epithelium, White Blood Cells, Habits, Mice, Pulmonary Disease, Chronic Obstructive, Animal Cells, Sphingosine, Medicine and Health Sciences, Smoking Habits, Public and Occupational Health, Alveolar Macrophages, lcsh:Science, Cells, Cultured, Multidisciplinary, Chemistry, phagocytic capacity, 3. Good health, Cell biology, medicine.anatomical_structure, Cell Processes, Signal transduction, Cellular Types, Anatomy, Intracellular, Research Article, Signal Transduction, Subcellular Fractions, Substance-Related Disorders, Phagocytosis, Immune Cells, Chronic Obstructive Pulmonary Disease, Immunology, Anion Transport Proteins, Chronic obstructive pulmonary disease (COPD), Research and Analysis Methods, Cigarette Smoking, 03 medical and health sciences, Mental Health and Psychiatry, Macrophages, Alveolar, medicine, Extracellular, Animals, Humans, Immunoassays, Behavior, Lung, Blood Cells, Macrophages, lcsh:R, Biology and Life Sciences, Smoking Related Disorders, Epithelial Cells, Cell Biology, Disease Models, Animal, 030104 developmental biology, Biological Tissue, Cell culture, Case-Control Studies, Alveolar macrophage, Immunologic Techniques, lcsh:Q, Lysophospholipids, defective phagocytic function

Abstract

Introduction We have previously established a link between impaired phagocytic capacity and deregulated S1P signaling in alveolar macrophages from COPD subjects. We hypothesize that this defect may include a disruption of epithelial-macrophage crosstalk via Spns2-mediated intercellular S1P signaling. Methods Primary alveolar macrophages and bronchial epithelial cells from COPD subjects and controls, cell lines, and a mouse model of chronic cigarette smoke exposure were studied. Cells were exposed to 10% cigarette smoke extract, or vehicle control. Spns2 expression and subcellular localization was studied by immunofluorescence, confocal microscopy and RT-PCR. Phagocytosis was assessed by flow-cytometry. Levels of intra- and extracellular S1P were measured by S1P [3H]-labeling. Results Spns2 expression was significantly increased (p < 0.05) in alveolar macrophages from current-smokers/COPD patients (n = 5) compared to healthy nonsmokers (n = 8) and nonsmoker lung transplant patients (n = 4). Consistent with this finding, cigarette smoke induced a significant increase in Spns2 expression in both human alveolar and THP-1 macrophages. In contrast, a remarkable Spns2 down-regulation was noted in response to cigarette smoke in 16HBE14o- cell line (p < 0.001 in 3 experiments), primary nasal epithelial cells (p < 0.01 in 2 experiments), and in smoke-exposed mice (p < 0.001, n = 6 animals per group). Spns2 was localized to cilia in primary bronchial epithelial cells. In both macrophage and epithelial cell types, Spns2 was also found localized to cytoplasm and the nucleus, in line with a predicted bipartile Nuclear Localization Signal at the position aa282 of the human Spns2 sequence. In smoke-exposed mice, alveolar macrophage phagocytic function positively correlated with Spns2 protein expression in bronchial epithelial cells. Conclusion Our data suggest that the epithelium may be the major source for extracellular S1P in the airway and that there is a possible disruption of epithelial/macrophage cross talk via Spns2-mediated S1P signaling in COPD and in response to cigarette smoke exposure.

Published

2017

25. Identifying Natural Substrates for Dipeptidyl Peptidases 8 and 9 Using Terminal Amine Isotopic Labeling of Substrates (TAILS) Reveals in Vivo Roles in Cellular Homeostasis and Energy Metabolism*♦

Author

Kym McNicholas, Claire H. Wilson, Catherine A. Abbott, Lisa D. Pogson, R. Ian Menz, Alain Doucet, Christopher M. Overall, Dono Indarto, Melissa R. Pitman, Wilson, Claire H, Indarto, Dono, Doucet, Alain, Pogson, Lisa D, Pitman, Melissa R, McNicholas, Kym, Menz, R Ian, Overall, Christopher M, and Abbott, Catherine A

Subjects

Proteomics, Cytoplasm, Dipeptidases, Cellular homeostasis, Cell Separation, Biochemistry, DP9/DPP9, Mass Spectrometry, dipeptidyl peptidase, Substrate Specificity, calreticulin, Dipeptidyl Peptidase 9, cell metabolism, energy metabolism, Homeostasis, chemistry.chemical_classification, 0303 health sciences, aminopeptidase, 030302 biochemistry & molecular biology, Terminal amine isotopic labeling of substrates, Flow Cytometry, Cell biology, Enzymes, Isotope Labeling, DP8/DPP8, Aminopeptidase, enzymes, Dipeptidyl Peptidase, Molecular Sequence Data, Adenylate kinase, Biology, Dipeptidyl peptidase, adenylate kinase, 03 medical and health sciences, proteomics, In vivo, Cations, Cell Line, Tumor, Humans, Amino Acid Sequence, Dipeptidyl-Peptidases and Tripeptidyl-Peptidases, Molecular Biology, Dipeptidyl peptidase-4, 030304 developmental biology, Adenylate Kinase, Cell Biology, Cell Metabolism, Protein Structure, Tertiary, Enzyme, chemistry, Enzymology, Energy Metabolism, Calreticulin

Abstract

Background: Biological roles for intracellular dipeptidyl peptidases 8 and 9 are unknown. Results: By degradomics, 29 new in vivo substrates were identified (nine validated) for DP8/DP9, including adenylate kinase 2 and calreticulin. Conclusion: These substrates indicate roles for DP8 and DP9 in metabolism and energy homeostasis. Significance: Being the first proteomics screen for DP8/DP9 substrates, unexpected new cellular roles were revealed., Dipeptidyl peptidases (DP) 8 and 9 are homologous, cytoplasmic N-terminal post-proline-cleaving enzymes that are anti-targets for the development of DP4 (DPPIV/CD26) inhibitors for treating type II diabetes. To date, DP8 and DP9 have been implicated in immune responses and cancer biology, but their pathophysiological functions and substrate repertoire remain unknown. This study utilizes terminal amine isotopic labeling of substrates (TAILS), an N-terminal positional proteomic approach, for the discovery of in vivo DP8 and DP9 substrates. In vivo roles for DP8 and DP9 in cellular metabolism and homeostasis were revealed via the identification of more than 29 candidate natural substrates and pathways affected by DP8/DP9 overexpression. Cleavage of 14 substrates was investigated in vitro; 9/14 substrates for both DP8 and DP9 were confirmed by MALDI-TOF MS, including two of high confidence, calreticulin and adenylate kinase 2. Adenylate kinase 2 plays key roles in cellular energy and nucleotide homeostasis. These results demonstrate remarkable in vivo substrate overlap between DP8/DP9, suggesting compensatory roles for these enzymes. This work provides the first global investigation into DP8 and DP9 substrates, providing a number of leads for future investigations into the biological roles and significance of DP8 and DP9 in human health and disease.

Published

2013

26. Recent advances in the development of sphingosine kinase inhibitors

Author

Stuart M. Pitson, Melissa R. Pitman, Maurizio Costabile, Pitman, Melissa R, Costabile, Maurizio, and Pitson, Stuart Maxwell

Subjects

0301 basic medicine, Ceramide, sphingosine kinase 1, sphingosine kinase 2, Sphingosine kinase, 03 medical and health sciences, chemistry.chemical_compound, Animals, Humans, Sphingosine-1-phosphate, ceramide, Protein Kinase Inhibitors, Sphingosine, biology, sphingosine, Sphingosine Kinase 2, Cell Biology, Lipid signaling, Small molecule, Phosphotransferases (Alcohol Group Acceptor), 030104 developmental biology, chemistry, Sphingosine kinase 1, Biochemistry, Gene Knockdown Techniques, biology.protein, sphingosine-1-phosphate

Abstract

Sphingosine kinase (SK) 1 and 2 are lipid kinases that catalyse the formation of sphingosine 1-phosphate (S1P), a potent signalling molecule with a wide array of cellular effects. SK1 and 2 have been shown to be up-regulated in tumours and their genetic ablation or inhibition has been shown to slow tumour growth as well as sensitise cancer cells to chemotherapeutics. The SKs have been extensively studied, with a plethora of inhibitors developed that target the sphingosine-binding pocket of the enzyme, some with nanomolar affinities. Recently, inhibitors targeting the ATP pocket of SK have also been described. Here we discuss the development of these new small molecule SK inhibitors, summarise the recent discovery of off-targets effects of many current SK inhibitors, and provide an overview of the usefulness of these inhibitors as in vitro tools and therapeutic agents. Refereed/Peer-reviewed

Published

2016

27. An oncogenic role for sphingosine kinase 2

Author

Melissa R. Pitman, Claudine S. Bonder, Michael S. Samuel, Heidi A. Neubauer, Darren J. Creek, Paul A.B. Moretti, Briony L. Gliddon, Stuart M. Pitson, Jason A. Powell, Huasheng Chan, Tamara M. Leclercq, Julia R. Zebol, Duyen H. Pham, Amanda L. Peterson, Neubauer, Heidi A, Pham, Duyen H, Zebol, Julia R, Moretti, Paul AB, Peterson, Amanda L, Leclercq, Tamara M, Chan, Huasheng, Powell, Jason A, Pitman, Melissa R, Samuel, Michael S, Bonder, Claudine S, Creek, Darren J, Gliddon, Briony L, and Pitson, Stuart M

Subjects

0301 basic medicine, Ceramide, Carcinogenesis, Cell Survival, sphingosine kinase 2, proliferation, Apoptosis, Biology, Ceramides, medicine.disease_cause, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Sphingosine, oncogenesis, medicine, Humans, Neoplastic transformation, Cell Proliferation, Cell Nucleus, Kinase, Cell growth, Cell Membrane, Sphingosine Kinase 2, 3. Good health, Gene Expression Regulation, Neoplastic, Phosphotransferases (Alcohol Group Acceptor), Protein Transport, neoplastic transformation, tumorigenesis, HEK293 Cells, 030104 developmental biology, Oncology, chemistry, 030220 oncology & carcinogenesis, Cancer research, Lysophospholipids, Signal transduction, Research Paper

Abstract

// Heidi A. Neubauer 1,2 , Duyen H. Pham 1,2 , Julia R. Zebol 1 , Paul A.B. Moretti 1 , Amanda L. Peterson 4 , Tamara M. Leclercq 1 , Huasheng Chan 1,2 , Jason A. Powell 1,3 , Melissa R. Pitman 1 , Michael S. Samuel 1,3 , Claudine S. Bonder 1,2,3 , Darren J. Creek 4 , Briony L. Gliddon 1 and Stuart M. Pitson 1,2,3 1 Centre for Cancer Biology, University of South Australia and SA Pathology, Adelaide, South Australia, Australia 2 School of Biological Sciences, University of Adelaide, Adelaide, South Australia, Australia 3 School of Medicine, University of Adelaide, Adelaide, South Australia, Australia 4 Monash Institute of Pharmaceutical Science, Monash University, Parkville, Victoria, Australia Correspondence to: Stuart M. Pitson , email: // Keywords : sphingosine kinase 2, neoplastic transformation, oncogenesis, proliferation, tumorigenesis Received : June 08, 2016 Accepted : August 25, 2016 Published : August 30, 2016 Abstract While both human sphingosine kinases (SK1 and SK2) catalyze the generation of the pleiotropic signaling lipid sphingosine 1-phosphate, these enzymes appear to be functionally distinct. SK1 has well described roles in promoting cell survival, proliferation and neoplastic transformation. The roles of SK2, and its contribution to cancer, however, are much less clear. Some studies have suggested an anti-proliferative/pro-apoptotic function for SK2, while others indicate it has a pro-survival role and its inhibition can have anti-cancer effects. Our analysis of gene expression data revealed that SK2 is upregulated in many human cancers, but only to a small extent (up to 2.5-fold over normal tissue). Based on these findings, we examined the effect of different levels of cellular SK2 and showed that high-level overexpression reduced cell proliferation and survival, and increased cellular ceramide levels. In contrast, however, low-level SK2 overexpression promoted cell survival and proliferation, and induced neoplastic transformation in vivo . These findings coincided with decreased nuclear localization and increased plasma membrane localization of SK2, as well as increases in extracellular S1P formation. Hence, we have shown for the first time that SK2 can have a direct role in promoting oncogenesis, supporting the use of SK2-specific inhibitors as anti-cancer agents.

Published

2016

28. From sphingosine kinase to dihydroceramide desaturase: A structure-activity relationship (SAR) study of the enzyme inhibitory and anticancer activity of 4-((4-(4-Chlorophenyl)thiazol-2-yl)amino)phenol (SKI-II)

Author

Lorena T. Davies, Richard J. Rebello, Bernard L. Flynn, Darren J. Creek, Victoria L. Oliver, Anna E. Sexton, Luc Furic, Luigi Aurelio, Melissa R. Pitman, Stuart M. Pitson, Carmen V. Scullino, Aurelio, Luigi, Scullino, Carmen V, Pitman, Melissa R, Sexton, Anna, Oliver, Victoria, Davies, Lorena, Rebello, Richard J, Furic, Luc, Creek, Darren J, Pitson, Stuart M, and Flynn, Bernard L

Subjects

0301 basic medicine, enzyme inhibitory, Cell Survival, Sphingosine kinase, Antineoplastic Agents, Pharmacology, Structure-Activity Relationship, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, In vivo, Cell Line, Tumor, Drug Discovery, Humans, Structure–activity relationship, Inducer, Sphingosine-1-phosphate, sphingolipid metabolites, Enzyme Inhibitors, Cell Proliferation, Dose-Response Relationship, Drug, Molecular Structure, Cell growth, Dihydroceramide desaturase, In vitro, Phosphotransferases (Alcohol Group Acceptor), Thiazoles, 030104 developmental biology, anticancer activity, chemistry, Biochemistry, 030220 oncology & carcinogenesis, dihydroceramide desaturase, Molecular Medicine, Drug Screening Assays, Antitumor, Oxidoreductases

Abstract

The sphingosine kinase (SK) inhibitor, SKI-II, has been employed extensively in biological investigations of the role of SK1 and SK2 in disease and has demonstrated impressive anticancer activity in vitro and in vivo. However, interpretations of results using this pharmacological agent are complicated by several factors: poor SK1/2 selectivity, additional activity as an inducer of SK1-degradation, and off-target effects, including its recently identified capacity to inhibit dihydroceramide desaturase-1 (Des1). In this study, we have delineated the structure-activity relationship (SAR) for these different targets and correlated them to that required for anticancer activity and determined that Des1 inhibition is primarily responsible for the antiproliferative effects of SKI-II and its analogues. In the course of these efforts, a series of novel SK1, SK2, and Des1 inhibitors have been generated, including compounds with significantly greater anticancer activity. Refereed/Peer-reviewed

Published

2016

29. A critical role for the protein phosphatase 2A B′α regulatory subunit in dephosphorylation of sphingosine kinase 1

Author

Paul A.B. Moretti, Briony L. Gliddon, Melissa R. Pitman, Stuart M. Pitson, Angus M. Magarey, Renae K. Barr, Pitman, Melissa R, Barr, Renae K, Gliddon, Briony L, Magarey, Angus M, Moretti, Paul AB, and Pitson, Stuart M

Subjects

Protein subunit, B56α, Sphingosine kinase, Biochemistry, PR61α, Dephosphorylation, Mice, Animals, Humans, Immunoprecipitation, Neoplastic transformation, Protein Phosphatase 2, Phosphorylation, biology, Kinase, protein phosphatase 2A, Cell Membrane, B'α, Cell Biology, Protein phosphatase 2, Cell biology, Phosphotransferases (Alcohol Group Acceptor), Protein Transport, Cell Transformation, Neoplastic, HEK293 Cells, Sphingosine kinase 1, PPP2R5A, sphingosine kinase, Gene Knockdown Techniques, NIH 3T3 Cells, sphingosine-1-phosphate, biology.protein, Protein Binding

Abstract

Sphingosine kinase 1 (SK1) is an important regulator of cellular signalling that has gained recent attention as a potential target for anti-cancer therapies. SK1 activity, subcellular localization and oncogenic function are regulated by phosphorylation and dephosphorylation at Ser225. ERK1/2 have been identified as the protein kinases responsible for phosphorylation and activation of SK1. Conversely, dephosphorylation and deactivation of SK1 occurs by protein phosphatase 2A (PP2A). Active PP2A, however, is a heterotrimer, composed of tightly associated catalytic and structural subunits that can interact with an array of regulatory subunits, which are critical for determining holoenzyme substrate specificity and subcellular localization. Thus, PP2A represents a large family of holoenzyme complexes with different activities and diverse substrate specificities. To date the regulatory subunit essential for targeting PP2A to SK1 has remained undefined. Here, we demonstrate a critical role for the B'α (B56α/PR61α/PPP2R5A) regulatory subunit of PP2A in SK1 dephosphorylation. B'α was found to interact with the c-terminus of SK1, and reduce SK1 phosphorylation when overexpressed, while having no effect on upstream ERK1/2 activation. siRNA-mediated knockdown of B'α increased SK1 phosphorylation, activity and membrane localization of endogenous SK1. Furthermore, overexpression of B'α blocked agonist-induced translocation of SK1 to the plasma membrane and abrogated SK1-induced neoplastic transformation of NIH3T3 fibroblasts. Thus, the PP2A-B'α holoenzyme appears to function as an important endogenous regulator of SK1. Refereed/Peer-reviewed

Published

2011

30. Sphingolipid Targeting Agent MIPS247 Attenuates Collagen Synthesis by Cardiac and Kidney Cells via Stabilisation of PPM1A

Author

Ian Wang, Bernard L. Flynn, J. Lu, Stuart M. Pitson, Henry Krum, L. Huang, Yue Hua, Melissa R. Pitman, Bing Hui Wang, J. Liu, Luigi Aurelio, Carmen V. Scullino, and Darren J. Creek

Subjects

Pulmonary and Respiratory Medicine, Kidney, medicine.anatomical_structure, business.industry, Medicine, Anatomy, Cardiology and Cardiovascular Medicine, business, Sphingolipid, Cell biology

Published

2016

31. Isoform-selective assays for sphingosine kinase activity

Author

Melissa R, Pitman, Duyen H, Pham, and Stuart M, Pitson

Subjects

Isoenzymes, Phosphotransferases (Alcohol Group Acceptor), Sphingosine, Biocatalysis, Chromatography, Thin Layer, Chemical Fractionation, Lysophospholipids, Phosphorylation, Enzyme Assays

Abstract

Sphingosine kinases (SK) 1 and 2 are unique lipid kinases that phosphorylate sphingosine to form -sphingosine-1-phosphate (S1P). S1P is a bioactive molecule eliciting multiple effects both extracellularly via cell surface S1P receptors and intracellularly through a number of recently identified protein targets. The two enzymes arise from different genes, and differ in their cellular localisation, developmental expression, catalytic properties, and in at least some functional roles. Here, we describe methods for selectively detecting SK1 and SK2 activities in vitro, highlighting conditions that can discriminate between the activities of these two enzymes. The assays measure the production of (32)P-labelled S1P following the addition of exogenous sphingosine and [γ(32)P] adenosine-5'-triphosphate. The S1P product can be purified by Bligh-Dyer solvent extraction, separated by thin-layer chromatography (TLC), and the radiolabelled S1P quantified by exposing the TLC plate to a storage phosphor screen. This sensitive, reproducible assay can be used to selectively detect SK1 and SK2 activities in tissue, cell, and recombinant protein samples.

Published

2012

32. Isoform-Selective Assays for Sphingosine Kinase Activity

Author

Stuart M. Pitson, Duyen H. Pham, and Melissa R. Pitman

Subjects

chemistry.chemical_classification, chemistry.chemical_compound, Enzyme, Sphingosine, chemistry, Biochemistry, Kinase, Sphingosine kinase, Phosphorylation, lipids (amino acids, peptides, and proteins), Lipid signaling, Sphingosine-1-phosphate, Receptor

Abstract

Sphingosine kinases (SK) 1 and 2 are unique lipid kinases that phosphorylate sphingosine to form -sphingosine-1-phosphate (S1P). S1P is a bioactive molecule eliciting multiple effects both extracellularly via cell surface S1P receptors and intracellularly through a number of recently identified protein targets. The two enzymes arise from different genes, and differ in their cellular localisation, developmental expression, catalytic properties, and in at least some functional roles. Here, we describe methods for selectively detecting SK1 and SK2 activities in vitro, highlighting conditions that can discriminate between the activities of these two enzymes. The assays measure the production of (32)P-labelled S1P following the addition of exogenous sphingosine and [γ(32)P] adenosine-5'-triphosphate. The S1P product can be purified by Bligh-Dyer solvent extraction, separated by thin-layer chromatography (TLC), and the radiolabelled S1P quantified by exposing the TLC plate to a storage phosphor screen. This sensitive, reproducible assay can be used to selectively detect SK1 and SK2 activities in tissue, cell, and recombinant protein samples.

Published

2012

33. Hydrophilic residues surrounding the S1 and S2 pockets contribute to dimerisation and catalysis in human dipeptidyl peptidase 8 (DP8)

Author

Melissa R. Pitman, Catherine A. Abbott, and R. Ian Menz

Subjects

Dipeptidases, Dipeptidyl Peptidase 4, Dimer, Clinical Biochemistry, Biochemistry, Dipeptidyl peptidase, Substrate Specificity, chemistry.chemical_compound, Endopeptidase activity, Protein structure, Fibroblast activation protein, alpha, Catalytic Domain, Endopeptidases, Hydrolase, Humans, Protein Interaction Domains and Motifs, Databases, Protein, Dipeptidyl-Peptidases and Tripeptidyl-Peptidases, Protein Structure, Quaternary, education, Molecular Biology, education.field_of_study, Sequence Homology, Amino Acid, biology, Protein Stability, Chemistry, Serine Endopeptidases, Membrane Proteins, Active site, Hydrogen-Ion Concentration, Dipeptidyl peptidase 8, Recombinant Proteins, Kinetics, Gelatinases, Biocatalysis, Mutagenesis, Site-Directed, biology.protein, Mutant Proteins, Dimerization, Hydrophobic and Hydrophilic Interactions, Sequence Alignment

Abstract

Dipeptidyl peptidase (DP) 8 belongs to the dipeptidyl peptidase IV gene family. DP8 has been implicated in immune function and asthma, although its biological function is yet unknown. Structures of the homologs, fibroblast activation protein (FAP) and DPIV, are known but the DP8 structure is yet to be resolved. To help characterise the DP8 substrate pocket, mutants of residues lining the pocket were produced at DP8D772, DP8Y315, DP8H434 and DP8D435 and assessed by substrate kinetics and size-exclusion chromatography. Mutations of DP8D772A/E/S/V affected catalysis but did not confer endopeptidase activity. Mutations of DP8H434F, DP8D435F and DP8Y315F reduced catalytic activity. Furthermore, mutations to DP8D772A/E/S/V, DP8H434F, DP8D435F and DP8Y315F affected dimer stabilisation. Homology modelling of DP8 using DPIV and FAP crystal structures suggested that DP8D772, DP8H434 and DP8D435 were located at the edge of the S2 catalytic pocket, contributing to the junction between the alpha-beta hydrolase and beta-propeller domains. This study provides insights into how the DP8 substrate pocket and dimer interface differ from DPIV and FAP which could be utilised for designing more selective DP8 inhibitors.

Published

2010

34. Inhibitors of the sphingosine kinase pathway as potential therapeutics

Author

Melissa R. Pitman, Stuart M. Pitson, Pitman, Melissa, and Pitson, Stuart Maxwell

Subjects

Cancer Research, Sphingosine kinase, lipid kinase, Substrate Specificity, Enzyme activator, chemistry.chemical_compound, In vivo, Drug Discovery, medicine, Animals, Humans, Enzyme Inhibitors, sphingosine 1-phosphate, Pharmacology, Sphingosine, sphingosine, Cancer, Lipid signaling, medicine.disease, Small molecule, Enzyme Activation, inhibitor, Phosphotransferases (Alcohol Group Acceptor), Oncology, chemistry, sphingosine kinase, Cancer cell, Cancer research, Biocatalysis, cancer therapy

Abstract

Sphingosine kinase (SK) 1 and 2 are lipid kinases that phosphorylate sphingosine to form sphingosine-1 phosphate, a potent signalling molecule with pleiotrophic effects. SK1 is commonly up-regulated in tumours and its inhibition or genetic ablation has been shown to slow tumour growth as well as sensitise cancer cells to other chemotherapeutics. Therefore, SK1 is of particular interest as a target therapeutic intervention in cancer. Initial SK inhibitors were sphingosine derivatives and displayed efficacy in a number of disease models, establishing a premise for SK inhibition for anti-proliferative and anti-inflammatory therapies, even though these compounds had questionable specificity. More recently, a number of new SK inhibitors have been developed that display higher affinities and greater specificity for the SKs. Here we summarise the current small molecule inhibitors and related approaches for targeting the SKs, and their in vitro and in vivo efficacy. Furthermore, we highlight findings demonstrating the success of SK inhibition in cancer and a range of other disease models that promotes the continued interest in targeting the SKs for therapeutic benefit.

Published

2010

35. The In Vivo Expression of Dipeptidyl Peptidases 8 and 9

Author

Denise M. T. Yu, Geoffrey W. McCaughan, Joohong Park, Kathryn A. Evans, Margaret G. Gall, C. Soon Lee, Catherine A. Abbott, Eileen A. McLaughlin, Mark D. Gorrell, Katerina Ajami, and Melissa R. Pitman

Subjects

Central Nervous System, Male, medicine.medical_specialty, Histology, Adolescent, Dipeptidyl Peptidase 4, Spleen, Endocrine System, In situ hybridization, Biology, Dipeptidyl peptidase, Article, Epithelium, Gene Expression Regulation, Enzymologic, Gene Knockout Techniques, Mice, Dipeptidyl Peptidase 9, Immune system, Internal medicine, Testis, medicine, Animals, Humans, Protease Inhibitors, RNA, Messenger, Child, Dipeptidyl peptidase-4, In Situ Hybridization, Gastrointestinal tract, Dipeptidyl-Peptidase IV Inhibitors, Muscles, Reproduction, Molecular biology, medicine.anatomical_structure, Endocrinology, Ethylmaleimide, Immune System, Anatomy, Papio

Abstract

The dipeptidyl peptidase IV (DPIV) enzyme family contains both potential and proven therapeutic targets. Recent reports indicate the presence of DP8 and DP9 in peripheral blood lymphocytes, testis, lung, and brain. For a more comprehensive understanding of DP8 and DP9 tissue and cellular expression, mRNA and enzyme activity were examined. Many organs from C57BL/6 wild-type and DPIV gene-knockout mice were examined; DP8/9 enzyme activity was detected in the immune system, brain, testis, muscle, and epithelia. In situ hybridization localized DP8 and DP9 mRNA to lymphocytes and epithelial cells in liver, gastrointestinal tract, lymph node, spleen, and lung. DP8 and DP9 mRNA was detected in baboon and mouse testis, and DP9 expression was elevated in human testicular cancers. DP8 and DP9 mRNA were ubiquitous in day 17 mouse embryo, with greatest expression in epithelium (skin and gastrointestinal tract) and brain. Thus, DP8 and DP9 are widely expressed enzymes. Their expression in lymphocytes and epithelia indicates potential for roles in the digestive and immune systems. This manuscript contains online supplemental material at http://www.jhc.org. Please visit this article online to view these materials. (J Histochem Cytochem 57:1025–1040, 2009)

Published

2009

36. Prediction of Dipeptidyl Peptidase (DP) 8 Structure by Homology Modelling

Author

Catherine A. Abbott, R. Ian Menz, and Melissa R. Pitman

Subjects

chemistry.chemical_classification, biology, Chemistry, Active site, Combinatorial chemistry, Dipeptidyl peptidase, Endopeptidase, Enzyme, Fibroblast activation protein, alpha, Biochemistry, Docking (molecular), Catalytic triad, Hydrolase, biology.protein

Abstract

The DP8 model produced was very similar to the DPIV structure in the α/β hydrolase domain. Analysis of the active site of the DP8 model revealed significant structural conservation in the catalytic triad between DPIV, PEP and ACPH. Further analysis is required to determine whether any differences in the substrate pockets or substrate access tunnel(s) may contribute to DP8’s ability to act as a dipeptidyl peptidase, endopeptidase and acylaminoacyl peptidase. As the structure of fibroblast activation protein has recently been published, an alternative model may be made using this structure together with DPIV to make a model based on two enzymatically active proteins. Simulated docking of substrates and inhibitors into the model may uncover subtle differences between the structures. This may aid in determining the reason for DP8’s multiple enzyme functionality and aid in the improvement of DPIV inhibitor specificity.

Published

2006

37. Prediction of dipeptidyl peptidase (DP) 8 structure by homology modelling

Author

Melissa R, Pitman, R Ian, Menz, and Catherine A, Abbott

Subjects

Models, Molecular, Dipeptidases, Binding Sites, Potassium Channels, Sequence Homology, Amino Acid, Dipeptidyl Peptidase 4, Molecular Sequence Data, Serine Endopeptidases, Nerve Tissue Proteins, Protein Structure, Tertiary, Humans, Dipeptidyl-Peptidases and Tripeptidyl-Peptidases, Prolyl Oligopeptidases, Peptide Hydrolases

Published

2006

38. Methods for Protein Homology Modelling

Author

Melissa R. Pitman and R. Ian Menz

Subjects

Fungal protein, Protein function, Protein structure, Data sequences, Protein homology, Computational biology, Fungal gene, Biology, Bioinformatics

Abstract

Homology modelling has become a useful tool for the prediction of protein structure when only sequence data are available. Structural information is often more valuable than sequence alone for determining protein function. Homology modelling is potentially a very useful tool for the mycologist, as the number of fungal gene sequences available has exploded in recent years, whilst the number of experimentally determined fungal protein structures remains low. Programs available for homology modelling utilise different approaches and methods to produce the final model. Within each step of the homology modelling process, many factors affect the quality of the model produced, and appropriate selection of the program can significantly improve the quality of the model. This review discusses the advantages and limitations of the currently available methods and programs and provides a starting point for novices wishing to create a structural model. We have taken a practical approach as we hope to enable any scientist to utilise homology modelling as a tool for the analysis of their protein, or genome, of interest.

Published

2006

39. Contributors

Author

Catherine A. Abbott, David L. Baillie, Manoj Bhasin, Gregory Butler, Sangdun Choi, Jacques Cohen, Brian Fayz, Michelle Green, Igor V. Grigoriev, Tom Hsiang, Peter D. Karp, Dmytro Kevorkov, Stephen A. Krawetz, Markus Krummenacker, Pierre Legendre, Robert Lennie, Diego A. Martinez, Vladimir Makarenkov, R. Ian Menz, Audrius Meškauskas, Xiang Jia Min, Helena Nevalainen, Suzanne M. Paley, Shobha Ranganathan, Melissa R. Pitman, Adrian E. Platts, G.P.S. Raghava, Asaf A. Salamov, Leah A. Santat, Gautam B. Singh, Reginald Storms, Nicholas O'Toole, Brian Tjaden, Adrian Tsang, Anna Tsykin, Dawei Wang, Christopher R. Wilkinson, Claire H. Wilson, Sangdao Wongsai, Bin Yao, and Yeisoo Yu

Published

2006

40. Targeting sphingosine kinase as a therapy for acute myeloid leukaemia

Author

Carl Coolen, Ian D. Lewis, Stuart M. Pitson, Jason A. Powell, Wenying Zhu, Angel F. Lopez, Hayley S. Ramshaw, Daniel Thomas, Richard J D'Andrea, Melissa R. Pitman, 42nd Annual Scientific Meeting of the International-Society-for-Experimental-Hematology-and-Stem-Cells (ISEH) Vienna, Austria 22-25 August 2013, Powell, Jason, Pitman, Melissa, Coolen, Carl, Zhu, Wenying, Lewis, Ian, D'Andrea, Richard, Thomas, Daniel, Pitson, Stuart, Ramshaw, Hayley, and Lopez, Angel

Subjects

Cancer Research, business.industry, Genetics, Cancer research, Sphingosine kinase, Medicine, Cell Biology, Hematology, Myeloid leukaemia, business, Molecular Biology

Abstract

usc

Published

2013

41. Dipeptidyl peptidase 8 and 9 - guilty by association?

Author

Catherine A. Abbott, Melissa R. Pitman, Bryone J. Kuss, and Melanie Sulda

Subjects

education.field_of_study, business.industry, Multiple sclerosis, Arthritis, Cancer, Plasma protein binding, medicine.disease, Acquired immune system, Dipeptidyl peptidase 8, Inflammatory bowel disease, Rats, Substrate Specificity, Fibroblast activation protein, alpha, Immunology, Animals, Humans, Medicine, Protease Inhibitors, Dipeptidyl-Peptidases and Tripeptidyl-Peptidases, business, education, Protein Processing, Post-Translational, Protein Binding

Abstract

Dipeptidyl peptidases (DP) 8 and 9 are members of the DPIV enzyme family. Other members include DPIV, fibroblast activation protein (FAP) and the non-enzymes DP6 and DP10. DPIV family members have diverse biological roles, and have been implicated in a range of diseases including diabetes, cancer, inflammatory bowel disease, multiple sclerosis (MS), arthritis and asthma. While DP8/9 biological functions are yet to be established, they have been predicted to have similar roles to the other DPs due to high sequence similarities within the active site of the enzymes. While there is mounting evidence towards the involvement of DP8 and/or DP9 in innate and acquired immunity, direct proof for the link between DP8 and DP9 and human disease is yet to be definitively shown, thus DP8 and 9 proteins remain guilty by association.

Published

2009

42. Corrigendum to 'Stromal cell-derived factors 1α and 1β, inflammatory protein-10 and interferon-inducible T cell chemo-attractant are novel substrates of dipeptidyl peptidase 8' [FEBS Lett. 582 (2008) 819-825]

Author

Joohong Park, Amanda E. Starr, Christopher M. Overall, Mark D. Gorrell, Claire H. Wilson, Katerina Ajami, Jennifer H. Cox, Melissa R. Pitman, Catherine A. Abbott, and R. Ian Menz

Subjects

medicine.medical_specialty, education.field_of_study, Stromal cell, Chemistry, T cell, Biophysics, Cell Biology, Biochemistry, Dipeptidyl peptidase 8, Endocrinology, medicine.anatomical_structure, Structural Biology, Interferon, Internal medicine, Genetics, medicine, Cancer research, education, Molecular Biology, medicine.drug

Published

2008

43. Stromal cell-derived factors 1α and 1β, inflammatory protein-10 and interferon-inducible T cell chemo-attractant are novel substrates of dipeptidyl peptidase 8

Author

Joohong Park, Amanda E. Starr, Catherine A. Abbott, Mark D. Gorrell, Katerina Ajami, R. Ian Menz, Jennifer H. Cox, Melissa R. Pitman, Christopher M. Overall, and Claire H. Wilson

Subjects

Dipeptidases, Chemokine, Dipeptidyl Peptidase 4, Substrate specificity, Biophysics, Oligopeptidase, Biochemistry, Dipeptidyl peptidase, Dipeptidyl peptidase 8, 03 medical and health sciences, 0302 clinical medicine, Structural Biology, Genetics, Humans, CXCL10, CXCL11, CXC chemokine receptors, Receptor, education, Molecular Biology, 030304 developmental biology, 0303 health sciences, education.field_of_study, biology, Cell Biology, Chemokine CXCL12, Recombinant Proteins, Chemokine CXCL11, 3. Good health, Chemokine CXCL10, Molecular Weight, Kinetics, Solubility, Dipeptidyl peptidase IV, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, 030220 oncology & carcinogenesis, biology.protein, Protein Processing, Post-Translational, Half-Life

Abstract

N-terminal truncation of chemokines by proteases including dipeptidyl peptidase (DP) IV significantly alters their biological activity; generally ablating cognate G-protein coupled receptor engagement and often generating potent receptor antagonists. DP8 is a recently recognised member of the prolyl oligopeptidase gene family that includes DPIV. Since DPIV is known to process chemokines we surveyed 27 chemokines for cleavage by DP8. We report DP8 cleavage of the N-terminal two residues of IP10 (CXCL10), ITAC (CXCL11) and SDF-1 (CXCL12). This has implications for DP8 substrate specificity. Chemokine cleavage and inactivation may occur in vivo upon cell lysis and release of DP8 or in the inactivation of internalized chemokine/receptor complexes.

44. A selective ATP-competitive sphingosine kinase inhibitor demonstrates anti-cancer properties

Author

Anthony S. Don, Melissa R. Pitman, Briony L. Gliddon, Stuart M. Pitson, Claudine S. Bonder, Jason A. Powell, Duyen H. Pham, John W. Finnie, Carl Coolen, Lisa M. Ebert, Julia R. Zebol, Paul A.B. Moretti, Pitman, Melissa R, Powell, Jason A, Coolen, Carl, Moretti, Paul AB, Zebol, Julia R, Pham, Duyen H, Finnie, John W, Don, Anthony S, Ebert, Lisa M, Bonder, Claudine S, Gliddon, Briony L, and Pitson, Stuart M

Subjects

Male, Ceramide, Lung Neoplasms, Molecular Conformation, Sphingosine kinase, Apoptosis, Antineoplastic Agents, Mice, Transgenic, Adenocarcinoma, Biology, Cell fate determination, Cell Line, In silico docking, Mice, chemistry.chemical_compound, Adenosine Triphosphate, Cell Line, Tumor, Animals, Humans, Enzyme Inhibitors, Sphingolipids, Binding Sites, Neovascularization, Pathologic, Sphingosine, molecular modeling, Kinase, HEK 293 cells, apoptosis, small molecule inhibitor, Small Molecule Libraries, in silico docking, Sphingolipid, Cell biology, Phosphotransferases (Alcohol Group Acceptor), HEK293 Cells, Oncology, chemistry, Mutagenesis, sphingosine kinase, Mutation, MCF-7 Cells, Cancer research, Female, Neoplasm Transplantation, Research Paper, Protein Binding

Abstract

// Melissa R. Pitman 1 , Jason A. Powell 1, 3 , Carl Coolen 1 , Paul A.B. Moretti 1 , Julia R. Zebol 1 , Duyen H. Pham 1 , John W. Finnie 4, 5 , Anthony S. Don 6 , Lisa M. Ebert 1, 3 , Claudine S. Bonder 1, 2, 3 , Briony L. Gliddon 1 , Stuart M. Pitson 1, 2, 3, * 1 Centre for Cancer Biology, University of South Australia and SA Pathology, Adelaide, SA 5000, Australia 2 School of Molecular and Biomedical Science, University of Adelaide, SA 5005, Australia 3 School of Medicine, University of Adelaide, SA 5005, Australia 4 School of Veterinary Science, University of Adelaide, SA 5005, Australia 5 SA Pathology, Hanson Institute Centre for Neurological Diseases, Adelaide, SA 5000, Australia 6 Prince of Wales Clinical School, University of New South Wales, Sydney, NSW 2052, Australia Correspondence to: Stuart M. Pitson, e-mail: stuart.pitson@unisa.edu.au Keywords: Apoptosis, in silico docking, molecular modeling, small molecule inhibitor, sphingosine kinase Received: September 05, 2014 Accepted: January 25, 2015 Published: March 11, 2015 ABSTRACT The dynamic balance of cellular sphingolipids, the sphingolipid rheostat, is an important determinant of cell fate, and is commonly deregulated in cancer. Sphingosine 1-phosphate is a signaling molecule with anti-apoptotic, pro-proliferative and pro-angiogenic effects, while conversely, ceramide and sphingosine are pro-apoptotic. The sphingosine kinases (SKs) are key regulators of this sphingolipid rheostat, and are attractive targets for anti-cancer therapy. Here we report a first-in-class ATP-binding site-directed small molecule SK inhibitor, MP-A08, discovered using an approach of structural homology modelling of the ATP-binding site of SK1 and in silico docking with small molecule libraries. MP-A08 is a highly selective ATP competitive SK inhibitor that targets both SK1 and SK2. MP-A08 blocks pro-proliferative signalling pathways, induces mitochondrial-associated apoptosis in a SK-dependent manner, and reduces the growth of human lung adenocarcinoma tumours in a mouse xenograft model by both inducing tumour cell apoptosis and inhibiting tumour angiogenesis. Thus, this selective ATP competitive SK inhibitor provides a promising candidate for potential development as an anti-cancer therapy, and also, due to its different mode of inhibition to other known SK inhibitors, both validates the SKs as targets for anti-cancer therapy, and represents an important experimental tool to study these enzymes.