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

Author

Lewis, AC, Pope, VS, Tea, MN, Li, M, Nwosu, GO, Nguyen, TM, Wallington-Beddoe, CT, Moretti, PAB, Anderson, D, Creek, DJ, Costabile, M, Ali, SR, Thompson-Peach, CAL, Dredge, BK, Bert, AG, Goodall, GJ, Ekert, PG, Brown, AL, D'Andrea, R, Robinson, N, Pitman, MR, Thomas, D, Ross, DM, Gliddon, BL, Powell, JA, Pitson, SM, Lewis, AC, Pope, VS, Tea, MN, Li, M, Nwosu, GO, Nguyen, TM, Wallington-Beddoe, CT, Moretti, PAB, Anderson, D, Creek, DJ, Costabile, M, Ali, SR, Thompson-Peach, CAL, Dredge, BK, Bert, AG, Goodall, GJ, Ekert, PG, Brown, AL, D'Andrea, R, Robinson, N, Pitman, MR, Thomas, D, Ross, DM, Gliddon, BL, Powell, JA, and Pitson, SM

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

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

Author

Pitman, MR, Lewis, AC, Davies, LT, Moretti, PAB, Anderson, D, Creek, DJ, Powell, JA, Pitson, SM, Pitman, MR, Lewis, AC, Davies, LT, Moretti, PAB, Anderson, D, Creek, DJ, Powell, JA, and Pitson, SM

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

Bennett, MK, Li, M, Tea, MN, Pitman, MR, Toubia, J, Wang, PP-S, Anderson, D, Creek, DJ, Orlowski, RZ, Gliddon, BL, Powell, JA, Wallington-Beddoe, CT, Pitson, SM, Bennett, MK, Li, M, Tea, MN, Pitman, MR, Toubia, J, Wang, PP-S, Anderson, D, Creek, DJ, Orlowski, RZ, Gliddon, BL, Powell, JA, Wallington-Beddoe, CT, and Pitson, SM

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

4. SARS-CoV-2 Seroprevalence Survey Among District Residents Presenting for Serologic Testing at Three Community-Based Test Sites — Washington, DC, July–August, 2020

Author

Tran A, Nesbitt L, Leonard S, Powell Ja, Puckett M, McCarroll M, Johnson-Clarke F, Gunn Jkl, Ellison Ja, Sherman A, Yohannes A, Raj P, Jacqueline Reuben, David N, Iyengar P, Quasie-Woode Dp, Nielsen Cf, Lloyd P, Davies-Cole J, and J. K. Smith

Subjects
education.field_of_study, business.industry, Transmission (medicine), media_common.quotation_subject, Population, Ethnic group, Surveillance Methods, Asymptomatic, Serology, Hygiene, Medicine, Seroprevalence, medicine.symptom, business, education, Demography, media_common
Abstract

BackgroundThe District of Columbia (DC), a major metropolitan area, continues to see community transmission of SARS-CoV-2. While serologic testing does not indicate current SARS-CoV-2 infection, it can indicate prior infection and help inform local policy and health guidance. The DC Department of Health (DC Health) conducted a community-based survey to estimate DC’s SARS-CoV-2 seroprevalence and identify seropositivity-associated factors.MethodsA mixed-methods cross-sectional serology survey was conducted among a convenience sample of DC residents during July 27–August 21, 2020. Free serology testing was offered at three public test sites. Participants completed an electronic questionnaire on household and demographic characteristics, COVID-like illness (CLI) since January 1, 2020, comorbidities, and SARS-CoV-2 exposures. Univariate and bivariate analyses were conducted to describe the sample population and assess factors associated with seropositivity.ResultsAmong a sample of 671 participants, 51 individuals were seropositive, yielding an estimated seroprevalence of 7.6%. More than half (56.9%) of the seropositive participants reported no prior CLI; nearly half (47.1%) had no prior SARS-CoV-2 testing. Race/ethnicity, prior SARS-CoV-2 testing, prior CLI, employment status, and contact with confirmed COVID-19 cases were associated with seropositivity (PConclusionsThese findings indicate many seropositive individuals reported no symptoms consistent with CLI since January or any prior SARS-CoV-2 testing. This underscores the potential for cases to go undetected in the community and suggests wider-spread transmission than previously reported in DC.What is already known on this subject?Traditional case-based detection and syndromic surveillance efforts might not identify mildly symptomatic or asymptomatic SARS-CoV-2 infections. This is particularly true among people in the general population who do not have increased risk of severe illness or might not be tested otherwise. Consequently, the true population prevalence of prior SARS-CoV-2 infections might not be known.What this study adds?A community-based seroprevalence survey conducted in Washington, DC, during July 27–August 21, 2020 estimated that 7.6% of the convenience sample had antibodies to SARS-CoV-2, indicating prior infection. At the time of this survey, most of the participants reported that they had not been previously infected with or tested for SARS-CoV-2. These findings highlight both the value of serologic surveillance in complementing other surveillance methods, and the importance of continued prevention and mitigation measures, such as maintaining physical distances of at least 6 feet, avoiding crowds and poorly ventilated spaces, practicing frequent hand hygiene, and wearing face masks properly and consistently around people who do not live with you.

Published
2021

5. Clinical MDR1 inhibitors enhance Smac-mimetic bioavailability to kill murine LSCs and improve survival in AML models

Author

Morrish, E, Copeland, A, Moujalled, DM, Powell, JA, Silke, N, Lin, A, Jarman, KE, Sandow, JJ, Ebert, G, Mackiewicz, L, Beach, JA, Christie, EL, Lewis, AC, Pomilio, G, Fischer, KC, MacPherson, L, Bowtell, DDL, Webb, A, Pellegrini, M, Dawson, MA, Pitson, SM, Wei, AH, Silke, J, Brumatti, G, Morrish, E, Copeland, A, Moujalled, DM, Powell, JA, Silke, N, Lin, A, Jarman, KE, Sandow, JJ, Ebert, G, Mackiewicz, L, Beach, JA, Christie, EL, Lewis, AC, Pomilio, G, Fischer, KC, MacPherson, L, Bowtell, DDL, Webb, A, Pellegrini, M, Dawson, MA, Pitson, SM, Wei, AH, Silke, J, and Brumatti, G

Abstract

The specific targeting of inhibitor of apoptosis (IAP) proteins by Smac-mimetic (SM) drugs, such as birinapant, has been tested in clinical trials of acute myeloid leukemia (AML) and certain solid cancers. Despite their promising safety profile, SMs have had variable and limited success. Using a library of more than 5700 bioactive compounds, we screened for approaches that could sensitize AML cells to birinapant and identified multidrug resistance protein 1 inhibitors (MDR1i) as a class of clinically approved drugs that can enhance the efficacy of SM therapy. Genetic or pharmacological inhibition of MDR1 increased intracellular levels of birinapant and sensitized AML cells from leukemia murine models, human leukemia cell lines, and primary AML samples to killing by birinapant. The combination of clinical MDR1 and IAP inhibitors was well tolerated in vivo and more effective against leukemic cells, compared with normal hematopoietic progenitors. Importantly, birinapant combined with third-generation MDR1i effectively killed murine leukemic stem cells (LSCs) and prolonged survival of AML-burdened mice, suggesting a therapeutic opportunity for AML. This study identified a drug combination strategy that, by efficiently killing LSCs, may have the potential to improve outcomes in patients with AML.

Published
2020

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

Author

Zhu, W, Gliddon, BL, Jarman, KE, Moretti, PAB, Tin, T, Parise, LV, Woodcock, JM, Powell, JA, Ruszkiewicz, A, Pitman, MR, Pitson, SM, Zhu, W, Gliddon, BL, Jarman, KE, Moretti, PAB, Tin, T, Parise, LV, Woodcock, JM, Powell, JA, Ruszkiewicz, A, Pitman, MR, and Pitson, SM

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.

Published
2017

7. Activation of protein phosphatase 2A in FLT3+ acute myeloid leukemia cells enhances the cytotoxicity of FLT3 tyrosine kinase inhibitors

Author

Smith, AM, Dun, MD, Lee, EM, Harrison, C, Kahl, R, Flanagan, H, Panicker, N, Mashkani, B, Don, AS, Morris, J, Toop, H, Lock, RB, Powell, JA, Thomas, D, Guthridge, MA, Moore, A, Ashman, LK, Skelding, KA, Enjeti, A, Verrills, NM, Smith, AM, Dun, MD, Lee, EM, Harrison, C, Kahl, R, Flanagan, H, Panicker, N, Mashkani, B, Don, AS, Morris, J, Toop, H, Lock, RB, Powell, JA, Thomas, D, Guthridge, MA, Moore, A, Ashman, LK, Skelding, KA, Enjeti, A, and Verrills, NM

Abstract

Constitutive activation of the receptor tyrosine kinase Fms-like tyrosine kinase 3 (FLT3), via co-expression of its ligand or by genetic mutation, is common in acute myeloid leukemia (AML). In this study we show that FLT3 activation inhibits the activity of the tumor suppressor, protein phosphatase 2A (PP2A). Using BaF3 cells transduced with wildtype or mutant FLT3, we show that FLT3-induced PP2A inhibition sensitizes cells to the pharmacological PP2A activators, FTY720 and AAL(S). FTY720 and AAL(S) induced cell death and inhibited colony formation of FLT3 activated cells. Furthermore, PP2A activators reduced the phosphorylation of ERK and AKT, downstream targets shared by both FLT3 and PP2A, in FLT3/ITD+ BaF3 and MV4-11 cell lines. PP2A activity was lower in primary human bone marrow derived AML blasts compared to normal bone marrow, with blasts from FLT3-ITD patients displaying lower PP2A activity than WT-FLT3 blasts. Reduced PP2A activity was associated with hyperphosphorylation of the PP2A catalytic subunit, and reduced expression of PP2A structural and regulatory subunits. AML patient blasts were also sensitive to cell death induced by FTY720 and AAL(S), but these compounds had minimal effect on normal CD34+ bone marrow derived monocytes. Finally, PP2A activating compounds displayed synergistic effects when used in combination with tyrosine kinase inhibitors in FLT3-ITD+ cells. A combination of Sorafenib and FTY720 was also synergistic in the presence of a protective stromal microenvironment. Thus combining a PP2A activating compound and a FLT3 inhibitor may be a novel therapeutic approach for treating AML.

Published
2016

8. Efficacy of an Fc-modified anti-CD123 antibody (CSL362) combined with chemotherapy in xenograft models of acute myelogenous leukemia in immunodeficient mice

Author

Lee, EM, Yee, D, Busfield, SJ, McManus, JF, Cummings, N, Vairo, G, We, A, Ramshaw, HS, Powell, JA, Lopez, AF, Lewis, ID, McCall, MN, Lock, RB, Lee, EM, Yee, D, Busfield, SJ, McManus, JF, Cummings, N, Vairo, G, We, A, Ramshaw, HS, Powell, JA, Lopez, AF, Lewis, ID, McCall, MN, and Lock, RB

Abstract

The prognosis of older patients with acute myelogenous leukemia is generally poor. The interleukin-3 receptor α- chain (CD123) is highly expressed on the surface of acute leukemia cells compared with normal hematopoietic stem cells. CSL362 is a fully humanized, CD123-neutralizing monoclonal antibody containing a modified Fc structure, which enhances human natural killer cell antibody-dependent cell-mediated cytotoxicity. Six continuous acute myelogenous leukemia xenografts established from patient explants and characterized by cell and molecular criteria, produced progressively lethal disease 42-202 days after transplantation. CSL362 alone reduced engraftment of one of four and three of four acute myelogenous leukemia xenografts in the bone marrow and peripheral organs, respectively. A cytarabine and daunorubicin regimen was optimized using this model to identify potentially synergistic interactions with CSL362. Cytarabine/daunorubicin improved the survival of mice engrafted with four of four acute myelogenous leukemia xenografts by 31-41 days. Moreover, CSL362 extended the survival of cytarabine/daunorubicin-treated mice for two of two acute myelogenous leukemia xenografts, while augmentation of natural killer cell-deficient NSG mice with adoptively transferred human natural killer cells improved survival against a single xenograft. Interestingly, this enhanced CSL362 efficacy was lost in the absence of chemotherapy. This study shows that acute myelogenous leukemia xenografts provide a platform for the evaluation of new therapeutics, simulating complex in vivo interactions, and that the in vivo efficacy of CSL362 supports continued clinical development of this drug.

Published
2015

12. Utilization of Combat Stress Control Detachments

Author

Hagar Mj, Berigan Tr, Deagle Ea rd, and Powell Ja

Subjects
Risk analysis (engineering), Combat stress reaction, Public Health, Environmental and Occupational Health, General Medicine, Control (linguistics), Psychology
Published
1998

15. Frontmatter

Author

Powell, James S.

Published
2010

18. Index

Author

Powell, James S.

Published
2010

21. Notes

Author

Powell, James S.

Published
2010

22. Cover

Author

Powell, James S.

Published
2010

29. Preface

Author

Powell, James S.

Published
2010

31. Oviposition Patterns and Egg Characteristics of Australian Tortricine Moths (Lepidoptera: Tortricidae).

Author

Powell, JA and Common, IFB

Abstract

Oviposition patterns and egg characteristics are recorded for representatives of five of six tribes that comprise the Tortricinae in Australia. Included are 57 species in 32 genera: Phricanthini (one sp.) deposit globose eggs singly or in non-overlapping rows; Schoenotenini (three spp., three genera) lay flat, circular eggs singly or in rows of two or three; 'Cnephasiini' (three spp., two genera) deploy strongly convex eggs singly; Epitymbiini (30 spp.. 16 genera) deposit flat eggs usually in weakly overlapped, small circular patches of5-15 eggs; Archipini (20 spp., 10 genera) typically oviposit in regularly imbricate rows in a large, oval mass, followed by several smaller ones. Two Australian Archipini are aberrant, laying eggs singly or in pairs. Four different kinds of morphological and correlated behavioural modifications are employed to ornament eggs with 'corethrogyne' scales, either from the female's abdomen (two genera of Epitymbiini and one of Archipini) or hindwings (analogous development in one species of Epitymbiini and one genus of Archipini).

Published
1985
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39. A CASE OF POST-PARTUM ANAEMIA

Author

Davey Jb and Powell Ja

Subjects
Pregnancy, medicine.medical_specialty, Blood transfusion, business.industry, Obstetrics, medicine.medical_treatment, General Engineering, General Medicine, Articles, medicine.disease, Bioinformatics, General Earth and Planetary Sciences, Medicine, business, General Environmental Science, Post partum
Published
1928

44. Property management for company commanders

Author

Powell, Jaren P., Capt

Subjects
PROPERTY, REAL, ARMY POSTS - United States - Maintenance and Repair, BASE OPERATIONS, INVENTORIES
Abstract

illus

Published
2006

48. Mountain man

Author

Powell, Jack William

Published
2011

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