Your search keyword '"Hunt, P"' showing total 255 results

1. Natural history of PF4 antibodies in vaccine-induced immune thrombocytopenia and thrombosis

Author

Craven, Brian, Lester, William, Boyce, Sara, Thomas, Will, Kanny, Angela, Davies, Claire, Pavord, Sue, Hermans, Joannes, Makris, Michael, Bart-Smith, Emily, Arnott, Sarah, Hunt, Beverley J., Chudakou, Pavel, Calvert, Anthony, Singh, Deepak, and Scully, Marie

Abstract

The COVID-19 pandemic has resulted in the rapid development of a range of vaccines against SARS-CoV-2. Vaccine-induced immune thrombocytopenia and thrombosis (VITT) is a rare but life-threatening complication of primarily adenoviral-based vaccines associated with the presence of antibodies to a PF4/polyanion neoepitope and measured by using enzyme-linked immunosorbent assays. Presented are serial anti–PF4/polyanion antibody, platelet, and D-dimer measurements in a large cohort of patients and their relation to relapse. Overall, 51% of patients using the Stago assay had persistently positive anti–PF4/polyanion levels 100 days' postdiagnosis, whereas 94% of patients monitored by using the Immucor assay remain positive. The median duration of positivity of the PF4 assay is 87 days, with 72% of patients remaining positive after a median follow-up of 105 days. The use of plasma exchange seemed to reduce anti–PF4/polyanion levels and increase platelet counts in the acute setting more rapidly than other therapies. The rate of relapse in this study was 12.6%, with all relapsed cases exhibiting persistently positive PF4 antibodies and falling platelet counts. Only one patient had extension of their thrombosis. Overall, despite the persistence of PF4 antibodies in 72% of patients, the rate of relapse was low and did not seem to result in recrudescence of the aggressive clinical picture seen at index presentation. Monitoring of these patients in the UK cohort is ongoing and will aid in definition of the natural history of this novel condition.

Published

2022

2. Targeting intracellular WT1 in AML with a novel RMF-peptide-MHC-specific T-cell bispecific antibody

Author

Augsberger, Christian, Hänel, Gerulf, Xu, Wei, Pulko, Vesna, Hanisch, Lydia Jasmin, Augustin, Angelique, Challier, John, Hunt, Katharina, Vick, Binje, Rovatti, Pier Eduardo, Krupka, Christina, Rothe, Maurine, Schönle, Anne, Sam, Johannes, Lezan, Emmanuelle, Ducret, Axel, Ortiz-Franyuti, Daniela, Walz, Antje-Christine, Benz, Jörg, Bujotzek, Alexander, Lichtenegger, Felix S., Gassner, Christian, Carpy, Alejandro, Lyamichev, Victor, Patel, Jigar, Konstandin, Nikola, Tunger, Antje, Schmitz, Marc, von Bergwelt-Baildon, Michael, Spiekermann, Karsten, Vago, Luca, Jeremias, Irmela, Marrer-Berger, Estelle, Umaña, Pablo, Klein, Christian, and Subklewe, Marion

Abstract

Antibody-based immunotherapy is a promising strategy for targeting chemoresistant leukemic cells. However, classical antibody-based approaches are restricted to targeting lineage-specific cell surface antigens. By targeting intracellular antigens, a large number of other leukemia-associated targets would become accessible. In this study, we evaluated a novel T-cell bispecific (TCB) antibody, generated by using CrossMAb and knob-into-holes technology, containing a bivalent T-cell receptor–like binding domain that recognizes the RMFPNAPYL peptide derived from the intracellular tumor antigen Wilms tumor protein (WT1) in the context of HLA-A*02. Binding to CD3ε recruits T cells irrespective of their T-cell receptor specificity. WT1-TCB elicited antibody-mediated T-cell cytotoxicity against AML cell lines in a WT1- and HLA-restricted manner. Specific lysis of primary acute myeloid leukemia (AML) cells was mediated in ex vivo long-term cocultures by using allogeneic (mean ± standard error of the mean [SEM] specific lysis, 67 ± 6% after 13-14 days; n = 18) or autologous, patient-derived T cells (mean ± SEM specific lysis, 54 ± 12% after 11-14 days; n = 8). WT1-TCB–treated T cells exhibited higher cytotoxicity against primary AML cells than an HLA-A*02 RMF-specific T-cell clone. Combining WT1-TCB with the immunomodulatory drug lenalidomide further enhanced antibody-mediated T-cell cytotoxicity against primary AML cells (mean ± SEM specific lysis on days 3-4, 45.4 ± 9.0% vs 70.8 ± 8.3%; P = .015; n = 9-10). In vivo, WT1-TCB–treated humanized mice bearing SKM-1 tumors exhibited a significant and dose-dependent reduction in tumor growth. In summary, we show that WT1-TCB facilitates potent in vitro, ex vivo, and in vivo killing of AML cell lines and primary AML cells; these results led to the initiation of a phase 1 trial in patients with relapsed/refractory AML (#NCT04580121).

Published

2021

3. Clinical Outcomes of Patients with Breast Implant- Associated Anaplastic Large- Cell Lymphoma (BIA-ALCL) Treated with Chemotherapy and Brentuximab Vedotin

Author

Elias, Alexandra, Prakash, Rishab, Nastoupil, Loretta J., Fowler, Nathan H., Ahmed, Sairah, Nair, Ranjit, Malpica Castillo, Luis Enrique, Dabaja, Bouthaina S., Xu, Jie, Medeiros, Jeffrey, Stewart, John, Wang, Wei, Pinnix, Chelsea C., Hunt, Kelly, Clemens, Mark W, Miranda, Roberto N., and Iyer, Swaminathan P.

Published

2022

4. Glucocorticoid-induced eosinopenia results from CXCR4-dependent bone marrow migration

Author

Hong, So Gun, Sato, Noriko, Legrand, Fanny, Gadkari, Manasi, Makiya, Michelle, Stokes, Kindra, Howe, Katherine N., Yu, Shiqin Judy, Linde, Nathaniel Seth, Clevenger, Randall R., Hunt, Timothy, Hu, Zonghui, Choyke, Peter L., Dunbar, Cynthia E., Klion, Amy D., and Franco, Luis M.

Abstract

Glucocorticoids are considered first-line therapy in a variety of eosinophilic disorders. They lead to a transient, profound decrease in circulating human eosinophils within hours of administration. The phenomenon of glucocorticoid-induced eosinopenia has been the basis for the use of glucocorticoids in eosinophilic disorders, and it has intrigued clinicians for 7 decades, yet its mechanism remains unexplained. To investigate, we first studied the response of circulating eosinophils to in vivo glucocorticoid administration in 3 species and found that the response in rhesus macaques, but not in mice, closely resembled that in humans. We then developed an isolation technique to purify rhesus macaque eosinophils from peripheral blood and performed live tracking of zirconium-89-oxine–labeled eosinophils by serial positron emission tomography/computed tomography imaging, before and after administration of glucocorticoids. Glucocorticoids induced rapid bone marrow homing of eosinophils. The kinetics of glucocorticoid-induced eosinopenia and bone marrow migration were consistent with those of the induction of the glucocorticoid-responsive chemokine receptor CXCR4, and selective blockade of CXCR4 reduced or eliminated the early glucocorticoid-induced reduction in blood eosinophils. Our results indicate that glucocorticoid-induced eosinopenia results from CXCR4-dependent migration of eosinophils to the bone marrow. These findings provide insight into the mechanism of action of glucocorticoids in eosinophilic disorders, with implications for the study of glucocorticoid resistance and the development of more targeted therapies. The human study was registered at ClinicalTrials.gov as #NCT02798523.

Published

2020

5. LGR6frameshift variant abrogates receptor expression on select leukocyte subsets and associates with viral infections

Author

Gomez, Esteban A., De Matteis, Roberta, Udomjarumanee, Palita, Akhtar, Shaheen, Anwar, Mohammad, Arciero, Elena, Asgar, Omar, Ashraf, Samina, Bidi, Saeed, Breen, Gerome, Broster, James, Chung, Raymond, Collier, David, Curtis, Charles J, Chaudhary, Shabana, Clinch, Megan, Colligan, Grainne, Deloukas, Panos, Durham, Ceri, Durrani, Faiza, Eto, Fabiola, Finer, Sarah, Gafton, Joseph, Angel, Ana, Griffiths, Chris, Harvey, Joanne, Heng, Teng, Hodgson, Sam, Huang, Qin Qin, Hurles, Matt, Hunt, Karen A, Hussain, Shapna, Islam, Kamrul, Iyer, Vivek, Jacobs, Benjamin M, Khan, Ahsan, Langenberg, Claudia, Lavery, Cath, Lee, Sang Hyuck, MacArthur, Daniel, Malik, Sidra, Malawsky, Daniel, Martin, Hilary, Mason, Dan, Mathur, Rohini, Mazid, Mohammed Bodrul, McDermott, John, Morton, Caroline, Newman, Bill, Owor, Elizabeth, Qureshi, Asma, Ramachandrappa, Shwetha, Raza, Mehru, Russell, Jessry, Safa, Nishat, Samuel, Miriam, Simpson, Michael, Solly, John, Daniel Stow, Marie Spreckley., Taylor, Michael, Trembath, Richard C, Tricker, Karen, van Heel, David A, Walter, Klaudia, Winckley, Caroline, Wood, Suzanne, Wright, John, Zengeya, Ishevanhu, Zöllner, Julia, Munroe, Patricia B., and Dalli, Jesmond

Abstract

•rs74355478 is linked with the ablation of LGR6 expression on neutrophils, monocytes and NK cells and loss of MaR1 activity on phagocytes•rs74355478 leads to altered immune responses to viruses and associates with increased incidence of viral infections at the population level

Published

2024

6. Reversing anti–factor Xa agents and the unmet needs in trauma patients

Author

Hunt, Beverley J., Neal, Matthew D., and Stensballe, Jakob

Abstract

Andexanet alfa, a reversing agent for anticoagulants that inhibit factor Xa, has recently been licensed in the United States. We discuss the impact of this licensure on current practice and review in detail the problems of a neglected and growing clinical area: reversing the anticoagulation effect of factor Xa inhibitors in bleeding trauma patients. We identify areas of practice that need research so that care of bleeding trauma patients receiving direct factor Xa inhibitors can be improved.

Published

2018

7. Observational Cohort Study of People Living with HIV (PWH) Treated with CD19-Directed CAR T Cell Therapy for B-Cell Lymphoid Malignancies - Interim Results of AIDS Malignancy Consortium (AMC) Study AMC-113

Author

Barta, Stefan K., Noy, Ariela, Pasquini, Marcelo C, He, Naya, Hunt, Tiffany, Litovich, Carlos, Ibrahim, Uroosa, Baiocchi, Robert A., and Ambinder, Richard F.

Published

2022

8. Real World Outcomes of Therapeutic Anticoagulation Use in Moderate COVID-19 Infection in Hospitalised Patients

Author

Creeper, Katherine J., White, Katie, Breen, Karen, and Hunt, Beverley J.

Published

2022

9. Pharmacotypes across the Genomic Landscape of Pediatric Acute Lymphoblastic Leukemia and Impact on Treatment Response

Author

Lee, Shawn, Yang, Wenjian, Gocho, Yoshihiro, John, August, Rowland, Lauren, Smart, Brandon, Williams, Hannah, Maxwell, Dylan, Hunt, Jeremy, Yang, Wentao, Crews, Kristine R., Roberts, Kathryn G, Jeha, Sima, Cheng, Cheng, Karol, Seth E., Relling, Mary V., Rosner, Gary, Inaba, Hiroto, Mullighan, Charles G., Pui, Ching-Hon, Evans, William E., and Yang, Jun J.

Published

2022

10. Real-World Outcomes with CD19 CAR T-Cell Therapy for B-Cell Malignancies in Regional/Rural Australia: Results from the Queensland CAR T-Cell Program

Author

Perera, Nilu, Scott, Ashleigh P, Hunt, Stewart, Curley, Cameron, Tey, Siok-Keen, Butler, Jason, Henden, Andrea S, Pillai, Elango S., Hutchins, Cheryl, Mudie, Kari Louise, and Kennedy, Glen A

Published

2022

11. Hematopoietic origin of Langerhans cell histiocytosis and Erdheim-Chester disease in adults

Author

Milne, Paul, Bigley, Venetia, Bacon, Chris M., Néel, Antoine, McGovern, Naomi, Bomken, Simon, Haniffa, Muzlifah, Diamond, Eli L., Durham, Benjamin H., Visser, Johannes, Hunt, David, Gunawardena, Harsha, Macheta, Mac, McClain, Kenneth L., Allen, Carl, Abdel-Wahab, Omar, and Collin, Matthew

Abstract

Langerhans cell histiocytosis (LCH) and Erdheim-Chester disease (ECD) are rare histiocytic disorders induced by somatic mutation of MAPK pathway genes. BRAFV600Emutation is the most common mutation in both conditions and also occurs in the hematopoietic neoplasm hairy cell leukemia (HCL). It is not known if adult LCH or ECD arises from hematopoietic stem cells (HSCs), nor which potential blood borne precursors lead to the formation of histiocytic lesions. In this study, BRAFV600Eallele–specific polymerase chain reaction was used to map the neoplastic clone in 20 adults with LCH, ECD, and HCL. BRAFV600Ewas tracked to classical monocytes, nonclassical monocytes, and CD1c+myeloid dendritic cells (DCs) in the blood, and mutations were observed in HSCs and myeloid progenitors in the bone marrow of 4 patients. The pattern of involvement of peripheral blood myeloid cells was indistinguishable between LCH and ECD, although the histiocytic disorders were distinct to HCL. As reported in children, detection of BRAFV600Ein peripheral blood of adults was a marker of active multisystem LCH. The healthy counterparts of myeloid cells affected by BRAFmutation had a range of differentiation potentials depending on exogenous signals. CD1c+DCs acquired high langerin and CD1a with granulocyte-macrophage colony-stimulating factor and transforming growth factor β alone, whereas CD14+classical monocytes required additional notch ligation. Both classical and nonclassical monocytes, but not CD1c+DCs, made foamy macrophages easily in vitro with macrophage colony-stimulating factor and human serum. These studies are consistent with a hematopoietic origin and >1 immediate cellular precursor in both LCH and ECD.

Published

2017

12. A mechanistic investigation of thrombotic microangiopathy associated with IV abuse of Opana ER

Author

Hunt, Ryan, Yalamanoglu, Ayla, Tumlin, James, Schiller, Tal, Baek, Jin Hyen, Wu, Andrew, Fogo, Agnes B., Yang, Haichun, Wong, Edward, Miller, Peter, Buehler, Paul W., and Kimchi-Sarfaty, Chava

Abstract

Since 2012, a number of case reports have described the occurrence of thrombotic microangiopathy (TMA) following IV abuse of extended-release oxymorphone hydrochloride (Opana ER), an oral opioid for long-term treatment of chronic pain. Here, we present unique clinical features of 3 patients and investigate IV exposure to the tablet's inert ingredients as a possible causal mechanism. Guinea pigs were used as an animal model to understand the hematopathologic and nephrotoxic potential of the inert ingredient mixture (termed here as PEO+) which primarily contains high-molecular-weight polyethylene oxide (HMW PEO). Microangiopathic hemolytic anemia, thrombocytopenia, and acute kidney injury were found in a group of 3 patients following recent injection of adulterated extended-release oxymorphone tablets. Varying degrees of cardiac involvement and retinal ischemia occurred, with TMA evident on kidney biopsy. A TMA-like state also developed in guinea pigs IV administered PEO+. Acute tubular and glomerular renal injury was accompanied by nonheme iron deposition and hypoxia-inducible factor-1α upregulation in the renal cortex. Similar outcomes were observed following dosing with HMW PEO alone. IV exposure to the inert ingredients in reformulated extended-release oxymorphone can elicit TMA. Although prescription opioid abuse shows geographic variation, all physicians should be highly inquisitive of IV drug abuse when presented with cases of TMA.

Published

2017

13. Type I interferon causes thrombotic microangiopathy by a dose-dependent toxic effect on the microvasculature

Author

Kavanagh, David, McGlasson, Sarah, Jury, Alexa, Williams, Jac, Scolding, Neil, Bellamy, Chris, Gunther, Claudia, Ritchie, Diane, Gale, Daniel P., Kanwar, Yashpal S., Challis, Rachel, Buist, Holly, Overell, James, Weller, Belinda, Flossmann, Oliver, Blunden, Mark, Meyer, Eric P., Krucker, Thomas, Evans, Stephen J. W., Campbell, Iain L., Jackson, Andrew P., Chandran, Siddharthan, and Hunt, David P. J.

Abstract

Many drugs have been reported to cause thrombotic microangiopathy (TMA), yet evidence supporting a direct association is often weak. In particular, TMA has been reported in association with recombinant type I interferon (IFN) therapies, with recent concern regarding the use of IFN in multiple sclerosis patients. However, a causal association has yet to be demonstrated. Here, we adopt a combined clinical and experimental approach to provide evidence of such an association between type I IFN and TMA. We show that the clinical phenotype of cases referred to a national center is uniformly consistent with a direct dose-dependent drug-induced TMA. We then show that dose-dependent microvascular disease is seen in a transgenic mouse model of IFN toxicity. This includes specific microvascular pathological changes seen in patient biopsies and is dependent on transcriptional activation of the IFN response through the type I interferon α/β receptor (IFNAR). Together our clinical and experimental findings provide evidence of a causal link between type I IFN and TMA. As such, recombinant type I IFN therapies should be stopped at the earliest stage in patients who develop this complication, with implications for risk mitigation.

Published

2016

14. How I approach the prevention and treatment of thrombotic complications in hospitalized patients

Author

Akpan, Imo J. and Hunt, Beverley J.

Abstract

[Display omitted]

Published

2023

15. The influence of immunodeficiency, disease features, and patient characteristics on survival in plasmablastic lymphoma

Author

Di Ciaccio, Pietro R., Polizzotto, Mark N., Cwynarski, Kate, Gerrie, Alina S., Burton, Catherine, Bower, Mark, Kuruvilla, John, Montoto, Silvia, McKay, Pam, Fox, Christopher P., Milliken, Samuel, Jiamsakul, Awachana, Osborne, Wendy, Collins, Graham P., Manos, Kate, Linton, Kim M., Iyengar, Sunil, Kassam, Shireen, Limei, Michelle Poon, Kliman, David, Wong Doo, Nicole, Watson, Anne-Marie, Fedele, Pasquale, Yannakou, Costas K., Hunt, Stewart, Ku, Matthew, Sehn, Laurie H., Smith, Alexandra, Renshaw, Hanna, Maxwell, Alice, Liu, Qin, Dhairyawan, Rageshri, Ferguson, Graeme, Pickard, Keir, Painter, Daniel, Thakrar, Nisha, Song, Kevin W., and Hamad, Nada

Abstract

•PBL is a rare non-Hodgkin lymphoma with a poor prognosis and uncertainty regarding optimal treatment approaches.•Advanced stage, bone marrow involvement, ECOG > 1, and EBV–negative lymphoma are associated with inferior OS.

Published

2023

16. Bone-derived C-terminal FGF23 cleaved peptides increase iron availability in acute inflammation

Author

Courbon, Guillaume, Thomas, Jane Joy, Martinez-Calle, Marta, Wang, Xueyan, Spindler, Jadeah, Von Drasek, John, Hunt-Tobey, Bridget, Mehta, Rupal, Isakova, Tamara, Chang, Wenhan, Creemers, John W. M., Ji, Peng, Martin, Aline, and David, Valentin

Abstract

•Osteocytes are the main source of Cter-FGF23 peptides in acute inflammation.•Bone-derived Cter-FGF23 peptides are iron conserving molecules and antagonize BMP-induced hepcidin production.

Published

2023

17. Systems analysis uncovers inflammatory Th/Tc17-driven modules during acute GVHD in monkey and human T cells

Author

Furlan, Scott N., Watkins, Benjamin, Tkachev, Victor, Cooley, Sarah, Panoskaltsis-Mortari, Angela, Betz, Kayla, Brown, Melanie, Hunt, Daniel J., Schell, John B., Zeleski, Katie, Yu, Alison, Giver, Cynthia R., Waller, Edmund K., Miller, Jeffrey S., Blazar, Bruce R., and Kean, Leslie S.

Abstract

One of the central challenges of transplantation is the development of alloreactivity despite the use of multiagent immunoprophylaxis. Effective control of this immune suppression–resistant T-cell activation represents one of the key unmet needs in the fields of both solid-organ and hematopoietic stem cell transplant (HCT). To address this unmet need, we have used a highly translational nonhuman primate (NHP) model to interrogate the transcriptional signature of T cells during breakthrough acute graft-versus-host disease (GVHD) that occurs in the setting of clinically relevant immune suppression and compared this to the hyperacute GVHD, which develops in unprophylaxed or suboptimally prophylaxed transplant recipients. Our results demonstrate the complex character of the alloreactivity that develops during ongoing immunoprophylaxis and identify 3 key transcriptional hallmarks of breakthrough acute GVHD that are not observed in hyperacute GVHD: (1) T-cell persistence rather than proliferation, (2) evidence for highly inflammatory transcriptional programming, and (3) skewing toward a T helper (Th)/T cytotoxic (Tc)17 transcriptional program. Importantly, the gene coexpression profiles from human HCT recipients who developed GVHD while on immunosuppressive prophylactic agents recapitulated the patterns observed in NHP, and demonstrated an evolution toward a more inflammatory signature as time posttransplant progressed. These results strongly implicate the evolution of both inflammatory and interleukin 17–based immune pathogenesis in GVHD, and provide the first map of this evolving process in primates in the setting of clinically relevant immunomodulation. This map represents a novel transcriptomic resource for further systems-based efforts to study the breakthrough alloresponse that occurs posttransplant despite immunoprophylaxis and to develop evidence-based strategies for effective treatment of this disease.

Published

2016

18. Dose-response effects of pegylated human megakaryocyte growth and development factor on platelet production and function in nonhuman primates

Author

Harker, LA, primary, Marzec, UM, additional, Hunt, P, additional, Kelly, AB, additional, Tomer, A, additional, Cheung, E, additional, Hanson, SR, additional, and Stead, RB, additional

Published

1996

19. Systemic hematologic effects of PEG-rHuMGDF-induced megakaryocyte hyperplasia in mice

Author

Ulich, TR, primary, del Castillo, J, additional, Senaldi, G, additional, Kinstler, O, additional, Yin, S, additional, Kaufman, S, additional, Tarpley, J, additional, Choi, E, additional, Kirley, T, additional, Hunt, P, additional, and Sheridan, WP, additional

Published

1996

20. Regulation of platelet production and function by megakaryocyte growth and development factor in nonhuman primates

Author

Harker, LA, primary, Hunt, P, additional, Marzec, UM, additional, Kelly, AB, additional, Tomer, A, additional, Hanson, SR, additional, and Stead, RB, additional

Published

1996

21. The Mpl-ligand or thrombopoietin or megakaryocyte growth and differentiative factor has both direct proliferative and differentiative activities on human megakaryocyte progenitors

Author

Debili, N, primary, Wendling, F, additional, Katz, A, additional, Guichard, J, additional, Breton-Gorius, J, additional, Hunt, P, additional, and Vainchenker, W, additional

Published

1995

22. Purification and biologic characterization of plasma-derived megakaryocyte growth and development factor

Author

Hunt, P, primary, Li, YS, additional, Nichol, JL, additional, Hokom, MM, additional, Bogenberger, JM, additional, Swift, SE, additional, Skrine, JD, additional, Hornkohl, AC, additional, Lu, H, additional, and Clogston, C, additional

Published

1995

23. Recombinant human megakaryocyte growth and development factor stimulates thrombocytopoiesis in normal nonhuman primates

Author

Farese, AM, primary, Hunt, P, additional, Boone, T, additional, and MacVittie, TJ, additional

Published

1995

24. Platelets generated in vitro from proplatelet-displaying human megakaryocytes are functional

Author

Choi, ES, primary, Nichol, JL, additional, Hokom, MM, additional, Hornkohl, AC, additional, and Hunt, P, additional

Published

1995

25. Evidence that stem cell factor is involved in the rebound thrombocytosis that follows 5-fluorouracil treatment

Author

Hunt, P, primary, Zsebo, KM, additional, Hokom, MM, additional, Hornkohl, A, additional, Birkett, NC, additional, del Castillo, JC, additional, and Martin, F, additional

Published

1992

26. PET-CT staging of DLBCL accurately identifies and provides new insight into the clinical significance of bone marrow involvement

Author

Khan, Anjum Bashir, Barrington, Sally Fiona, Mikhaeel, Nabegh George, Hunt, Alesia Abigael, Cameron, Laura, Morris, Tim, and Carr, Robert

Abstract

We investigated whether positron emission tomography combined with computed tomography (PET-CT) identifies clinically important bone marrow involvement by diffuse large B-cell lymphoma (DLBCL) with sufficient accuracy to replace routine staging bone marrow biopsy. All patients from a single centre diagnosed as DLBCL since 2005 had data extracted from staging PET-CT, marrow biopsy, and treatment records. Of 130 patients, 35 (27%) were judged to have marrow involvement; 33 were identified by PET-CT compared with 14 by marrow histology. PET identified all clinically important marrow lymphoma, while biopsy did not upstage any patient. Sensitivity and specificity were 94% and 100% for PET-CT and 40% and 100% for marrow biopsy. As a secondary aim, we compared the prognosis of marrow involvement, as detected by PET-CT or biopsy. Cases with marrow deposits identified by PET-CT but not biopsy had progression-free survival (PFS) and overall survival similar to stage IV disease without involved marrow. Positive biopsy conferred significantly inferior PFS (P = .003); these cases frequently had other markers of poor-risk disease. These data confirm that in experienced hands PET-CT has a high level of accuracy for identifying marrow disease in DLBCL, and provide new insight into the nature and clinical significance of marrow involvement.

Published

2013

27. The immunologic effects of maraviroc intensification in treated HIV-infected individuals with incomplete CD4+ T-cell recovery: a randomized trial

Author

Hunt, Peter W., Shulman, Nancy S., Hayes, Timothy L., Dahl, Viktor, Somsouk, Ma, Funderburg, Nicholas T., McLaughlin, Bridget, Landay, Alan L., Adeyemi, Oluwatoyin, Gilman, Lee E., Clagett, Brian, Rodriguez, Benigno, Martin, Jeffrey N., Schacker, Timothy W., Shacklett, Barbara L., Palmer, Sarah, Lederman, Michael M., and Deeks, Steven G.

Abstract

The CCR5 inhibitor maraviroc has been hypothesized to decrease T-cell activation in HIV-infected individuals, but its independent immunologic effects have not been established in a placebo-controlled trial. We randomized 45 HIV-infected subjects with CD4 counts <350 cells per mm3and plasma HIV RNA levels <48 copies per mL on antiretroviral therapy (ART) to add maraviroc vs placebo to their regimen for 24 weeks followed by 12 weeks on ART alone. Compared with placebo-treated subjects, maraviroc-treated subjects unexpectedly experienced a greater median increase in % CD38+HLA-DR+ peripheral blood CD8+ T cells at week 24 (+2.2% vs −0.7%, P= .014), and less of a decline in activated CD4+ T cells (P< .001). The % CD38+HLA-DR+ CD4+ and CD8+ T cells increased nearly twofold in rectal tissue (both P< .001), and plasma CC chemokine receptor type 5 (CCR5) ligand (macrophage-inflammatory protein 1β) levels increased 2.4-fold during maraviroc intensification (P< .001). During maraviroc intensification, plasma lipopolysaccharide declined, whereas sCD14 levels and neutrophils tended to increase in blood and rectal tissue. Although the mechanisms explaining these findings remain unclear, CCR5 ligand-mediated activation of T cells, macrophages, and neutrophils via alternative chemokine receptors should be explored. These results may have relevance for trials of maraviroc for HIV preexposure prophylaxis and graft-versus-host disease. This trial was registered at www.clinicaltrials.govas #NCT00735072.

Published

2013

28. Activation, exhaustion, and persistent decline of the antimicrobial MR1-restricted MAIT-cell population in chronic HIV-1 infection

Author

Leeansyah, Edwin, Ganesh, Anupama, Quigley, Máire F., Sönnerborg, Anders, Andersson, Jan, Hunt, Peter W., Somsouk, Ma, Deeks, Steven G., Martin, Jeffrey N., Moll, Markus, Shacklett, Barbara L., and Sandberg, Johan K.

Abstract

Mucosal-associated invariant T (MAIT) cells are an evolutionarily conserved antimicrobial MR1-restricted T-cell subset. MAIT cells are CD161+, express a Vα7.2 TCR, are primarily CD8+ and numerous in blood and mucosal tissues. However, their role in HIV-1 infection is unknown. In this study, we found levels of MAIT cells to be severely reduced in circulation in patients with chronic HIV-1 infection. Residual MAIT cells were highly activated and functionally exhausted. Their decline was associated with time since diagnosis, activation levels, and the concomitant expansion of a subset of functionally impaired CD161− Vα7.2+ T cells. Such cells were generated in vitro by exposure of MAIT cells to Escherichia coli. Notably, whereas the function of residual MAIT cells was at least partly restored by effective antiretroviral therapy, levels of MAIT cells in peripheral blood were not restored. Interestingly, MAIT cells in rectal mucosa were relatively preserved, although some of the changes seen in blood were recapitulated in the mucosa. These findings are consistent with a model in which the MAIT-cell compartment, possibly as a result of persistent exposure to microbial material, is engaged, activated, exhausted, and progressively and persistently depleted during chronic HIV-1 infection.

Published

2013

29. Expansion of CD8+ T cells lacking Sema4D/CD100 during HIV-1 infection identifies a subset of T cells with decreased functional capacity

Author

Eriksson, Emily M., Milush, Jeffrey M., Ho, Emily L., Batista, Mariana D., Holditch, Sara J., Keh, Chris E., Norris, Philip J., Keating, Sheila M., Deeks, Steven G., Hunt, Peter W., Martin, Jeffrey N., Rosenberg, Michael G., Hecht, Frederick M., and Nixon, Douglas F.

Abstract

Sema4D, also known as CD100, is a constitutively expressed immune semaphorin on T cells and NK cells. CD100 has important immune regulatory functions that improve antigen-specific priming by antigen-presenting cells, and can also act as a costimulatory molecule on T cells. We investigated the consequence of HIV-1 infection on CD100 expression by T cells, and whether CD100 expression signifies functionally competent effector cells. CD100 expression on T cells from healthy individuals was compared with HIV-1–infected subjects including elite controllers, noncontrollers, and patients receiving antiretroviral therapy. The frequency and fluorescence intensity of CD100 on CD8+ and CD4+ T cells were decreased during HIV-1 infection. Furthermore, the absolute number of CD100-expressing CD8+ T cells was positively associated with the magnitude of HIV-1–specific T-cell responses. CD8+ T cells lacking CD100 expression were functionally impaired and present in increased numbers in HIV-1–infected individuals. The number of CD100−CD8+ T cells positively correlated with T-cell immunosenescence, immune activation, and viral load. Loss of CD100 expression appears to result from direct antigen stimulation, as in vitro cytokine exposure and viral replication did not significantly impact CD100 expression. These data suggest that loss of CD100 expression probably plays an important role in dysfunctional immunity in HIV-1 infection.

Published

2012

30. Expansion of CD8+T cells lacking Sema4D/CD100 during HIV-1 infection identifies a subset of T cells with decreased functional capacity

Author

Eriksson, Emily M., Milush, Jeffrey M., Ho, Emily L., Batista, Mariana D., Holditch, Sara J., Keh, Chris E., Norris, Philip J., Keating, Sheila M., Deeks, Steven G., Hunt, Peter W., Martin, Jeffrey N., Rosenberg, Michael G., Hecht, Frederick M., and Nixon, Douglas F.

Abstract

Sema4D, also known as CD100, is a constitutively expressed immune semaphorin on T cells and NK cells. CD100 has important immune regulatory functions that improve antigen-specific priming by antigen-presenting cells, and can also act as a costimulatory molecule on T cells. We investigated the consequence of HIV-1 infection on CD100 expression by T cells, and whether CD100 expression signifies functionally competent effector cells. CD100 expression on T cells from healthy individuals was compared with HIV-1–infected subjects including elite controllers, noncontrollers, and patients receiving antiretroviral therapy. The frequency and fluorescence intensity of CD100 on CD8+and CD4+T cells were decreased during HIV-1 infection. Furthermore, the absolute number of CD100-expressing CD8+T cells was positively associated with the magnitude of HIV-1–specific T-cell responses. CD8+T cells lacking CD100 expression were functionally impaired and present in increased numbers in HIV-1–infected individuals. The number of CD100−CD8+T cells positively correlated with T-cell immunosenescence, immune activation, and viral load. Loss of CD100 expression appears to result from direct antigen stimulation, as in vitro cytokine exposure and viral replication did not significantly impact CD100 expression. These data suggest that loss of CD100 expression probably plays an important role in dysfunctional immunity in HIV-1 infection.

Published

2012

31. A phase 2 study of the safety and efficacy of rituximab with plasma exchange in acute acquired thrombotic thrombocytopenic purpura

Author

Scully, Marie, McDonald, Vickie, Cavenagh, Jamie, Hunt, Beverley J., Longair, Ian, Cohen, Hannah, and Machin, Samuel J.

Abstract

The safety and efficacy of weekly rituximab 375 mg/m2(×4), given within 3 days of acute TTP admission, with standard therapy (PEX and steroids) was evaluated. Clinical outcomes were compared to historical controls (n = 40) who had not received rituximab. Within the trial group, 15 of 40 required ICU admission and 15% of all cases with the highest troponin T levels on admission were ventilated. Before the second rituximab infusion, 68% of cases had a platelet count > 50 × 109/L and 38% > 150 × 109/L. Fewer PEX were required in whites compared to nonwhite in the rituximab group (mean 14 vs 21, P= .0095). Inpatient stay was reduced by 7 days in the non-ICU trial cases compared to historical controls (P= .04), especially in whites, with a mean reduction of 7 days (P= .05). Ten percent of trial cases relapsed, median, 27 months (17-31 months), compared to 57% in historical controls, median 18 months (3-60 months; P= .0011). There were no excess infections or serious adverse events with rituximab. In conclusion, rituximab appears a safe and effective therapy. Inpatient stay and relapse are significantly reduced in the rituximab cohort. Rituximab should be considered in conjunction with standard therapy on acute presentation of TTP. This study was registered at www.clinicaltrials.govas NCT009-3713.

Published

2011

32. First-trimester low-dose prednisolone in refractory antiphospholipid antibody–related pregnancy loss

Author

Bramham, Kate, Thomas, Mari, Nelson-Piercy, Catherine, Khamashta, Munther, and Hunt, Beverley J.

Abstract

The objective of this study was to assess pregnancy outcome in women with a history of refractory antiphospholipid antibody–associated pregnancy loss(es) who were treated with early low-dose prednisolone in addition to aspirin and heparin. Eighteen women with antiphospholipid antibodies who had refractory pregnancy loss(es) were given prednisolone (10 mg) from the time of their positive pregnancy test to 14 weeks' gestation. Before low-dose prednisolone was given as treatment, 4 (4%) of 97 pregnancies had resulted in live births. Among 23 pregnancies supplemented with prednisolone, 9 women had 14 live births (61%), including 8 uncomplicated pregnancies. The remainder were complicated by preterm delivery, preeclampsia, and/or small-for-gestational-age infants. There were 8 first-trimester miscarriages and 1 ectopic pregnancy. There were no fetal deaths after 10 weeks' gestation and no evidence of maternal morbidity. The addition of first-trimester low-dose prednisolone to conventional treatment is worthy of further assessment in the management of refractory antiphospholipid antibody–related pregnancy loss(es), although complications remain elevated.

Published

2011

33. HIV disease progression despite suppression of viral replication is associated with exhaustion of lymphopoiesis

Author

Sauce, Delphine, Larsen, Martin, Fastenackels, Solène, Pauchard, Michèle, Ait-Mohand, Hocine, Schneider, Luminita, Guihot, Amélie, Boufassa, Faroudy, Zaunders, John, Iguertsira, Malika, Bailey, Michelle, Gorochov, Guy, Duvivier, Claudine, Carcelain, Guislaine, Kelleher, Anthony D., Simon, Anne, Meyer, Laurence, Costagliola, Dominique, Deeks, Steven G., Lambotte, Olivier, Autran, Brigitte, Hunt, Peter W., Katlama, Christine, and Appay, Victor

Abstract

The mechanisms of CD4+T-cell count decline, the hallmark of HIV disease progression, and its relationship to elevated levels of immune activation are not fully understood. Massive depletion of CD4+T cells occurs during the course of HIV-1 infection, so that maintenance of adequate CD4+T-cell levels probably depends primarily on the capacity to renew depleted lymphocytes, that is, the lymphopoiesis. We performed here a comprehensive study of quantitative and qualitative attributes of CD34+hematopoietic progenitor cells directly from the blood of a large set of HIV-infected persons compared with uninfected donors, in particular the elderly. Our analyses underline a marked impairment of primary immune resources with the failure to maintain adequate lymphocyte counts. Systemic immune activation emerges as a major correlate of altered lymphopoiesis, which can be partially reversed with prolonged antiretroviral therapy. Importantly, HIV disease progression despite elite control of HIV replication or virologic success on antiretroviral treatment is associated with persistent damage to the lymphopoietic system or exhaustion of lymphopoiesis. These findings highlight the importance of primary hematopoietic resources in HIV pathogenesis and the response to antiretroviral treatments.

Published

2011

34. Correlating cellular and molecular signatures of mucosal immunity that distinguish HIV controllers from noncontrollers

Author

Loke, P'ng, Favre, David, Hunt, Peter W., Leung, Jacqueline M., Kanwar, Bittoo, Martin, Jeffrey N., Deeks, Steven G., and McCune, Joseph M.

Abstract

HIV “controllers” are persons infected with human immunodeficiency virus, type I (HIV) who maintain long-term control of viremia without antiviral therapy and who usually do not develop the acquired immune deficiency syndrome (AIDS). In this study, we have correlated results from polychromatic flow cytometry and oligonucleotide expression arrays to characterize the mucosal immune responses of these subjects in relation to untreated HIV+ persons with high viral loads and progressive disease (“noncontrollers”). Paired peripheral blood and rectosigmoid biopsies were analyzed from 9 controllers and 11 noncontrollers. Several cellular immune parameters were found to be concordant between the 2 compartments. Compared with noncontrollers, the mucosal tissues of controllers had similar levels of effector T cells and fewer regulatory T cells (Tregs). Using principal component analysis to correlate immunologic parameters with gene expression profiles, transcripts were identified that accurately distinguished between controllers and noncontrollers. Direct 2-way comparison also revealed genes that are significantly different in their expression between controllers and noncontrollers, all of which had reduced expression in controllers. In addition to providing an approach that integrates flow cytometry datasets with transcriptional profiling analysis, these results underscore the importance of the sustained inflammatory response that attends progressive HIV disease.

Published

2010

35. International consensus report on the investigation and management of primary immune thrombocytopenia

Author

Provan, Drew, Stasi, Roberto, Newland, Adrian C., Blanchette, Victor S., Bolton-Maggs, Paula, Bussel, James B., Chong, Beng H., Cines, Douglas B., Gernsheimer, Terry B., Godeau, Bertrand, Grainger, John, Greer, Ian, Hunt, Beverley J., Imbach, Paul A., Lyons, Gordon, McMillan, Robert, Rodeghiero, Francesco, Sanz, Miguel A., Tarantino, Michael, Watson, Shirley, Young, Joan, and Kuter, David J.

Abstract

Previously published guidelines for the diagnosis and management of primary immune thrombocytopenia (ITP) require updating largely due to the introduction of new classes of therapeutic agents, and a greater understanding of the disease pathophysiology. However, treatment-related decisions still remain principally dependent on clinical expertise or patient preference rather than high-quality clinical trial evidence. This consensus document aims to report on new data and provide consensus-based recommendations relating to diagnosis and treatment of ITP in adults, in children, and during pregnancy. The inclusion of summary tables within this document, supported by information tables in the online appendices, is intended to aid in clinical decision making.

Published

2010

36. Mucosal immune responses to HIV-1 in elite controllers: a potential correlate of immune control

Author

Ferre, April L., Hunt, Peter W., Critchfield, J. William, Young, Delandy H., Morris, Megan M., Garcia, Juan C., Pollard, Richard B., Yee, Hal F., Martin, Jeffrey N., Deeks, Steven G., and Shacklett, Barbara L.

Abstract

There exists a unique group of persons who are able to durably control HIV in the absence of therapy. The mechanisms of control in these persons remain poorly defined. In this study, we examined CD8+ T-cell responses in blood and rectal mucosa from 17 “elite controllers” (viral load < 75 copies/mL), 11 “viremic controllers” (75-2000 copies/mL), 14 noncontrollers (> 10 000 copies/mL), and 10 antiretroviral-treated persons (< 75 copies/mL). Production of interferon-γ, interleukin-2, tumor necrosis factor-α, macrophage inflammatory protein-1β, and CD107a by CD8+ T cells in response to HIV-1 Gag stimulation was measured using flow cytometry. Our hypothesis was that “polyfunctional” T cells producing multiple antiviral factors would be most abundant in mucosal tissues of HIV controllers. Mucosal CD8+ T-cell responses were significantly stronger and more complex in controllers than in antiretroviral-suppressed persons (P = .0004). The frequency of 4-function responses in rectal mucosa was higher in controllers than in noncontrollers and patients on therapy (P < .0001). Mucosal responses in controllers were frequently stronger and more complex than blood responses. These findings demonstrate that many controllers mount strong, complex HIV-specific T-cell responses in rectal mucosa. These responses may play an important role in mucosal immune surveillance, as suggested by their relative enrichment among persons who control HIV in the absence of therapy.

Published

2009

37. Peripheral tachykinins and the neurokinin receptor NK1 are required for platelet thrombus formation

Author

Jones, Sarah, Tucker, Katherine L., Sage, Tanya, Kaiser, William J., Barrett, Natasha E., Lowry, Philip J., Zimmer, Andreas, Hunt, Stephen P., Emerson, Michael, and Gibbins, Jonathan M.

Abstract

Platelets play an important role in hemostasis, with inappropriate platelet activation being a major contributor to debilitating and often fatal thrombosis by causing myocardial infarction and stroke. Although current antithrombotic treatment is generally well tolerated and effective, many patients still experience cardiovascular problems, which may reflect the existence of alternative underlying regulatory mechanisms in platelets to those targeted by existing drugs. In this study, we define a role for peripherally distributed members of the tachykinin family of peptides, namely substance P and the newly discovered endokinins A and B that are present in platelets, in the activation of platelet function and thrombus formation. We have reported previously that the preferred pharmacologically characterized receptor for these peptides, the NK1 receptor, is present on platelets. Inhibition or deficiency of the NK1 receptor, or SP agonist activity, resulted in substantially reduced thrombus formation in vitro under arterial flow conditions, increased bleeding time in mice, and a decrease in experimentally induced thromboembolism. Inhibition of the NK1 receptor may therefore provide benefit in patients vulnerable to thrombosis and may offer an alternative therapeutic target.

Published

2008

38. Survival Outcomes for Plasmablastic Lymphoma: An International, Multicentre Study By the Australasian Lymphoma Alliance

Author

Di Ciaccio, Pietro R, Polizzotto, Mark N., Cwynarski, Kate, Burton, Cathy, Jiamsakul, Awachana, Bower, Mark, Kuruvilla, John, Montoto, Silvia, McKay, Pam, Osborne, Wendy, Milliken, Sam, Linton, Kim, Manos, Kate, Kassam, Shireen, Wong Doo, Nicole, Watson, Anne-Marie, Fedele, Pasquale L, Yannakou, Costas K., Hunt, Stewart, Renshaw, Hanna, Thakrar, Nisha, Smith, Alexandra, Painter, Daniel, Maxwell, Alice, Liu, Qin, Dhairyawan, Rageshri, Ferguson, Graeme, Pickard, Keir, and Hamad, Nada

Abstract

Introduction

Published

2020

39. Pegaspargase Re-Challenge after Grade 2 Hypersensitivity Reaction in Childhood Acute Lymphoblastic Leukemia: Results from DFCI 16-001

Author

Vrooman, Lynda M., Flamand, Yael, Koch, Victoria, Burns, Melissa A., Cronholm, Sarah M., Hunt, Sarah K., Cole, Peter D., Gennarini, Lisa M., Kahn, Justine M., Kelly, Kara M., Michon, Bruno, Neuberg, Donna S., Place, Andrew E., Tran, Thai Hoa, Welch, Jennifer J.G., Stevenson, Kristen E., Sallan, Stephen E., and Silverman, Lewis B.

Abstract

Introduction:Hypersensitivity reactions with asparaginase occur frequently in pediatric patients (pts) with acute lymphoblastic leukemia (ALL). The standard approach for pts with reaction to E.coli-derived asparaginase is to switch to Erwinia asparaginase, given concern that clinical reactions reflect presence of neutralizing antibodies; however, Erwinia requires more frequent dosing and is often unavailable. Therapeutic drug monitoring allows for discrimination between pts with pegaspargase hypersensitivity who have sub-therapeutic asparaginase activity and those still able to derive therapeutic benefit from pegaspargase. We prospectively piloted re-challenging pts with pegaspargase after initial Grade 2 hypersensitivity to this agent, with premedication at re-challenge and assessment of serum asparaginase activity (SAA).

Published

2020

40. The PANE1 gene encodes a novel human minor histocompatibility antigen that is selectively expressed in B-lymphoid cells and B-CLL

Author

Brickner, Anthony G., Evans, Anne M., Mito, Jeffrey K., Xuereb, Suzanne M., Feng, Xin, Nishida, Tetsuya, Fairfull, Liane, Ferrell, Robert E., Foon, Kenneth A., Hunt, Donald F., Shabanowitz, Jeffrey, Engelhard, Victor H., Riddell, Stanley R., and Warren, Edus H.

Abstract

Minor histocompatibility antigens (mHAg's) are peptides encoded by polymorphic genes that are presented by major histocompatibility complex (MHC) molecules and recognized by T cells in recipients of allogeneic hematopoietic cell transplants. Here we report that an alternative transcript of the proliferation-associated nuclear element 1 (PANE1) gene encodes a novel human leukocyte antigen (HLA)-A*0301-restricted mHAg that is selectively expressed in B-lymphoid cells. The antigenic peptide is entirely encoded within a unique exon not present in other PANE1 transcripts. Sequencing of PANE1 alleles in mHAg-positive and mHAg-negative cells demonstrates that differential T-cell recognition is due to a single nucleotide polymorphism within the variant exon that replaces an arginine codon with a translation termination codon. The PANE1 transcript that encodes the mHAg is expressed at high levels in resting CD19+ B cells and B-lineage chronic lymphocytic leukemia (B-CLL) cells, and at significantly lower levels in activated B cells. Activation of B-CLL cells through CD40 ligand (CD40L) stimulation decreases expression of the mHAg-encoding PANE1 transcript and reciprocally increases expression of PANE1 transcripts lacking the mHAg-encoding exon. These studies suggest distinct roles for different PANE1 isoforms in resting compared with activated CD19+ cells, and identify PANE1 as a potential therapeutic target in B-CLL.

Published

2006

41. The PANE1gene encodes a novel human minor histocompatibility antigen that is selectively expressed in B-lymphoid cells and B-CLL

Author

Brickner, Anthony G., Evans, Anne M., Mito, Jeffrey K., Xuereb, Suzanne M., Feng, Xin, Nishida, Tetsuya, Fairfull, Liane, Ferrell, Robert E., Foon, Kenneth A., Hunt, Donald F., Shabanowitz, Jeffrey, Engelhard, Victor H., Riddell, Stanley R., and Warren, Edus H.

Abstract

Minor histocompatibility antigens (mHAg's) are peptides encoded by polymorphic genes that are presented by major histocompatibility complex (MHC) molecules and recognized by T cells in recipients of allogeneic hematopoietic cell transplants. Here we report that an alternative transcript of the proliferation-associated nuclear element 1 (PANE1)gene encodes a novel human leukocyte antigen (HLA)-A*0301-restricted mHAg that is selectively expressed in B-lymphoid cells. The antigenic peptide is entirely encoded within a unique exon not present in other PANE1transcripts. Sequencing of PANE1alleles in mHAg-positive and mHAg-negative cells demonstrates that differential T-cell recognition is due to a single nucleotide polymorphism within the variant exon that replaces an arginine codon with a translation termination codon. The PANE1transcript that encodes the mHAg is expressed at high levels in resting CD19+B cells and B-lineage chronic lymphocytic leukemia (B-CLL) cells, and at significantly lower levels in activated B cells. Activation of B-CLL cells through CD40 ligand (CD40L) stimulation decreases expression of the mHAg-encoding PANE1transcript and reciprocally increases expression of PANE1transcripts lacking the mHAg-encoding exon. These studies suggest distinct roles for different PANE1 isoforms in resting compared with activated CD19+cells, and identify PANE1as a potential therapeutic target in B-CLL.

Published

2006

42. Immune activation set point during early HIV infection predicts subsequent CD4+ T-cell changes independent of viral load

Author

Deeks, Steven G., Kitchen, Christina M. R., Liu, Lea, Guo, Hua, Gascon, Ron, Narváez, Amy B., Hunt, Peter, Martin, Jeffrey N., Kahn, James O., Levy, Jay, McGrath, Michael S., and Hecht, Frederick M.

Abstract

Although generalized T-cell activation is an important factor in chronic HIV disease pathogenesis, its role in primary infection remains poorly defined. To investigate the effect of immune activation on T-cell changes in subjects with early HIV infection, and to test the hypothesis that an immunologic activation “set point” is established early in the natural history of HIV disease, a prospective cohort of acutely infected adults was performed. The median density of CD38 molecules on CD4+ and CD8+ T cells was measured longitudinally in 68 antiretroviral-untreated individuals and 83 antiretroviral-treated individuals. At study entry, T-cell activation was positively associated with viremia, with CD8+ T-cell activation levels increasing exponentially at plasma HIV RNA levels more than 10 000 copies/mL. Among untreated patients, the level of CD8+ T-cell activation varied widely among individuals but often remained stable within a given individual. CD8+ T-cell activation and plasma HIV RNA levels over time were independently associated with the rate of CD4+ T-cell loss in untreated individuals. These data indicate that immunologic activation set point is established early in HIV infection, and that this set point determines the rate at which CD4+ T cells are lost over time.

Published

2004

43. Immune activation set point during early HIV infection predicts subsequent CD4+T-cell changes independent of viral load

Author

Deeks, Steven G., Kitchen, Christina M.R., Liu, Lea, Guo, Hua, Gascon, Ron, Narváez, Amy B., Hunt, Peter, Martin, Jeffrey N., Kahn, James O., Levy, Jay, McGrath, Michael S., and Hecht, Frederick M.

Abstract

Although generalized T-cell activation is an important factor in chronic HIV disease pathogenesis, its role in primary infection remains poorly defined. To investigate the effect of immune activation on T-cell changes in subjects with early HIV infection, and to test the hypothesis that an immunologic activation“set point” is established early in the natural history of HIV disease, a prospective cohort of acutely infected adults was performed. The median density of CD38 molecules on CD4+and CD8+T cells was measured longitudinally in 68 antiretroviral-untreated individuals and 83 antiretroviral-treated individuals. At study entry, T-cell activation was positively associated with viremia, with CD8+T-cell activation levels increasing exponentially at plasma HIV RNA levels more than 10 000 copies/mL. Among untreated patients, the level of CD8+T-cell activation varied widely among individuals but often remained stable within a given individual. CD8+T-cell activation and plasma HIV RNA levels over time were independently associated with the rate of CD4+T-cell loss in untreated individuals. These data indicate that immunologic activation set point is established early in HIV infection, and that this set point determines the rate at which CD4+T cells are lost over time.

Published

2004

44. The minor histocompatibility antigen HA-3 arises from differential proteasome–mediated cleavage of the lymphoid blast crisis (Lbc) oncoprotein

Author

Spierings, Eric, Brickner, Anthony G., Caldwell, Jennifer A., Zegveld, Suzanne, Tatsis, Nia, Blokland, Els, Pool, Jos, Pierce, Richard A., Mollah, Sahana, Shabanowitz, Jeffrey, Eisenlohr, Laurence C., Van Veelen, Peter, Ossendorp, Ferry, Hunt, Donald F., Goulmy, Els, and Engelhard, Victor H.

Abstract

Minor histocompatibility (H) antigens crucially affect the outcome of human leukocyte antigen (HLA)–identical allogeneic stem cell transplantation (SCT). To understand the basis of alloimmune responses against minor H antigens, identification of minor H peptides and their antigenicity-determining mechanisms is essential. Here we report the identification of HA-3 and its encoding gene. The HA-3 peptide, VTEPGTAQY (HA-3T), is encoded by the lymphoid blast crisis (Lbc) oncogene. We thus show for the first time that a leukemia-associated oncogene can give rise to immunogenic T-cell epitopes that may have participated in antihost and antileukemic alloimmune responses. Genotypic analysis of HA-3- individuals revealed the allelic counterpart VMEPGTAQY (HA-3M). Despite the lack of T-cell recognition of HA-3- cells, the Thr→Met substitution had only a modest effect on peptide binding to HLA-A1 and a minimal impact on recognition by T cells when added exogenously to target cells. This substitution did not influence transporter associated with antigen processing (TAP) transport, but, in contrast to the HA-3T peptide, HA-3M is destroyed by proteasome-mediated digestion. Thus, the immunogenicity of minor H antigens can result from proteasome-mediated destruction of the negative allelic peptide.

Published

2003

45. The toxicity and efficacy of donor lymphocyte infusions given after reduced-intensity conditioning allogeneic stem cell transplantation

Author

Marks, David I., Lush, Richard, Cavenagh, Jamie, Milligan, Donald W., Schey, Steven, Parker, Anne, Clark, Fiona J., Hunt, Linda, Yin, John, Fuller, Steven, Vandenberghe, Elisabeth, Marsh, Judith, Littlewood, Timothy, Smith, Graeme M., Culligan, Dominic, Hunter, Ann, Chopra, Rajesh, Davies, Andrew, Towlson, Keiren, and Williams, Catherine D.

Abstract

We describe the toxicity and efficacy of donor lymphocyte infusions (DLIs) given to 81 patients (median age, 50 years) after reduced-intensity conditioning (RIC) transplantations performed at 16 centers in the United Kingdom. The diseases treated included non-Hodgkin lymphoma (NHL; n = 29), chronic myeloid leukemia (CML; n = 12), myeloma (n = 11), acute myeloid leukemia (AML; n = 10), and chronic lymphocytic leukemia (CLL; n = 9). Eighty-eight percent received stem cells from sibling donors. The patients received 130 infusions (median, 1; range, 1-4). Indications for DLI were unsatisfactory response/disease progression in 51 patients, mixed chimerism in 18, preemptive in 10, and other in 2. Graft hypoplasia was uncommon (11%). Grade II to IV graft-versus-host disease (GVHD) occurred in 23 of 81 patients (28%) and limited and extensive chronic GVHD in 5 of 69 and 18 of 69 evaluable patients (total incidence 33%). Conversion from mixed to full donor chimerism occurred in 19 of 55 evaluable patients (35%) at a median of 48 days after the DLI; partial responses occurred in 6 patients (total response rate 45%). Eighteen of 51 (35%) patients with measurable disease after stem cell transplantation had a complete response (2 molecular), and 5 a partial response (total response rate 45%). Eleven of 17 evaluable complete responders had full donor chimerism. Eight of 13 patients with follicular NHL had complete responses as did 4 of 12 patients with CML. Clinical and chimeric responses correlated strongly with acute and chronic GVHD. Forty-seven patients (58%) survive at a median of 508 days after transplantation (range, 155-1171 days) with a median Karnofsky score of 90. Thirty-four patients (42%) died at a median of 211 days after transplantation with the major causes being progressive disease (26%) and GVHD (9%). Further systematic studies are required to determine the efficacy and optimum use of DLI for patients with each disease treated by nonmyeloablative stem cell transplantation.

Published

2002

46. Nuclear factor-?B activation by the photochemotherapeutic agent verteporfin

Author

Granville, D. J., Carthy, C. M., Jiang, H., Levy, J. G., McManus, B. M., Matroule, J.-Y., Piette, J., and Hunt, D. W. C.

Abstract

The nuclear factor-kappa B (NF-?B) gene transactivator serves in the formation of immune, inflammatory, and stress responses. In quiescent cells, NF-?B principally resides within the cytoplasm in association with inhibitory ? (I?B) proteins. The status of I?B and NF-?B proteins was evaluated for promyelocytic leukemia HL-60 cells treated at different intensities of photodynamic therapy (PDT). The action of the potent photosensitizer, benzoporphyrin derivative monoacid ring A (verteporfin), and visible light irradiation were assessed. At a verteporfin concentration that produced the death of a high proportion of cells after light irradiation, evidence of caspase-3 and caspase-9 processing and of poly(ADP-ribose) polymerase cleavage was present within whole cell lysates. The general caspase inhibitor Z-Val-Ala-Asp-fluoromethylketone (ZVAD.fmk) effectively blocked these apoptosis-related changes. Recent studies indicate that I?B proteins may be caspase substrates during apoptosis. However, the level of I?Bß was unchanged for HL-60 cells undergoing PDT-induced apoptosis. I?B? levels decreased during PDT-induced apoptosis, though ZVAD.fmk did not affect this change. At a less intensive level of photosensitization, cellular I?B? levels were transiently depressed after PDT. At these times, p50 and RelA NF-?B species were increased within nuclear extracts, as revealed by electrophoretic mobility supershift assays. HL-60 cells transiently transfected with a ?B-luciferase reporter construct exhibited elevated luciferase activity after PDT or treatment with tumor necrosis factor-?, a well-characterized NF-?B activator. Productive NF-?B activation and associated gene transcription may influence the phenotype and behavior of cells exposed to less intensive PDT regimens. However, I?B? is not subject to caspase-mediated degradation as a component of PDT-induced apoptosis. (Blood. 2000;95:256-262)

Published

2000

47. Incidence of Breakthrough Fungal Infections in Acute Myeloid Leukemia Patients Receiving Low Intensity Therapy in the Upfront and Relapsed/Refractory Setting

Author

Shuman, Kaci, Hunt, Rebecca Garcia, Hibino, Maho, Stone, Tyler, Dralle, Sarah, Manuel, Megan, Lyerly, Susan, Ellis, Leslie Renee, Bhave, Rupali, Pardee, Timothy S., Powell, Bayard L., and Reed, Daniel R.

Abstract

Introduction:New treatment strategies with low intensity therapy have emerged for acute myeloid leukemia (AML) patients who are not candidates for intensive therapy. To date, there is limited data on the frequency of invasive fungal infections (IFIs) in patients treated with low intensity regimens, and there is no consensus on the most appropriate prophylactic antifungal agent to use in either the newly diagnosed or relapsed/refractory setting. At our institution, fluconazole is the prophylactic antifungal agent of choice for neutropenic patients receiving low intensity therapy, however the appropriateness of fluconazole is being questioned due to the depth and duration of neutropenia observed in these patients. Rates of breakthrough IFIs need to be better characterized to optimize antifungal prophylaxis in this patient population.

Published

2021

48. Minimal Residual Disease Status Before Allogeneic Bone Marrow Transplantation Is an Important Determinant of Successful Outcome for Children and Adolescents With Acute Lymphoblastic Leukemia

Author

Knechtli, Christopher J.C., Goulden, Nicholas J., Hancock, Jeremy P., Grandage, Victoria L.G., Harris, Emma L., Garland, Russell J., Jones, Claire G., Rowbottom, Anthony W., Hunt, Linda P., Green, Ann F., Clarke, Emer, Lankester, Alan W., Cornish, Jacqueline M., Pamphilon, Derwood H., Steward, Colin G., and Oakhill, Anthony

Abstract

The efficacy of allografting in acute lymphoblastic leukemia (ALL) is heavily influenced by remission status at the time of transplant. Using polymerase chain reaction (PCR)-based minimal residual disease (MRD) analysis, we have investigated retrospectively the impact of submicroscopic leukemia on outcome in 64 patients receiving allogeneic bone marrow transplantation (BMT) for childhood ALL. Remission BM specimens were taken 6 to 81 days (median, 23) before transplant. All patients received similar conditioning therapy; 50 received grafts from unrelated donors and 14 from related donors. Nineteen patients were transplanted in first complete remission (CR1) and 45 in second or subsequent CR. MRD was analyzed by PCR of Ig or T-cell receptor d or ? rearrangements, electrophoresis, and allele-specific oligoprobing. Samples were rated high-level positive (clonal band evident after electrophoresis; sensitivity 10-2 to 10-3), low-level positive (MRD detected only after oligoprobing; sensitivity 10-3 to 10-5), or negative. Excluding 8 patients transplanted in CR2 for isolated extramedullary relapse (all MRD-), MRD was detected at high level in 12 patients, low level in 11, and was undetectable in 33. Two-year event-free survival for these groups was 0%, 36%, and 73%, respectively (P < .001). Follow-up in patients remaining in continuing remission is 20 to 96 months (median, 35). These results suggest that MRD analysis could be used routinely in this setting. This would allow identification of patients with resistant leukemia (who may benefit from innovative BMT protocols) and of those with more responsive disease (who may be candidates for randomized trials of BMT versus modern intensive relapse chemotherapy).

Published

1998

49. Children With Acute Lymphoblastic Leukemia Who Receive T-Cell–Depleted HLA Mismatched Marrow Allografts From Unrelated Donors Have an Increased Incidence of Primary Graft Failure but a Similar Overall Transplant Outcome

Author

Green, Ann, Clarke, Emer, Hunt, Linda, Canterbury, Andrew, Lankester, Alan, Hale, Geoff, Waldmann, Herman, Goodman, Sally, Cornish, Jacqueline M., Marks, David I., Steward, Colin G., Oakhill, Anthony, and Pamphilon, Derwood H.

Abstract

Disparity for HLA in unrelated donor bone marrow transplantation (BMT) increases the risk of graft rejection and graft-versus-host disease (GVHD) and may compromise transplant outcome. We have compared the outcome of matched and mismatched transplants from unrelated donors in 137 children with acute lymphoblastic leukemia (ALL). Their disease status was complete remission (CR)-1, 24 patients; CR-2, 88 patients; CR-3, 18 patients; CR-4, 2 patients; and relapse, 5 patients. CAMPATH monoclonal antibodies were used for T-cell depletion and cyclosporin A was given to 134 children together with short-course methotrexate in 43, mainly when there was HLA disparity. Fifty-two donor/recipient pairs were HLA-mismatched, 41 at HLA-A and -B and 11 at HLA-DR and -DQ loci. Overall graft failure was increased in recipients of marrow mismatched at either HLA-A, -B, -DR, or -DQ (15.7% v 4.8%; P = .057) mainly because there was a higher proportion of children with primary graft failure (11.8% v 1.2%; P = .012). The presence of an HLA-C locus mismatch did not independently increase the likelihood of graft failure. There was no significant difference in the incidence of acute GVHD ≥ grade 2 between the matched and mismatched groups (P = .849). For patients in CR-2, the risk of relapse post-BMT was significantly lower if leukemic relapse occurred off-treatment (P = .005). The Kaplan-Meier overall and leukemia-free survival (LFS) estimates for recipients of matched and mismatched BMT, respectively, at 36 months were 49% versus 42% (P = .380) and 45% versus 40% (P = .654). Although HLA mismatching results in an increased occurrence of primary graft failure with T-cell–depleted allografts, it allows more donors to be identified rapidly for children with ALL without compromising overall transplant outcome.

Published

1999

50. Platelet Adhesion to Collagen Under Flow Causes Dissociation of a Phosphoprotein Complex of Heat-Shock Proteins and Protein Phosphatase 1

Author

Polanowska-Grabowska, Renata, Simon, Carl G., Falchetto, Rocco, Shabanowitz, Jeffrey, Hunt, Donald F., and Gear, Adrian R.L.

Abstract

Phosphorylation/dephosphorylation events in human blood platelets were investigated during their adhesion to collagen under flow conditions. Using 32P-labeled platelets and one-dimensional gel electrophoresis, we found that adhesion to collagen mediated primarily by the a2ß1 integrin resulted in a strong dephosphorylation of several protein bands. Neither adhesion to polylysine nor thrombin-induced aggregation caused similar protein dephosphorylation. In addition, treatment with okadaic acid (OA), an inhibitor of serine/threonine protein phosphatases type 1 (PP1) and 2A (PP2A), caused significant inhibition of adhesion, suggesting that adhesion is regulated by OA-sensitive phosphatases. Recent studies indicate that phosphatases may be associated with the heat-shock proteins. Immunoprecipitations with antibodies against either the heat-shock cognate protein 70 (hsc70) or heat-shock protein 90 (hsp90) showed the presence of a phosphoprotein complex in 32P-labeled, resting human platelets. Antibody probing of this complex detected hsc70, hsp90, two isoforms of the catalytic subunit of PP1, PP1Ca and PP1Cd, as well as the M regulatory subunit of PP1 (PP1M). OA, at concentrations that markedly blocked platelet adhesion to collagen, caused hyperphosphorylation of the hsc70 complex. In platelets adhering to collagen, hsc70 was completely dephosphorylated and hsp90, PP1a, and PP1M were dissociated from the complex, suggesting involvement of heat-shock proteins and protein phosphatases in platelet adhesion.

Published

1997