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270 results on '"DYER, MARTIN"'

1. The Gravitational-wave Optical Transient Observer (GOTO)

Author

Marshall, Heather K., Spyromilio, Jason, Usuda, Tomonori, Dyer, Martin J., Ackley, Kendall, Jiménez-Ibarra, Felipe, Lyman, Joseph, Ulaczyk, Krzysztof, Steeghs, Danny, Galloway, Duncan K., Dhillon, Vik S., O'Brien, Paul, Ramsay, Gavin, Noysena, Kanthanakorn, Kotak, Rubina, Breton, Rene, Nuttall, Laura, Pallé, Enric, Pollacco, Don, Killestein, Tom, Kumar, Amit, O'Neill, David, Kelsey, Lisa, Godson, Ben, and Jarvis, Dan

Published
2024
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2. Heavy-element production in a compact object merger observed by JWST

Author

Levan, Andrew J., Gompertz, Benjamin P., Salafia, Om Sharan, Bulla, Mattia, Burns, Eric, Hotokezaka, Kenta, Izzo, Luca, Lamb, Gavin P., Malesani, Daniele B., Oates, Samantha R., Ravasio, Maria Edvige, Rouco Escorial, Alicia, Schneider, Benjamin, Sarin, Nikhil, Schulze, Steve, Tanvir, Nial R., Ackley, Kendall, Anderson, Gemma, Brammer, Gabriel B., Christensen, Lise, Dhillon, Vikram S., Evans, Phil A., Fausnaugh, Michael, Fong, Wen-fai, Fruchter, Andrew S., Fryer, Chris, Fynbo, Johan P. U., Gaspari, Nicola, Heintz, Kasper E., Hjorth, Jens, Kennea, Jamie A., Kennedy, Mark R., Laskar, Tanmoy, Leloudas, Giorgos, Mandel, Ilya, Martin-Carrillo, Antonio, Metzger, Brian D., Nicholl, Matt, Nugent, Anya, Palmerio, Jesse T., Pugliese, Giovanna, Rastinejad, Jillian, Rhodes, Lauren, Rossi, Andrea, Saccardi, Andrea, Smartt, Stephen J., Stevance, Heloise F., Tohuvavohu, Aaron, van der Horst, Alexander, Vergani, Susanna D., Watson, Darach, Barclay, Thomas, Bhirombhakdi, Kornpob, Breedt, Elmé, Breeveld, Alice A., Brown, Alexander J., Campana, Sergio, Chrimes, Ashley A., D’Avanzo, Paolo, D’Elia, Valerio, De Pasquale, Massimiliano, Dyer, Martin J., Galloway, Duncan K., Garbutt, James A., Green, Matthew J., Hartmann, Dieter H., Jakobsson, Páll, Kerry, Paul, Kouveliotou, Chryssa, Langeroodi, Danial, Le Floc’h, Emeric, Leung, James K., Littlefair, Stuart P., Munday, James, O’Brien, Paul, Parsons, Steven G., Pelisoli, Ingrid, Sahman, David I., Salvaterra, Ruben, Sbarufatti, Boris, Steeghs, Danny, Tagliaferri, Gianpiero, Thöne, Christina C., de Ugarte Postigo, Antonio, and Kann, David Alexander

Abstract

The mergers of binary compact objects such as neutron stars and black holes are of central interest to several areas of astrophysics, including as the progenitors of gamma-ray bursts (GRBs)1, sources of high-frequency gravitational waves (GWs)2and likely production sites for heavy-element nucleosynthesis by means of rapid neutron capture (the r-process)3. Here we present observations of the exceptionally bright GRB 230307A. We show that GRB 230307A belongs to the class of long-duration GRBs associated with compact object mergers4–6and contains a kilonova similar to AT2017gfo, associated with the GW merger GW170817 (refs. 7–12). We obtained James Webb Space Telescope (JWST) mid-infrared imaging and spectroscopy 29 and 61 days after the burst. The spectroscopy shows an emission line at 2.15 microns, which we interpret as tellurium (atomic mass A= 130) and a very red source, emitting most of its light in the mid-infrared owing to the production of lanthanides. These observations demonstrate that nucleosynthesis in GRBs can create r-process elements across a broad atomic mass range and play a central role in heavy-element nucleosynthesis across the Universe.

Published
2024
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3. A rotating white dwarf shows different compositions on its opposite faces

Author

Caiazzo, Ilaria, Burdge, Kevin B., Tremblay, Pier-Emmanuel, Fuller, James, Ferrario, Lilia, Gänsicke, Boris T., Hermes, J. J., Heyl, Jeremy, Kawka, Adela, Kulkarni, S. R., Marsh, Thomas R., Mróz, Przemek, Prince, Thomas A., Richer, Harvey B., Rodriguez, Antonio C., van Roestel, Jan, Vanderbosch, Zachary P., Vennes, Stéphane, Wickramasinghe, Dayal, Dhillon, Vikram S., Littlefair, Stuart P., Munday, James, Pelisoli, Ingrid, Perley, Daniel, Bellm, Eric C., Breedt, Elmé, Brown, Alex J., Dekany, Richard, Drake, Andrew, Dyer, Martin J., Graham, Matthew J., Green, Matthew J., Laher, Russ R., Kerry, Paul, Parsons, Steven G., Riddle, Reed L., Rusholme, Ben, and Sahman, Dave I.

Abstract

White dwarfs, the extremely dense remnants left behind by most stars after their death, are characterized by a mass comparable to that of the Sun compressed into the size of an Earth-like planet. In the resulting strong gravity, heavy elements sink towards the centre and the upper layer of the atmosphere contains only the lightest element present, usually hydrogen or helium1,2. Several mechanisms compete with gravitational settling to change a white dwarf’s surface composition as it cools3, and the fraction of white dwarfs with helium atmospheres is known to increase by a factor of about 2.5 below a temperature of about 30,000 kelvin4–8; therefore, some white dwarfs that appear to have hydrogen-dominated atmospheres above 30,000 kelvin are bound to transition to be helium-dominated as they cool below it. Here we report observations of ZTF J203349.8+322901.1, a transitioning white dwarf with two faces: one side of its atmosphere is dominated by hydrogen and the other one by helium. This peculiar nature is probably caused by the presence of a small magnetic field, which creates an inhomogeneity in temperature, pressure or mixing strength over the surface9–11. ZTF J203349.8+322901.1 might be the most extreme member of a class of magnetic, transitioning white dwarfs—together with GD 323 (ref. 12), a white dwarf that shows similar but much more subtle variations. This class of white dwarfs could help shed light on the physical mechanisms behind the spectral evolution of white dwarfs.

Published
2023
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5. The Gravitational-wave Optical Transient Observer (GOTO)

Author

Marshall, Heather K., Spyromilio, Jason, Usuda, Tomonori, Dyer, Martin J., Ackley, Kendall, Lyman, Joe, Ulaczyk, Krzysztof, Steeghs, Danny, Galloway, Duncan K., Dhillon, Vik S., O'Brien, Paul, Ramsay, Gavin, Noysena, Kanthanakorn, Kotak, Rubina, Breton, Rene, Nuttall, Laura, Pallé, Enric, and Pollacco, Don

Published
2022
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6. Venetoclax retreatment of patients with chronic lymphocytic leukemia after a previous venetoclax-based regimen

Author

Thompson, Meghan C., Harrup, Rosemary A., Coombs, Catherine C., Roeker, Lindsey E., Pu, Jeffrey J., Choi, Michael Y., Barr, Paul M., Allan, John N., Šimkovič, Martin, Leslie, Lori, Rhodes, Joanna, Chong, Elise A., Kamdar, Manali, Skarbnik, Alan, Lansigan, Frederick, McCall, Brittany, Saja, Khalid, Dyer, Martin J. S., Walter, Harriet S., Lefebure, Marcus, Thadani-Mulero, Maria, Boyer, Michelle, Biondo, Juliana, Sail, Kavita, Manzoor, Beenish S., Furman, Richard, Bantilan, Kurt S., Goy, Andre, Feldman, Tatyana, Labella, Dominic, Schuster, Stephen J., Park, Jae, Palomba, Lia, Zelenetz, Andrew, Eyre, Toby A., Kater, Arnon P., Seymour, John F., and Mato, Anthony R.

Published
2022
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7. Venetoclax retreatment of patients with chronic lymphocytic leukemia after a previous venetoclax-based regimen

Author

Thompson, Meghan C., Harrup, Rosemary A., Coombs, Catherine C., Roeker, Lindsey E., Pu, Jeffrey J., Choi, Michael Y., Barr, Paul M., Allan, John N., Šimkovič, Martin, Leslie, Lori, Rhodes, Joanna, Chong, Elise A., Kamdar, Manali, Skarbnik, Alan, Lansigan, Frederick, McCall, Brittany, Saja, Khalid, Dyer, Martin J.S., Walter, Harriet S., Lefebure, Marcus, Thadani-Mulero, Maria, Boyer, Michelle, Biondo, Juliana, Sail, Kavita, Manzoor, Beenish S., Furman, Richard, Bantilan, Kurt S., Goy, Andre, Feldman, Tatyana, Labella, Dominic, Schuster, Stephen J., Park, Jae, Palomba, Lia, Zelenetz, Andrew, Eyre, Toby A., Kater, Arnon P., Seymour, John F., and Mato, Anthony R.

Published
2022
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8. GERry: A code to optimise the hunt for the electromagnetic counter-parts to gravitational wave events

Author

Benn, Chris R., Chrysostomou, Antonio, Storrie-Lombardi, Lisa J., O'Neill, David, Lyman, Joseph, Ackley, Kendall, Steeghs, Danny, Galloway, Duncan, Dhillon, Vik, O'Brien, Paul, Ramsay, Gavin, Noysena, Kanthanakorn, Kotak, Rubina, Breton, Rene, Nuttall, Laura, Pallé, Enric, Pollacco, Don, Ulaczyk, Krzysztof, Dyer, Martin, Jiménez-Ibarra, Felipe, Killestein, Tom, Kumar, Amit, Kelsey, Lisa, Godson, Ben, and Jarvis, Dan

Published
2024
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9. Pooled analysis of safety data from clinical trials evaluating acalabrutinib monotherapy in mature B-cell malignancies

Author

Furman, Richard R., Byrd, John C., Owen, Roger G., O’Brien, Susan M., Brown, Jennifer R., Hillmen, Peter, Stephens, Deborah M., Chernyukhin, Nataliya, Lezhava, Tamara, Hamdy, Ahmed M., Izumi, Raquel, Patel, Priti, Baek, Marshall, Christian, Beth, Dyer, Martin J. S., Streetly, Matthew J., Sun, Clare, Rule, Simon, Wang, Michael, Ghia, Paolo, Jurczak, Wojciech, Pagel, John M., and Sharman, Jeff P.

Abstract

Bruton tyrosine kinase (BTK) inhibition is an effective therapy for many B-cell malignancies. Acalabrutinib is a next-generation, potent, highly selective, covalent BTK inhibitor. To characterize acalabrutinib tolerability, we pooled safety data from 1040 patients with mature B-cell malignancies treated with acalabrutinib monotherapy in nine clinical studies (treatment-naïve: n= 366 [35%], relapsed/refractory: n= 674 [65%]; median [range] age: 67 [32–90] years; median [range] prior treatments: 1 [0–13]; median [range] duration of exposure: 24.6 [0.0–58.5] months). The most common adverse events (AEs) were headache (38%), diarrhea (37%), upper respiratory tract infection (22%), contusion (22%), nausea (22%), fatigue (21%), and cough (21%). Serious AEs (SAEs) occurred in 39% of patients; pneumonia (6%) was the only SAE that occurred in ≥2%. Deaths due to AEs occurred in 52 patients (5%); pneumonia (n= 8) was the only fatal AE to occur in ≥3 patients. AEs led to treatment discontinuation in 9%. Rates for the AEs of interest (all grades) included infections (67%), hemorrhages (46%), neutropenia (16%), anemia (14%), second primary malignancies (12%), thrombocytopenia (9%), hypertension (8%), and atrial fibrillation (4%). This pooled analysis confirmed acalabrutinib’s tolerability and identified no newly emerging late toxicities, supporting acalabrutinib as a long-term treatment for patients with mature B-cell malignancies.

Published
2021
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10. Phase 1b study of tirabrutinib in combination with idelalisib or entospletinib in previously treated B-cell lymphoma

Author

Morschhauser, Franck, Dyer, Martin J. S., Walter, Harriet S., Danilov, Alexey V., Ysebaert, Loic, Hodson, Daniel James, Fegan, Christopher, Rule, Simon A., Radford, John, Cartron, Guillaume, Bouabdallah, Krimo, Davies, Andrew John, Spurgeon, Stephen, Rajakumaraswamy, Nishanthan, Li, Biao, Humeniuk, Rita, Huang, Xi, Bhargava, Pankaj, Jürgensmeier, Juliane M., and Salles, Gilles

Published
2021
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13. Developing the GOTO telescope control system

Author

Guzman, Juan C., Ibsen, Jorge, Dyer, Martin J., Dhillon, Vik S., Littlefair, Stuart, Steeghs, Danny, Ulaczyk, Krzysztof, Chote, Paul, Lyman, Joseph, Galloway, Duncan K., Ackley, Kendall, and Mong, Yik Lun

Published
2020
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14. The Gravitational-wave Optical Transient Observer (GOTO)

Author

Marshall, Heather K., Spyromilio, Jason, Usuda, Tomonori, Dyer, Martin J., Steeghs, Danny, Galloway, Duncan K., Dhillon, Vik S., O'Brien, Paul, Ramsay, Gavin, Noysena, Kanthanakorn, Pallé, Enric, Kotak, Rubina, Breton, Rene, Nuttall, Laura, Pollacco, Don, Ulaczyk, Krzysztof, Lyman, Joseph, and Ackley, Kendall D.

Published
2020
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15. In search of genetic factors predisposing to familial hairy cell leukemia (HCL): exome-sequencing of four multiplex HCL pedigrees

Author

Pemov, Alexander, Pathak, Anand, Jones, Samantha J., Dewan, Ramita, Merberg, Jessica, Karra, Sirisha, Kim, Jung, Arons, Evgeny, Ravichandran, Sarangan, Luke, Brian T., Suman, Shalabh, Yeager, Meredith, Dyer, Martin J. S., Lynch, Henry T., Greene, Mark H., Caporaso, Neil E., Kreitman, Robert J., Goldin, Lynn R., Spinelli, John J., Brooks-Wilson, Angela, McMaster, Mary L., and Stewart, Douglas R.

Published
2020
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18. Dual dependence on BCL2 and MCL1 in T-cell prolymphocytic leukemia

Author

Smith, Victoria M., Lomas, Oliver, Constantine, Donna, Palmer, Lianne, Schuh, Anna H., Bruce, David, Gonchar, Oksana, Macip, Salvador, Jayne, Sandrine, Dyer, Martin J.S., and Eyre, Toby A.

Abstract

•Treatment of relapsed refractory T-PLL with venetoclax monotherapy results in only transient and minor clinical responses.•In vitro analyses pre- and postvenetoclax indicate dual dependence on BCL2 and MCL1; combined BCL2 and MCL1 inhibition are synergistic.

Published
2020
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19. Phase 1b study of venetoclax-obinutuzumab in previously untreated and relapsed/refractory chronic lymphocytic leukemia

Author

Flinn, Ian W., Gribben, John G., Dyer, Martin J.S., Wierda, William, Maris, Michael B., Furman, Richard R., Hillmen, Peter, Rogers, Kerry A., Iyer, Swaminathan Padmanabhan, Quillet-Mary, Anne, Ysebaert, Loic, Walter, Harriet S., Verdugo, Maria, Klein, Christian, Huang, Huang, Jiang, Yanwen, Lozanski, Gerard, Pignataro, Daniela Soriano, Humphrey, Kathryn, Mobasher, Mehrdad, and Kipps, Thomas J.

Abstract

This single-arm, open-label, phase 1b study evaluated the maximum tolerated dose (MTD) of venetoclax when given with obinutuzumab and its safety and tolerability in patients with relapsed/refractory (R/R) or previously untreated (first line [1L]) chronic lymphocytic leukemia (CLL). Venetoclax dose initially was escalated (100-400 mg) in a 3 + 3 design to define MTD combined with standard-dose obinutuzumab. Patients received venetoclax (schedule A) or obinutuzumab (schedule B) first to compare safety and determine dose/schedule for expansion. Venetoclax-obinutuzumab was administered for 6 cycles, followed by venetoclax monotherapy until disease progression (R/R) or fixed duration 1-year treatment (1L). Fifty R/R and 32 1L patients were enrolled. No dose-limiting toxicities were observed. Safety, including incidence of tumor lysis syndrome (TLS), did not differ between schedules (2 laboratory TLSs per schedule). Schedule B and a 400-mg dose of venetoclax were chosen for expansion. The most common grade 3-4 adverse event was neutropenia (R/R, 58% of patients; 1L, 53%). Rates of grade 3-4 infections were 29% (R/R) and 13% (1L); no fatal infections occurred in 1L. All infusion-related reactions were grade 1-2, except for 2 grade 3 events. No clinical TLS was observed. Overall best response rate was 95% in R/R (complete response [CR]/CR with incomplete marrow recovery [CRi], 37%) and 100% in 1L (CR/CRi, 78%) patients. Rate of undetectable (<10−4) minimal residual disease (uMRD) in peripheral blood for R/R and 1L patients, respectively, was 64% and 91% ≥3 months after last obinutuzumab dose. Venetoclax and obinutuzumab therapy had an acceptable safety profile and elicited durable responses and high rates of uMRD. This trial was registered at www.clinicaltrials.govas #NCT01685892.

Published
2019
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20. Phase 1b study of venetoclax-obinutuzumab in previously untreated and relapsed/refractory chronic lymphocytic leukemia

Author

Flinn, Ian W., Gribben, John G., Dyer, Martin J. S., Wierda, William, Maris, Michael B., Furman, Richard R., Hillmen, Peter, Rogers, Kerry A., Iyer, Swaminathan Padmanabhan, Quillet-Mary, Anne, Ysebaert, Loic, Walter, Harriet S., Verdugo, Maria, Klein, Christian, Huang, Huang, Jiang, Yanwen, Lozanski, Gerard, Pignataro, Daniela Soriano, Humphrey, Kathryn, Mobasher, Mehrdad, and Kipps, Thomas J.

Abstract

This single-arm, open-label, phase 1b study evaluated the maximum tolerated dose (MTD) of venetoclax when given with obinutuzumab and its safety and tolerability in patients with relapsed/refractory (R/R) or previously untreated (first line [1L]) chronic lymphocytic leukemia (CLL). Venetoclax dose initially was escalated (100-400 mg) in a 3?+?3 design to define MTD combined with standard-dose obinutuzumab. Patients received venetoclax (schedule A) or obinutuzumab (schedule B) first to compare safety and determine dose/schedule for expansion. Venetoclax-obinutuzumab was administered for 6 cycles, followed by venetoclax monotherapy until disease progression (R/R) or fixed duration 1-year treatment (1L). Fifty R/R and 32 1L patients were enrolled. No dose-limiting toxicities were observed. Safety, including incidence of tumor lysis syndrome (TLS), did not differ between schedules (2 laboratory TLSs per schedule). Schedule B and a 400-mg dose of venetoclax were chosen for expansion. The most common grade 3-4 adverse event was neutropenia (R/R, 58% of patients; 1L, 53%). Rates of grade 3-4 infections were 29% (R/R) and 13% (1L); no fatal infections occurred in 1L. All infusion-related reactions were grade 1-2, except for 2 grade 3 events. No clinical TLS was observed. Overall best response rate was 95% in R/R (complete response [CR]/CR with incomplete marrow recovery [CRi], 37%) and 100% in 1L (CR/CRi, 78%) patients. Rate of undetectable (<10-4) minimal residual disease (uMRD) in peripheral blood for R/R and 1L patients, respectively, was 64% and 91% =3 months after last obinutuzumab dose. Venetoclax and obinutuzumab therapy had an acceptable safety profile and elicited durable responses and high rates of uMRD. This trial was registered at www.clinicaltrials.gov as #NCT01685892.

Published
2019
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22. Ibrutinib efficacy and tolerability in patients with relapsed chronic lymphocytic leukemia following allogeneic HCT

Author

Ryan, Christine E., Sahaf, Bita, Logan, Aaron C., O’Brien, Susan, Byrd, John C., Hillmen, Peter, Brown, Jennifer R., Dyer, Martin J. S., Mato, Anthony R., Keating, Michael J., Jaglowski, Samantha, Clow, Fong, Rezvani, Andrew R., Styles, Lori, Coutre, Steven E., and Miklos, David B.

Abstract

Ibrutinib, a potent and irreversible small-molecule inhibitor of both Bruton’s tyrosine kinase and interleukin-2 inducible kinase (ITK), has been used to treat relapsed/refractory chronic lymphocytic leukemia (CLL) with prolongation of progression-free and overall survival. Here, we present 27 patients with relapsed CLL following allogeneic hematopoietic cell transplant (HCT) who subsequently received ibrutinib salvage therapy. Sixteen of these patients were part of multi-institutional clinical trials and achieved an overall response rate of 87.5%. An additional 11 patients were treated at Stanford University following US Food and Drug Administration approval of ibrutinib; 7 (64%) achieved a complete response, and 3 (27%) achieved a partial response. Of the 9 patients treated at Stanford who had mixed chimerism–associated CLL relapse, 4 (44%) converted to full donor chimerism following ibrutinib initiation, in association with disease response. Four of 11 (36%) patients evaluated by ClonoSeq achieved minimal residual disease negativity with CLL <1/10 000 white blood cells, which persisted even after ibrutinib was discontinued, in 1 case even after 26 months. None of the 27 patients developed graft-versus-host-disease (GVHD) following ibrutinib initiation. We postulate that ibrutinib augments the graft-versus-leukemia (GVL) benefit through a T-cell–mediated effect, most likely due to ITK inhibition. To investigate the immune modulatory effects of ibrutinib, we completed comprehensive immune phenotype characterization of peripheral B and T cells from treated patients. Our results show that ibrutinib selectively targets pre–germinal B cells and depletes Th2 helper cells. Furthermore, these effects persisted after drug discontinuation. In total, our results provide evidence that ibrutinib effectively augments GVL without causing GVHD.

Published
2016
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23. Ibrutinib efficacy and tolerability in patients with relapsed chronic lymphocytic leukemia following allogeneic HCT

Author

Ryan, Christine E., Sahaf, Bita, Logan, Aaron C., O'Brien, Susan, Byrd, John C., Hillmen, Peter, Brown, Jennifer R., Dyer, Martin J.S., Mato, Anthony R., Keating, Michael J., Jaglowski, Samantha, Clow, Fong, Rezvani, Andrew R., Styles, Lori, Coutre, Steven E., and Miklos, David B.

Abstract

Ibrutinib, a potent and irreversible small-molecule inhibitor of both Bruton's tyrosine kinase and interleukin-2 inducible kinase (ITK), has been used to treat relapsed/refractory chronic lymphocytic leukemia (CLL) with prolongation of progression-free and overall survival. Here, we present 27 patients with relapsed CLL following allogeneic hematopoietic cell transplant (HCT) who subsequently received ibrutinib salvage therapy. Sixteen of these patients were part of multi-institutional clinical trials and achieved an overall response rate of 87.5%. An additional 11 patients were treated at Stanford University following US Food and Drug Administration approval of ibrutinib; 7 (64%) achieved a complete response, and 3 (27%) achieved a partial response. Of the 9 patients treated at Stanford who had mixed chimerism–associated CLL relapse, 4 (44%) converted to full donor chimerism following ibrutinib initiation, in association with disease response. Four of 11 (36%) patients evaluated by ClonoSeq achieved minimal residual disease negativity with CLL <1/10 000 white blood cells, which persisted even after ibrutinib was discontinued, in 1 case even after 26 months. None of the 27 patients developed graft-versus-host-disease (GVHD) following ibrutinib initiation. We postulate that ibrutinib augments the graft-versus-leukemia (GVL) benefit through a T-cell–mediated effect, most likely due to ITK inhibition. To investigate the immune modulatory effects of ibrutinib, we completed comprehensive immune phenotype characterization of peripheral B and T cells from treated patients. Our results show that ibrutinib selectively targets pre–germinal B cells and depletes Th2 helper cells. Furthermore, these effects persisted after drug discontinuation. In total, our results provide evidence that ibrutinib effectively augments GVL without causing GVHD.

Published
2016
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25. Proteomic Analysis of Cell Surface Membrane Proteins in Leukemic Cells.

Author

Walker, John M., Coutts, Amanda S., Boyd, Robert S., Dyer, Martin J. S., and Cain, Kelvin

Abstract

Plasma membrane proteins play a key role in cellular processes such as migration, adhesion, and cell survival. The comprehensive annotation of the leukemic cell plasma membrane proteome allows the identification of proteins that may be involved in the pathogenesis of disease and may provide novel therapeutic targets. The identification of known adhesion molecules or novel proteins with similar attributes to adhesion molecules provides the starting point for the generation of hypothesis on the role of these proteins in adhesion processes. In order to identify these novel proteins, we have developed a proteomics methodology using purified plasma membranes prepared from human leukemic cells. [ABSTRACT FROM AUTHOR]

Published
2007
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26. Path Coupling Using Stopping Times.

Author

Liśkiewicz, Maciej, Reischuk, Rüdiger, Bordewich, Magnus, Dyer, Martin, and Karpinski, Marek

Abstract

We analyse the mixing time of Markov chains using path coupling with stopping times. We apply this approach to two hypergraph problems. We show that the Glauber dynamics for independent sets in a hypergraph mixes rapidly as long as the maximum degree Δ of a vertex and the minimum size m of an edge satisfy m ≥ 2Δ +1. We also state results that the Glauber dynamics for proper q-colourings of a hypergraph mixes rapidly if m ≥ 4 and q > Δ, and if m = 3 and q ≥1.65Δ. We give related results on the hardness of exact and approximate counting for both problems. [ABSTRACT FROM AUTHOR]

Published
2005
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27. Cloning of Immunoglobulin Chromosomal Translocations by Long-Distance Inverse Polymerase Chain Reaction.

Author

Illidge, Tim, Johnson, Peter W. M., Karran, E. Loraine, Sonoki, Takashi, and Dyer, Martin J. S.

Abstract

Many subtypes of B-cell malignancy are characterized by chromosomal translocations that target the immunoglobulin loci. Molecular cloning of such translocations continues to allow the identification of genes whose deregulated expression plays a pivotal role in the pathogenesis of B-cell malignancy. The clustering of breakpoints within the immunoglobulin loci has allowed the development of rapid and robust polymerase chain reaction methods for cloning. We discuss in this chapter the use of long-distance inverse polymerase chain reaction methods to clone immunoglobulin chromosomal translocation breakpoints from clinical material. These methods have been successfully applied to several other types of chromosomal translocation including those involving other genes such as BCL6, ETV6, and MYC. [ABSTRACT FROM AUTHOR]

Published
2005
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28. Listing Vertices of Simple Polyhedra Associated with Dual LI(2) Systems.

Author

Goos, Gerhard, Hartmanis, Juris, van Leeuwen, Jan, Calude, Cristian S., Dinneen, Michael J., Vajnovszki, Vincent, Abdullahi, Sammani D., Dyer, Martin E., and Proll, Les G.

Abstract

We present an O(nv) Basis Oriented Pivoting (BOP) algorithm for enumerating vertices of simple polyhedra associated with dual LI(2) systems. The algorithm is based on a characterisation of their graphical basis structures, whose set of edges are shown to consist of vertex-disjoint components that are either a tree or a subgraph with only one cycle. The algorithm generates vertices via operations on the basis graph, rather than by simplex transformations. [ABSTRACT FROM AUTHOR]

Published
2003
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29. Germ line mutations in shelterin complex genes are associated with familial chronic lymphocytic leukemia

Author

Speedy, Helen E., Kinnersley, Ben, Chubb, Daniel, Broderick, Peter, Law, Philip J., Litchfield, Kevin, Jayne, Sandrine, Dyer, Martin J. S., Dearden, Claire, Follows, George A., Catovsky, Daniel, and Houlston, Richard S.

Abstract

Chronic lymphocytic leukemia (CLL) can be familial; however, thus far no rare germ line disruptive alleles for CLL have been identified. We performed whole-exome sequencing of 66 CLL families, identifying 4 families where loss-of-function mutations in protection of telomeres 1 (POT1) co-segregated with CLL. The p.Tyr36Cys mutation is predicted to disrupt the interaction between POT1 and the telomeric overhang. The c.1164-1G>A splice-site, p.Gln358SerfsTer13 frameshift, and p.Gln376Arg missense mutations are likely to impact the interaction between POT1 and adrenocortical dysplasia homolog (ACD), which is a part of the telomere-capping shelterin complex. We also identified mutations in ACD (c.752-2A>C) and another shelterin component, telomeric repeat binding factor 2, interacting protein (p.Ala104Pro and p.Arg133Gln), in 3 CLL families. In a complementary analysis of 1083 cases and 5854 controls, the POT1 p.Gln376Arg variant, which has a global minor allele frequency of 0.0005, conferred a 3.61-fold increased risk of CLL (P = .009). This study further highlights telomere dysregulation as a key process in CLL development.

Published
2016
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30. Germ line mutations in shelterin complex genes are associated with familial chronic lymphocytic leukemia

Author

Speedy, Helen E., Kinnersley, Ben, Chubb, Daniel, Broderick, Peter, Law, Philip J., Litchfield, Kevin, Jayne, Sandrine, Dyer, Martin J.S., Dearden, Claire, Follows, George A., Catovsky, Daniel, and Houlston, Richard S.

Abstract

Chronic lymphocytic leukemia (CLL) can be familial; however, thus far no rare germ line disruptive alleles for CLL have been identified. We performed whole-exome sequencing of 66 CLL families, identifying 4 families where loss-of-function mutations in protection of telomeres 1 (POT1) co-segregated with CLL. The p.Tyr36Cys mutation is predicted to disrupt the interaction between POT1 and the telomeric overhang. The c.1164-1G>A splice-site, p.Gln358SerfsTer13 frameshift, and p.Gln376Arg missense mutations are likely to impact the interaction between POT1 and adrenocortical dysplasia homolog (ACD), which is a part of the telomere-capping shelterin complex. We also identified mutations in ACD(c.752-2A>C) and another shelterin component, telomeric repeat binding factor 2, interacting protein (p.Ala104Pro and p.Arg133Gln), in 3 CLL families. In a complementary analysis of 1083 cases and 5854 controls, the POT1p.Gln376Arg variant, which has a global minor allele frequency of 0.0005, conferred a 3.61-fold increased risk of CLL (P= .009). This study further highlights telomere dysregulation as a key process in CLL development.

Published
2016
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31. BRAF inhibition in hairy cell leukemia with low-dose vemurafenib

Author

Dietrich, Sascha, Pircher, Andreas, Endris, Volker, Peyrade, Frédéric, Wendtner, Clemens-Martin, Follows, George A., Hüllein, Jennifer, Jethwa, Alexander, Ellert, Elena, Walther, Tatjana, Liu, Xiyang, Dyer, Martin J. S., Elter, Thomas, Brummer, Tilman, Zeiser, Robert, Hermann, Michael, Herold, Michael, Weichert, Wilko, Dearden, Claire, Haferlach, Torsten, Seiffert, Martina, Hallek, Michael, von Kalle, Christof, Ho, Anthony D., Gaehler, Anita, Andrulis, Mindaugas, Steurer, Michael, and Zenz, Thorsten

Abstract

The activating mutation of the BRAF serine/threonine protein kinase (BRAF V600E) is the key driver mutation in hairy cell leukemia (HCL), suggesting opportunities for therapeutic targeting. We analyzed the course of 21 HCL patients treated with vemurafenib outside of trials with individual dosing regimens (240-1920 mg/d; median treatment duration, 90 days). Vemurafenib treatment improved blood counts in all patients, with platelets, neutrophils, and hemoglobin recovering within 28, 43, and 55 days (median), respectively. Complete remission was achieved in 40% (6/15 of evaluable patients) and median event-free survival was 17 months. Response rate and kinetics of response were independent of vemurafenib dosing. Retreatment with vemurafenib led to similar response patterns (n = 6). Pharmacodynamic analysis of BRAF V600E downstream targets showed that vemurafenib (480 mg/d) completely abrogated extracellular signal-regulated kinase phosphorylation of hairy cells in vivo. Typical side effects also occurred at low dosing regimens. We observed the development of acute myeloid lymphoma (AML) subtype M6 in 1 patient, and the course suggested disease acceleration triggered by vemurafenib. The phosphatidylinositol 3-kinase hotspot mutation (E545K) was identified in the AML clone, providing a potential novel mechanism for paradoxical BRAF activation. These data provide proof of dependence of HCL on active BRAF signaling. We provide evidence that antitumor and side effects are observed with 480 mg vemurafenib, suggesting that dosing regimens in BRAF-driven cancers could warrant reassessment in trials with implications for cost of cancer care.

Published
2016
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32. BRAF inhibition in hairy cell leukemia with low-dose vemurafenib

Author

Dietrich, Sascha, Pircher, Andreas, Endris, Volker, Peyrade, Frédéric, Wendtner, Clemens-Martin, Follows, George A., Hüllein, Jennifer, Jethwa, Alexander, Ellert, Elena, Walther, Tatjana, Liu, Xiyang, Dyer, Martin J.S., Elter, Thomas, Brummer, Tilman, Zeiser, Robert, Hermann, Michael, Herold, Michael, Weichert, Wilko, Dearden, Claire, Haferlach, Torsten, Seiffert, Martina, Hallek, Michael, von Kalle, Christof, Ho, Anthony D., Gaehler, Anita, Andrulis, Mindaugas, Steurer, Michael, and Zenz, Thorsten

Abstract

The activating mutation of the BRAF serine/threonine protein kinase (BRAF V600E) is the key driver mutation in hairy cell leukemia (HCL), suggesting opportunities for therapeutic targeting. We analyzed the course of 21 HCL patients treated with vemurafenib outside of trials with individual dosing regimens (240-1920 mg/d; median treatment duration, 90 days). Vemurafenib treatment improved blood counts in all patients, with platelets, neutrophils, and hemoglobin recovering within 28, 43, and 55 days (median), respectively. Complete remission was achieved in 40% (6/15 of evaluable patients) and median event-free survival was 17 months. Response rate and kinetics of response were independent of vemurafenib dosing. Retreatment with vemurafenib led to similar response patterns (n = 6). Pharmacodynamic analysis of BRAF V600E downstream targets showed that vemurafenib (480 mg/d) completely abrogated extracellular signal-regulated kinase phosphorylation of hairy cells in vivo. Typical side effects also occurred at low dosing regimens. We observed the development of acute myeloid lymphoma (AML) subtype M6 in 1 patient, and the course suggested disease acceleration triggered by vemurafenib. The phosphatidylinositol 3-kinase hotspot mutation (E545K) was identified in the AML clone, providing a potential novel mechanism for paradoxical BRAF activation. These data provide proof of dependence of HCL on active BRAF signaling. We provide evidence that antitumor and side effects are observed with 480 mg vemurafenib, suggesting that dosing regimens in BRAF-driven cancers could warrant reassessment in trials with implications for cost of cancer care.

Published
2016
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33. A phase 1 clinical trial of the selective BTK inhibitor ONO/GS-4059 in relapsed and refractory mature B-cell malignancies

Author

Walter, Harriet S., Rule, Simon A., Dyer, Martin J. S., Karlin, Lionel, Jones, Ceri, Cazin, Bruno, Quittet, Philippe, Shah, Nimish, Hutchinson, Claire V., Honda, Hideyuki, Duffy, Kevin, Birkett, Joseph, Jamieson, Virginia, Courtenay-Luck, Nigel, Yoshizawa, Toshio, Sharpe, John, Ohno, Tomoya, Abe, Shinichiro, Nishimura, Akihisa, Cartron, Guillaume, Morschhauser, Franck, Fegan, Christopher, and Salles, Gilles

Abstract

We report the results of a multicenter phase 1 dose-escalation study of the selective Bruton tyrosine kinase (BTK) inhibitor ONO/GS-4059 in 90 patients with relapsed/refractory B-cell malignancies. There were 9 dose-escalation cohorts ranging from 20 mg to 600 mg once daily with twice-daily regimens of 240 mg and 300 mg. Twenty-four of 25 evaluable chronic lymphocytic leukemia (CLL) patients (96%) responded to ONO/GS-4059, with a median treatment duration of 80 weeks; 21 CLL patients remain on treatment. Lymph node responses were rapid and associated with a concurrent lymphocytosis. Eleven of 12 evaluable patients with mantle cell lymphoma (92%) responded (median treatment duration, 40 weeks). Eleven of 31 non–germinal center B-cell diffuse large B-cell lymphoma patients (35%) responded but median treatment duration was 12 weeks due to development of progressive disease. ONO/GS-4059 was very well tolerated with 75% of adverse events (AEs) being Common Toxicity Criteria for Adverse Events version 4.0 grade 1 or grade 2. Grade 3/4 AEs were mainly hematologic and recovered spontaneously during therapy. One CLL patient experienced a grade 3 treatment-related bleeding event (spontaneous muscle hematoma) but no clinically significant diarrhea, cardiac dysrhythmias, or arthralgia were observed. No maximal tolerated dose (MTD) was reached in the CLL cohort. In the non-Hodgkin lymphoma cohort, 4 patients developed a dose-limiting toxicity, yielding an MTD of 480 mg once daily. ONO/GS-4059 has significant activity in relapsed/refractory B-cell malignancies without major drug-related toxicity. The selectivity of ONO/GS-4059 should confer advantages in combination therapies. This trial was registered at www.clinicaltrials.gov as #NCT01659255.

Published
2016
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34. A phase 1 clinical trial of the selective BTK inhibitor ONO/GS-4059 in relapsed and refractory mature B-cell malignancies

Author

Walter, Harriet S., Rule, Simon A., Dyer, Martin J.S., Karlin, Lionel, Jones, Ceri, Cazin, Bruno, Quittet, Philippe, Shah, Nimish, Hutchinson, Claire V., Honda, Hideyuki, Duffy, Kevin, Birkett, Joseph, Jamieson, Virginia, Courtenay-Luck, Nigel, Yoshizawa, Toshio, Sharpe, John, Ohno, Tomoya, Abe, Shinichiro, Nishimura, Akihisa, Cartron, Guillaume, Morschhauser, Franck, Fegan, Christopher, and Salles, Gilles

Abstract

We report the results of a multicenter phase 1 dose-escalation study of the selective Bruton tyrosine kinase (BTK) inhibitor ONO/GS-4059 in 90 patients with relapsed/refractory B-cell malignancies. There were 9 dose-escalation cohorts ranging from 20 mg to 600 mg once daily with twice-daily regimens of 240 mg and 300 mg. Twenty-four of 25 evaluable chronic lymphocytic leukemia (CLL) patients (96%) responded to ONO/GS-4059, with a median treatment duration of 80 weeks; 21 CLL patients remain on treatment. Lymph node responses were rapid and associated with a concurrent lymphocytosis. Eleven of 12 evaluable patients with mantle cell lymphoma (92%) responded (median treatment duration, 40 weeks). Eleven of 31 non–germinal center B-cell diffuse large B-cell lymphoma patients (35%) responded but median treatment duration was 12 weeks due to development of progressive disease. ONO/GS-4059 was very well tolerated with 75% of adverse events (AEs) being Common Toxicity Criteria for Adverse Events version 4.0 grade 1 or grade 2. Grade 3/4 AEs were mainly hematologic and recovered spontaneously during therapy. One CLL patient experienced a grade 3 treatment-related bleeding event (spontaneous muscle hematoma) but no clinically significant diarrhea, cardiac dysrhythmias, or arthralgia were observed. No maximal tolerated dose (MTD) was reached in the CLL cohort. In the non-Hodgkin lymphoma cohort, 4 patients developed a dose-limiting toxicity, yielding an MTD of 480 mg once daily. ONO/GS-4059 has significant activity in relapsed/refractory B-cell malignancies without major drug-related toxicity. The selectivity of ONO/GS-4059 should confer advantages in combination therapies. This trial was registered at www.clinicaltrials.govas #NCT01659255.

Published
2016
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35. Recurrent CDKN1B(p27) mutations in hairy cell leukemia

Author

Dietrich, Sascha, Hüllein, Jennifer, Lee, Stanley Chun-Wei, Hutter, Barbara, Gonzalez, David, Jayne, Sandrine, Dyer, Martin J.S., Oleś, Małgorzata, Else, Monica, Liu, Xiyang, Słabicki, Mikołaj, Wu, Bian, Troussard, Xavier, Dürig, Jan, Andrulis, Mindaugas, Dearden, Claire, von Kalle, Christof, Granzow, Martin, Jauch, Anna, Fröhling, Stefan, Huber, Wolfgang, Meggendorfer, Manja, Haferlach, Torsten, Ho, Anthony D., Richter, Daniela, Brors, Benedikt, Glimm, Hanno, Matutes, Estella, Abdel Wahab, Omar, and Zenz, Thorsten

Abstract

Hairy cell leukemia (HCL) is marked by near 100% mutational frequency of BRAFV600E mutations. Recurrent cooperating genetic events that may contribute to HCL pathogenesis or affect the clinical course of HCL are currently not described. Therefore, we performed whole exome sequencing to explore the mutational landscape of purine analog refractory HCL. In addition to the disease-defining BRAFV600E mutations, we identified mutations in EZH2, ARID1A, and recurrent inactivating mutations of the cell cycle inhibitor CDKN1B(p27). Targeted deep sequencing of CDKN1Bin a larger cohort of HCL patients identify deleterious CDKN1B mutations in 16% of patients with HCL (n = 13 of 81). In 11 of 13 patients the CDKN1Bmutation was clonal, implying an early role of CDKN1Bmutations in the pathogenesis of HCL. CDKN1Bmutations were not found to impact clinical characteristics or outcome in this cohort. These data identify HCL as having the highest frequency of CDKN1Bmutations among cancers and identify CDNK1Bas the second most common mutated gene in HCL. Moreover, given the known function of CDNK1B, these data suggest a novel role for alterations in regulation of cell cycle and senescence in HCL with CDKN1Bmutations.

Published
2015
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36. Recurrent CDKN1B (p27) mutations in hairy cell leukemia

Author

Dietrich, Sascha, Hüllein, Jennifer, Lee, Stanley Chun-Wei, Hutter, Barbara, Gonzalez, David, Jayne, Sandrine, Dyer, Martin J. S., Oleś, Małgorzata, Else, Monica, Liu, Xiyang, Słabicki, Mikołaj, Wu, Bian, Troussard, Xavier, Dürig, Jan, Andrulis, Mindaugas, Dearden, Claire, von Kalle, Christof, Granzow, Martin, Jauch, Anna, Fröhling, Stefan, Huber, Wolfgang, Meggendorfer, Manja, Haferlach, Torsten, Ho, Anthony D., Richter, Daniela, Brors, Benedikt, Glimm, Hanno, Matutes, Estella, Abdel Wahab, Omar, and Zenz, Thorsten

Abstract

Hairy cell leukemia (HCL) is marked by near 100% mutational frequency of BRAFV600E mutations. Recurrent cooperating genetic events that may contribute to HCL pathogenesis or affect the clinical course of HCL are currently not described. Therefore, we performed whole exome sequencing to explore the mutational landscape of purine analog refractory HCL. In addition to the disease-defining BRAFV600E mutations, we identified mutations in EZH2, ARID1A, and recurrent inactivating mutations of the cell cycle inhibitor CDKN1B (p27). Targeted deep sequencing of CDKN1B in a larger cohort of HCL patients identify deleterious CDKN1B mutations in 16% of patients with HCL (n = 13 of 81). In 11 of 13 patients the CDKN1B mutation was clonal, implying an early role of CDKN1B mutations in the pathogenesis of HCL. CDKN1B mutations were not found to impact clinical characteristics or outcome in this cohort. These data identify HCL as having the highest frequency of CDKN1B mutations among cancers and identify CDNK1B as the second most common mutated gene in HCL. Moreover, given the known function of CDNK1B, these data suggest a novel role for alterations in regulation of cell cycle and senescence in HCL with CDKN1B mutations.

Published
2015
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38. A genuinely polynomial-time algorithm for sampling two-rowed contingency tables.

Author

Goos, Gerhard, Hartmanis, Juris, Leeuwen, Jan, Larsen, Kim G., Skyum, Sven, Winskel, Glynn, Dyer, Martin, and Greenhill, Catherine

Abstract

In this paper a Markov chain for contingency tallies with two lows is defined. The chain is shown to be rapidly mixing using the path coupling method. The mixing time of the chain is quadratic in the number of columns and linear in the logarithm of the table sum. Two extensions of the new chain are discussed: one for three-rowed contingency tables and one for m-rowed contingency tables. We show that, unfortunately, it is not possible to prove rapid mixing for these chains by simply extending the path coupling approach used in the two-rowed case. [ABSTRACT FROM AUTHOR]

Published
1998
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41. Path coupling without contraction.

Author

Bordewich, Magnus and Dyer, Martin

Subjects
MARKOV processes, COUPLINGS (Gearing), STOCHASTIC processes, ALGORITHMS
Abstract

Abstract: Path coupling is a useful technique for simplifying the analysis of a coupling of a Markov chain. Rather than defining and analysing the coupling on every pair in , where Ω is the state space of the Markov chain, analysis is done on a smaller set . If the coefficient of contraction β is strictly less than one, no further analysis is needed in order to show rapid mixing. However, if then analysis (of the variance) is still required for all pairs in . In this paper we present a new approach which shows rapid mixing in the case with a further condition which only needs to be checked for pairs in S, greatly simplifying the work involved. We also present a technique applicable when and our condition is not met. [Copyright &y& Elsevier]

Published
2007
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45. t(X;14)(p11;q32) in MALT lymphoma involving GPR34 reveals a role for GPR34 in tumor cell growth

Author

Ansell, Stephen M., Akasaka, Takashi, McPhail, Ellen, Manske, Michelle, Braggio, Esteban, Price-Troska, Tammy, Ziesmer, Steven, Secreto, Frank, Fonseca, Rafael, Gupta, Mamta, Law, Mark, Witzig, Thomas E., Dyer, Martin J. S., Dogan, Ahmet, Cerhan, James R., and Novak, Anne J.

Abstract

Genetic aberrations, including trisomies 3 and 18, and well-defined IGH translocations, have been described in marginal zone lymphomas (MZLs); however, these known genetic events are present in only a subset of cases. Here, we report the cloning of an IGH translocation partner on chromosome X, t(X;14)(p11.4;q32) that deregulates expression of an poorly characterized orphan G-protein–coupled receptor, GPR34. Elevated GPR34 gene expression was detected independent of the translocation in multiple subtypes of non-Hodgkin lymphoma and distinguished a unique molecular subtype of MZL. Increased expression of GPR34 was also detected in tissue from brain tumors and surface expression of GPR34 was detected on human MZL tumor cells and normal immune cells. Overexpression of GPR34 in lymphoma and HeLa cells resulted in phosphorylation of ERK, PKC, and CREB; induced CRE, AP1, and NF-κB–mediated gene transcription; and increased cell proliferation. In summary, these results are the first to identify a role for a GPR34 in lymphoma cell growth, provide insight into GPR34-mediated signaling, identify a genetically unique subset of MZLs that express high levels of GPR34, and suggest that MEK inhibitors may be useful for treatment of GPR34-expressing tumors.

Published
2012
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46. t(X;14)(p11;q32) in MALT lymphoma involving GPR34reveals a role for GPR34 in tumor cell growth

Author

Ansell, Stephen M., Akasaka, Takashi, McPhail, Ellen, Manske, Michelle, Braggio, Esteban, Price-Troska, Tammy, Ziesmer, Steven, Secreto, Frank, Fonseca, Rafael, Gupta, Mamta, Law, Mark, Witzig, Thomas E., Dyer, Martin J.S., Dogan, Ahmet, Cerhan, James R., and Novak, Anne J.

Abstract

Genetic aberrations, including trisomies 3 and 18, and well-defined IGHtranslocations, have been described in marginal zone lymphomas (MZLs); however, these known genetic events are present in only a subset of cases. Here, we report the cloning of an IGHtranslocation partner on chromosome X, t(X;14)(p11.4;q32) that deregulates expression of an poorly characterized orphan G-protein–coupled receptor, GPR34. Elevated GPR34 gene expression was detected independent of the translocation in multiple subtypes of non-Hodgkin lymphoma and distinguished a unique molecular subtype of MZL. Increased expression of GPR34 was also detected in tissue from brain tumors and surface expression of GPR34 was detected on human MZL tumor cells and normal immune cells. Overexpression of GPR34 in lymphoma and HeLa cells resulted in phosphorylation of ERK, PKC, and CREB; induced CRE, AP1, and NF-κB–mediated gene transcription; and increased cell proliferation. In summary, these results are the first to identify a role for a GPR34 in lymphoma cell growth, provide insight into GPR34-mediated signaling, identify a genetically unique subset of MZLs that express high levels of GPR34, and suggest that MEK inhibitors may be useful for treatment of GPR34-expressing tumors.

Published
2012
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47. Safety and efficacy of ofatumumab in patients with fludarabine and alemtuzumab refractory chronic lymphocytic leukaemia

Author

Dyer, Martin

Abstract

There are now many therapeutic CD20 monoclonal antibodies undergoing clinical trials for B-cell malignancy and autoimmune conditions; which is optimal for cancer therapy is not clear. The novel human IgG1 CD20 monoclonal antibody ofatumumab has shown significant activity in difficult to treat patients with chronic lymphocytic leukemia, namely those resistant or refractory to fludarabine and alemtuzumab and has now been licensed for this uncommon indication. This brief review summarizes the clinical data obtained with ofatumumab in CLL in terms of both efficacy and toxicity.

Published
2012
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48. Common variation at 6p21.31 (BAK1) influences the risk of chronic lymphocytic leukemia

Author

Slager, Susan L., Skibola, Christine F., Di Bernardo, Maria Chiara, Conde, Lucia, Broderick, Peter, McDonnell, Shannon K., Goldin, Lynn R., Croft, Naomi, Holroyd, Amy, Harris, Shelley, Riby, Jacques, Serie, Daniel J., Kay, Neil E., Call, Timothy G., Bracci, Paige M., Halperin, Eran, Lanasa, Mark C., Cunningham, Julie M., Leis, Jose F., Morrison, Vicki A., Spector, Logan G., Vachon, Celine M., Shanafelt, Tait D., Strom, Sara S., Camp, Nicola J., Weinberg, J. Brice, Matutes, Estella, Caporaso, Neil E., Wade, Rachel, Dyer, Martin J. S., Dearden, Claire, Cerhan, James R., Catovsky, Daniel, and Houlston, Richard S.

Abstract

We performed a meta-analysis of 3 genome-wide association studies to identify additional common variants influencing chronic lymphocytic leukemia (CLL) risk. The discovery phase was composed of genome-wide association study data from 1121 cases and 3745 controls. Replication analysis was performed in 861 cases and 2033 controls. We identified a novel CLL risk locus at 6p21.33 (rs210142; intronic to the BAK1 gene, BCL2 antagonist killer 1; P = 9.47 × 10−16). A strong relationship between risk genotype and reduced BAK1 expression was shown in lymphoblastoid cell lines. This finding provides additional support for polygenic inheritance to CLL and provides further insight into the biologic basis of disease development.

Published
2012
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49. Common variation at 6p21.31 (BAK1) influences the risk of chronic lymphocytic leukemia

Author

Slager, Susan L., Skibola, Christine F., Di Bernardo, Maria Chiara, Conde, Lucia, Broderick, Peter, McDonnell, Shannon K., Goldin, Lynn R., Croft, Naomi, Holroyd, Amy, Harris, Shelley, Riby, Jacques, Serie, Daniel J., Kay, Neil E., Call, Timothy G., Bracci, Paige M., Halperin, Eran, Lanasa, Mark C., Cunningham, Julie M., Leis, Jose F., Morrison, Vicki A., Spector, Logan G., Vachon, Celine M., Shanafelt, Tait D., Strom, Sara S., Camp, Nicola J., Weinberg, J. Brice, Matutes, Estella, Caporaso, Neil E., Wade, Rachel, Dyer, Martin J.S., Dearden, Claire, Cerhan, James R., Catovsky, Daniel, and Houlston, Richard S.

Abstract

We performed a meta-analysis of 3 genome-wide association studies to identify additional common variants influencing chronic lymphocytic leukemia (CLL) risk. The discovery phase was composed of genome-wide association study data from 1121 cases and 3745 controls. Replication analysis was performed in 861 cases and 2033 controls. We identified a novel CLL risk locus at 6p21.33 (rs210142; intronic to the BAK1gene, BCL2 antagonist killer 1; P= 9.47 × 10−16). A strong relationship between risk genotype and reduced BAK1expression was shown in lymphoblastoid cell lines. This finding provides additional support for polygenic inheritance to CLL and provides further insight into the biologic basis of disease development.

Published
2012
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50. BCL2/BCL-XL inhibition induces apoptosis, disrupts cellular calcium homeostasis, and prevents platelet activation

Author

Vogler, Meike, Hamali, Hassan A., Sun, Xiao-Ming, Bampton, Edward T. W., Dinsdale, David, Snowden, Roger T., Dyer, Martin J. S., Goodall, Alison H., and Cohen, Gerald M.

Abstract

Apoptosis in megakaryocytes results in the formation of platelets. The role of apoptotic pathways in platelet turnover and in the apoptotic-like changes seen after platelet activation is poorly understood. ABT-263 (Navitoclax), a specific inhibitor of antiapoptotic BCL2 proteins, which is currently being evaluated in clinical trials for the treatment of leukemia and other malignancies, induces a dose-limiting thrombocytopenia. In this study, the relationship between BCL2/BCL-XL inhibition, apoptosis, and platelet activation was investigated. Exposure to ABT-263 induced apoptosis but repressed platelet activation by physiologic agonists. Notably, ABT-263 induced an immediate calcium response in platelets and the depletion of intracellular calcium stores, indicating that on BCL2/BCL-XL inhibition platelet activation is abrogated because of a diminished calcium signaling. By comparing the effects of ABT-263 and its analog ABT-737 on platelets and leukemia cells from the same donor, we show, for the first time, that these BCL2/BCL-XL inhibitors do not offer any selective toxicity but induce apoptosis at similar concentrations in leukemia cells and platelets. However, reticulated platelets are less sensitive to apoptosis, supporting the hypothesis that treatment with ABT-263 induces a selective loss of older platelets and providing an explanation for the transient thrombocytopenia observed on ABT-263 treatment.

Published
2011
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