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11 results on '"Winston, Drew J"'

1. Utilization of whole genome sequencing for resolution of discrepant Mycobacterium tuberculosis drug susceptibility results: A case report.

Author

Realegeno, Susan, Realegeno, Susan, Adeyiga, Oladunni, Winston, Drew J, Beaird, Omer E, Garner, Omai B, Yang, Shangxin, Realegeno, Susan, Realegeno, Susan, Adeyiga, Oladunni, Winston, Drew J, Beaird, Omer E, Garner, Omai B, and Yang, Shangxin

Abstract

A 44-year-old woman undergoing therapy for acute promyelocytic leukemia (APL) developed disseminated tuberculosis. Mycobacterium tuberculosis (TB) was isolated from the blood and sputum. Initial drug susceptibility testing (DST) of the blood isolate revealed resistance to isoniazid and ethambutol but the sputum isolate showed no resistance. Due to drug resistance concerns, the patient was treated with multiple second and third-line drugs, and suffered from drug side effects. To further investigate the DST discrepancies, whole genome sequencing (WGS) was performed on both isolates. No known resistance mutations to first line or second line drugs were identified in either isolate, which was confirmed by additional susceptibility testing performed by a different reference laboratory and the California Department of Public Health (CDPH) laboratory. Treatment was reduced to a simpler and less toxic regimen due to these investigations. WGS is shown to be a valuable tool for resolving discordant phenotypic DST results of TB isolates and has the potential to provide accurate and timely results guiding appropriate therapy in the clinical setting.

Published
2021

2. Increased Incidence of Nocardial Infections in an Era of Atovaquone Prophylaxis in Allogeneic Hematopoietic Stem Cell Transplant Recipients.

Author

Molina, Alfonso, Molina, Alfonso, Winston, Drew J, Pan, Darren, Schiller, Gary J, Molina, Alfonso, Molina, Alfonso, Winston, Drew J, Pan, Darren, and Schiller, Gary J

Abstract

Nocardial infections have been rare after allogeneic hematopoietic stem cell transplantation (HSCT). We report 10 recent cases of late-onset nocardiosis (median time of onset of 508 days after transplantation) primarily in patients on high doses of corticosteroids for graft-versus-host disease. All 10 patients had pulmonary infection caused by Nocardia species susceptible to trimethoprim-sulfamethoxazole (TMP-SMX). At time of diagnosis 8 of 10 patients were not receiving TMP-SMX for prophylaxis of Pneumocystis jiroveci pneumonia (PJP; 7 on atovaquone, 1 on i.v. pentamidine). After the initiation of atovaquone prophylaxis for PJP in place of TMP-SMX for many UCLA allogeneic HSCT patients in 2012, 9 cases of nocardiosis occurred in 411 patients (2.2%) over the next 6 years (2012 to 2017) compared with only 1 case in 575 patients (0.17%) during the previous 12 years (2000 to 2011). Although there were no deaths directly related to nocardial infection treated primarily with TMP-SMX, overall mortality in this group of patients was 40%. Based on this experience, the use of atovaquone for PJP prophylaxis in place of TMP-SMX may be associated with an increased risk for previously rare nocardial infections after allogeneic HSCT.

Published
2018

3. Inactivated varicella zoster vaccine in autologous haemopoietic stem-cell transplant recipients: an international, multicentre, randomised, double-blind, placebo-controlled trial

Author

Winston, Drew J., Mullane, Kathleen M., Cornely, Oliver A., Boeckh, Michael J., Brown, Janice Wes, Pergam, Steven A., Trociukas, Igoris, Zak, Pavel, Craig, Michael D., Papanicolaou, Genovefa A., Velez, Juan D., Panse, Jens, Hurtado, Kimberly, Fernsler, Doreen A., Stek, Jon E., Pang, Lei, Su, Shu-Chih, Zhao, Yanli, Chan, Ivan S. F., Kaplan, Susan S., Parrino, Janie, Lee, Ingi, Popmihajlov, Zoran, Annunziato, Paula W., Arvin, Ann, Winston, Drew J., Mullane, Kathleen M., Cornely, Oliver A., Boeckh, Michael J., Brown, Janice Wes, Pergam, Steven A., Trociukas, Igoris, Zak, Pavel, Craig, Michael D., Papanicolaou, Genovefa A., Velez, Juan D., Panse, Jens, Hurtado, Kimberly, Fernsler, Doreen A., Stek, Jon E., Pang, Lei, Su, Shu-Chih, Zhao, Yanli, Chan, Ivan S. F., Kaplan, Susan S., Parrino, Janie, Lee, Ingi, Popmihajlov, Zoran, Annunziato, Paula W., and Arvin, Ann

Abstract

Background Recipients of autologous haemopoietic stem-cell transplants (auto-HSCT) have an increased risk of herpes zoster and herpes zoster-related complications. The aim of this study was to establish the efficacy and safety of an inactivated varicella zoster vaccine for the prevention of herpes zoster after auto-HSCT. Methods In this randomised, double-blind, placebo-controlled phase 3 trial, participants were recruited from 135 medical centres (ie, stem-cell transplant centres and hospitals) in North America, South America, Europe, and Asia. Patients were eligible if they were aged 18 years or older, scheduled to receive an auto-HSCT within 60 days of enrolment, and had a history of varicella infection or were seropositive for antibodies to varicella zoster virus, or both. Exclusion criteria included a history of herpes zoster within the previous year of enrolment, and intended antiviral prophylaxis for longer than 6 months after transplantation. Participants were randomly assigned according to a central randomisation schedule generated by the trial statistician, to receive either the inactivated-virus vaccine from one of three consistency lots, a high-antigen lot, or placebo, stratified by age (< 50 vs >= 50 years) and intended duration of antiviral prophylaxis after transplantation (<= 3 months vs > 3 to <= 6 months). Participants, investigators, trial staff, and the funder's clinical and laboratory personnel were masked to group assignment. Participants were given four doses of inactivated vaccine or placebo, with the first dose 5-60 days before auto-HSCT, and the second, third, and fourth doses at about 30, 60, and 90 days after transplantation. The primary efficacy endpoint was the incidence of herpes zoster, confirmed by PCR or adjudication by a masked clinical committee, or both, assessed in all participants randomly assigned to the vaccine consistency lot group or placebo group who received at least one dose of vaccine and had auto-HSCT. Safety was asses

Published
2018

4. Increased Incidence of Nocardial Infections in an Era of Atovaquone Prophylaxis in Allogeneic Hematopoietic Stem Cell Transplant Recipients.

Author

Molina, Alfonso, Molina, Alfonso, Winston, Drew J, Pan, Darren, Schiller, Gary J, Molina, Alfonso, Molina, Alfonso, Winston, Drew J, Pan, Darren, and Schiller, Gary J

Abstract

Nocardial infections have been rare after allogeneic hematopoietic stem cell transplantation (HSCT). We report 10 recent cases of late-onset nocardiosis (median time of onset of 508 days after transplantation) primarily in patients on high doses of corticosteroids for graft-versus-host disease. All 10 patients had pulmonary infection caused by Nocardia species susceptible to trimethoprim-sulfamethoxazole (TMP-SMX). At time of diagnosis 8 of 10 patients were not receiving TMP-SMX for prophylaxis of Pneumocystis jiroveci pneumonia (PJP; 7 on atovaquone, 1 on i.v. pentamidine). After the initiation of atovaquone prophylaxis for PJP in place of TMP-SMX for many UCLA allogeneic HSCT patients in 2012, 9 cases of nocardiosis occurred in 411 patients (2.2%) over the next 6 years (2012 to 2017) compared with only 1 case in 575 patients (0.17%) during the previous 12 years (2000 to 2011). Although there were no deaths directly related to nocardial infection treated primarily with TMP-SMX, overall mortality in this group of patients was 40%. Based on this experience, the use of atovaquone for PJP prophylaxis in place of TMP-SMX may be associated with an increased risk for previously rare nocardial infections after allogeneic HSCT.

Published
2018

5. Inactivated varicella zoster vaccine in autologous haemopoietic stem-cell transplant recipients: an international, multicentre, randomised, double-blind, placebo-controlled trial

Author

Winston, Drew J., Mullane, Kathleen M., Cornely, Oliver A., Boeckh, Michael J., Brown, Janice Wes, Pergam, Steven A., Trociukas, Igoris, Zak, Pavel, Craig, Michael D., Papanicolaou, Genovefa A., Velez, Juan D., Panse, Jens, Hurtado, Kimberly, Fernsler, Doreen A., Stek, Jon E., Pang, Lei, Su, Shu-Chih, Zhao, Yanli, Chan, Ivan S. F., Kaplan, Susan S., Parrino, Janie, Lee, Ingi, Popmihajlov, Zoran, Annunziato, Paula W., Arvin, Ann, Winston, Drew J., Mullane, Kathleen M., Cornely, Oliver A., Boeckh, Michael J., Brown, Janice Wes, Pergam, Steven A., Trociukas, Igoris, Zak, Pavel, Craig, Michael D., Papanicolaou, Genovefa A., Velez, Juan D., Panse, Jens, Hurtado, Kimberly, Fernsler, Doreen A., Stek, Jon E., Pang, Lei, Su, Shu-Chih, Zhao, Yanli, Chan, Ivan S. F., Kaplan, Susan S., Parrino, Janie, Lee, Ingi, Popmihajlov, Zoran, Annunziato, Paula W., and Arvin, Ann

Abstract

Background Recipients of autologous haemopoietic stem-cell transplants (auto-HSCT) have an increased risk of herpes zoster and herpes zoster-related complications. The aim of this study was to establish the efficacy and safety of an inactivated varicella zoster vaccine for the prevention of herpes zoster after auto-HSCT. Methods In this randomised, double-blind, placebo-controlled phase 3 trial, participants were recruited from 135 medical centres (ie, stem-cell transplant centres and hospitals) in North America, South America, Europe, and Asia. Patients were eligible if they were aged 18 years or older, scheduled to receive an auto-HSCT within 60 days of enrolment, and had a history of varicella infection or were seropositive for antibodies to varicella zoster virus, or both. Exclusion criteria included a history of herpes zoster within the previous year of enrolment, and intended antiviral prophylaxis for longer than 6 months after transplantation. Participants were randomly assigned according to a central randomisation schedule generated by the trial statistician, to receive either the inactivated-virus vaccine from one of three consistency lots, a high-antigen lot, or placebo, stratified by age (< 50 vs >= 50 years) and intended duration of antiviral prophylaxis after transplantation (<= 3 months vs > 3 to <= 6 months). Participants, investigators, trial staff, and the funder's clinical and laboratory personnel were masked to group assignment. Participants were given four doses of inactivated vaccine or placebo, with the first dose 5-60 days before auto-HSCT, and the second, third, and fourth doses at about 30, 60, and 90 days after transplantation. The primary efficacy endpoint was the incidence of herpes zoster, confirmed by PCR or adjudication by a masked clinical committee, or both, assessed in all participants randomly assigned to the vaccine consistency lot group or placebo group who received at least one dose of vaccine and had auto-HSCT. Safety was asses

Published
2018

8. Donor-derived West Nile virus infection in solid organ transplant recipients: report of four additional cases and review of clinical, diagnostic, and therapeutic features.

Author

Winston, Drew J, Winston, Drew J, Vikram, Holenarasipur R, Rabe, Ingrid B, Dhillon, Gundeep, Mulligan, David, Hong, Johnny C, Busuttil, Ronald W, Nowicki, Marek J, Mone, Thomas, Civen, Rachel, Tecle, Selam A, Trivedi, Kavita K, Hocevar, Susan N, West Nile Virus Transplant-Associated Transmission Investigation Team, Winston, Drew J, Winston, Drew J, Vikram, Holenarasipur R, Rabe, Ingrid B, Dhillon, Gundeep, Mulligan, David, Hong, Johnny C, Busuttil, Ronald W, Nowicki, Marek J, Mone, Thomas, Civen, Rachel, Tecle, Selam A, Trivedi, Kavita K, Hocevar, Susan N, and West Nile Virus Transplant-Associated Transmission Investigation Team

Abstract

We describe four solid-organ transplant recipients with donor-derived West Nile virus (WNV) infection (encephalitis 3, asymptomatic 1) from a common donor residing in a region of increased WNV activity. All four transplant recipients had molecular evidence of WNV infection in their serum and/or cerebrospinal fluid (CSF) by reverse transcription polymerase chain reaction (RT-PCR) testing. Serum from the organ donor was positive for WNV IgM but negative for WNV RNA, whereas his lymph node and spleen tissues tested positive for WNV by RT-PCR. Combination therapy included intravenous immunoglobulin (4 cases), interferon (3 cases), fresh frozen plasma with WNV IgG (2 cases), and ribavirin (1 case). Two of the four transplant recipients survived.Review of the 20 published cases of organ-derived WNV infection found that this infection is associated with a high incidence of neuroinvasive disease (70%) and severe morbidity and mortality (30%). Median time to onset of symptomatic WNV infection was 13 days after transplantation (range 5-37 days). Initial unexplained fever unresponsive to antibiotic therapy followed by rapid onset of neurologic deficits was the most common clinical presentation. Confirmation of infection was made by testing serum and CSF for both WNV RNA by RT-PCR and WNV IgM by serological assays. Treatment usually included supportive care, reduction of immunosuppression, and frequent intravenous immunoglobulin. The often negative results for WNV by current RT-PCR and serological assays and the absence of clinical signs of acute infection in donors contribute to the sporadic occurrence of donor-derived WNV infection. Potential organ donors should be assessed for unexplained fever and neurological symptoms, particularly if they reside in areas of increased WNV activity.

Published
2014

9. A Phase III, Double-Blind, Randomized, Placebo-Controlled, Multicenter Clinical Trial to Study the Safety, Tolerability, Efficacy, and Immunogenicity of Inactivated Vzv Vaccine (ZVIN) in Recipients of Autologous Hematopoietic Cell Transplants (Auto-Hcts)

Author

Winston, Drew J., Mullane, Kathleen M., Boeckh, Michael J., Cornely, Oliver A., Hurtado, Kimberly, Su, Shu-Chih, Pang, Lei, Zhao, Yanli, Chan, Ivan S. F., Stek, Jon E., Kaplan, Susan S., Parrino, Janie, Annunziato, Paula, Popmihajlov, Zoran, Arvin, Ann, Winston, Drew J., Mullane, Kathleen M., Boeckh, Michael J., Cornely, Oliver A., Hurtado, Kimberly, Su, Shu-Chih, Pang, Lei, Zhao, Yanli, Chan, Ivan S. F., Stek, Jon E., Kaplan, Susan S., Parrino, Janie, Annunziato, Paula, Popmihajlov, Zoran, and Arvin, Ann

Published
2017

10. A Phase III, Double-Blind, Randomized, Placebo-Controlled, Multicenter Clinical Trial to Study the Safety, Tolerability, Efficacy, and Immunogenicity of Inactivated Vzv Vaccine (ZVIN) in Recipients of Autologous Hematopoietic Cell Transplants (Auto-Hcts)

Author

Winston, Drew J., Mullane, Kathleen M., Boeckh, Michael J., Cornely, Oliver A., Hurtado, Kimberly, Su, Shu-Chih, Pang, Lei, Zhao, Yanli, Chan, Ivan S. F., Stek, Jon E., Kaplan, Susan S., Parrino, Janie, Annunziato, Paula, Popmihajlov, Zoran, Arvin, Ann, Winston, Drew J., Mullane, Kathleen M., Boeckh, Michael J., Cornely, Oliver A., Hurtado, Kimberly, Su, Shu-Chih, Pang, Lei, Zhao, Yanli, Chan, Ivan S. F., Stek, Jon E., Kaplan, Susan S., Parrino, Janie, Annunziato, Paula, Popmihajlov, Zoran, and Arvin, Ann

Published
2017

11. Maribavir prophylaxis for prevention of cytomegalovirus disease in recipients of allogeneic stem-cell transplants: A phase 3, double-blind, placebo-controlled, randomised trial

Author

UCL - (SLuc) Service d'hématologie, Marty, Francisco M, Ljungman, Per, Papanicolaou, Genovefa A, Winston, Drew J, Chemaly, Roy F, Strasfeld, Lynne, Young, Jo-Anne H, Rodriguez, Tulio, Maertens, Johan, Schmitt, Michael, Einsele, Hermann, Ferrant, Augustin, Lipton, Jeffrey H, Villano, Stephen A, Chen, Hongzi, Boeckh, Michael, UCL - (SLuc) Service d'hématologie, Marty, Francisco M, Ljungman, Per, Papanicolaou, Genovefa A, Winston, Drew J, Chemaly, Roy F, Strasfeld, Lynne, Young, Jo-Anne H, Rodriguez, Tulio, Maertens, Johan, Schmitt, Michael, Einsele, Hermann, Ferrant, Augustin, Lipton, Jeffrey H, Villano, Stephen A, Chen, Hongzi, and Boeckh, Michael

Abstract

Background: Available drugs against cytomegalovirus have adverse effects that compromise their prophylactic use in recipients of allogeneic stem-cell transplants. We assessed the safety, tolerability, and antiviral activity of oral maribavir in such patients. Methods: In this placebo-controlled, randomised, double-blind, multicentre phase 3 study, we enrolled adult patients recipient-seropositive or donor-seropositive for cytomegalovirus who had undergone allogeneic stem-cell transplantation. Patients were recruited from 90 centres in Canada, Europe, and the USA. After engraftment, patients were stratified by recipient cytomegalovirus serostatus and conditioning regimen (myeloablative or reduced-intensity) and assigned (2:1) by masked computer-generated randomisation sequence to receive maribavir 100 mg twice daily or placebo for up to 12 weeks, with weekly blood cytomegalovirus surveillance. If the virus was detected, administration of study drug was stopped and pre-emptive anticytomegalovirus treatment started. The primary endpoint was cytomegalovirus disease within 6 months of transplantation. Analysis was by intention-to-treat. This study is registered with ClinicalTrials.gov, NCT00411645. Findings: Between December, 2006, and May, 2008, 681 patients were enrolled and assigned to receive maribavir (454) or placebo (227). The incidence of cytomegalovirus disease within 6 months was 20 of 454 (4%) for the maribavir group and 11 of 227 (5%) for the placebo group (OR 0·90; 95% CI 0·42-1·92). During the 100 days following transplantation, cytomegalovirus infection rates as measured by pp65 antigenaemia were lower in the maribavir group (26·4%) than in the placebo group (34·8%; OR 0·67; 0·47-0·95), but not when measured by plasma cytomegalovirus DNA PCR (27·8% vs 30·4%; OR 0·88; 0·62-1·25), nor by initiation of treatment against cytomegalovirus (30·6% vs 37·4%; OR 0·73, 0·52-1·03). Maribavir was well tolerated: most adverse events, including incident acute graft-versu

Published
2011

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