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Extension of Letermovir (LET) From Day 100 to Day 200 Post-transplant for the Prevention of Cytomegalovirus (CMV) Infection in Hematopoietic Stem Cell Transplant (HSCT) Participants (MK-8228-040)

Primary Purpose

Cytomegalovirus Infection

Status

Completed

Phase

Phase 3

Locations

International

Study Type

Interventional

Intervention

Letermovir

Placebo

About this trial

This is an interventional prevention trial for Cytomegalovirus Infection

Eligibility Criteria

18 Years - undefined (Adult, Older Adult)All SexesDoes not accept healthy volunteers

Inclusion Criteria:

have documented positive CMV serostatus (CMV immunoglobulin G [IgG] seropositive) for recipient (R+) at the time of transplant
has a history of allogeneic HSCT (bone marrow, peripheral blood stem cell, or cord blood transplant) within ~100 days prior to randomization
has undetectable CMV deoxyribonucleic acid (DNA) or detectable/not quantifiable CMV DNA from a plasma sample collected within 14 days prior to randomization
has received LET as primary prophylaxis that started within 28 days of HSCT and continued through Week 14 post-transplant (± 1 week) prior to randomization
is at high risk of CMV disease, defined as meeting one or more of the following criteria:
has a related donor with at least 1 mismatch at 1 of the specified 3 human leukocyte antigen (HLA) gene loci (HLA-A, B, or DR)
has an unrelated donor with at least one mismatch at one of the specified four HLA gene loci (HLA-A, B, C, and DRB1)
has a haploidentical donor
has umbilical cord blood as the stem-cell source
has ex-vivo T-cell-depleted grafts
has received anti-thymocyte globulin
has received alemtuzumab
has graft versus host disease (GVHD) or other conditions, requiring the use of systemic prednisone (or equivalent) at a dose of ≥1 mg/kg of body weight per day within 6 weeks of randomization
for female participants, is not pregnant or breastfeeding, and is either not a woman of childbearing potential (WOCBP) or is a WOBCP who agrees to use acceptable contraception during the treatment period and for ≥28 days after the last dose of study drug.

Exclusion Criteria:

has a history of CMV end-organ disease or preemptive treatment therapy for CMV after HSCT prior to randomization
has a history of >14 days total of LET interruption during the first 100 days post-transplant prior to randomization
has suspected or known hypersensitivity to active or inactive ingredients of LET formulations
has severe hepatic insufficiency defined as Child-Pugh Class C within 14 days prior to randomization.
has serum aspartate aminotransferase (AST) or alanine aminotransferase (ALT) >5× the upper limit of normal (ULN) within 14 days prior to randomization
has end-stage renal impairment with a creatinine clearance less than 10 mL/min, as calculated by the Cockcroft-Gault equation using serum creatinine within 14 days prior to randomization
has both moderate hepatic insufficiency AND moderate-to-severe renal insufficiency
has an uncontrolled infection on the day of enrollment
requires mechanical ventilation or is hemodynamically unstable at the time of enrollment
has a documented positive result for a human immunodeficiency virus antibody (HIV-Ab) test at any time prior to screening, or for hepatitis C virus antibody (HCV-Ab) with detectable HCV ribonucleic acid (RNA), or hepatitis B surface antigen (HBsAg) within 6 months prior to screening.
has active solid tumor malignancies with the exception of localized basal cell or squamous cell skin cancer or the condition under treatment (eg, lymphomas)
has received cidofovir or CMV immunoglobulin with 30 days prior to screening
is currently participating or has participated in a study with an unapproved investigational compound, monoclonal antibody, or device within 28 days or 5× half-life of the investigational compound or monoclonal antibody, whichever is longer, of initial dosing in this study
has previously participated in this study or any other study involving LET, or is currently participating in any study involving administration of a CMV vaccine or another CMV investigational agent, or is planning to participate in a study of a CMV vaccine or another CMV investigational agent during the course of this study
is pregnant or expecting to conceive, is breastfeeding, or plans to breastfeed from the time of consent through 28 days after the last dose of study therapy
is expecting to donate eggs starting from the time of consent through 28 days after the last dose of study therapy
has clinically relevant drug or alcohol abuse within 12 months of screening that may interfere with participant treatment, assessment, or compliance with the protocol as assessed by the investigator
has a history or current evidence of any condition, therapy, lab abnormality, or other circumstance that might confound the results of the study, interfere with the participant's participation for the full duration of the study, or would be put at undue risk as judged by the investigator, such that it is not in the best interest of the participant to participate in this study

Sites / Locations

City of Hope National Medical Center ( Site 0158)
University of California Davis Medical Center ( Site 0156)
University of Miami, Sylvester Comprehensive Cancer Center ( Site 0160)
Indiana Blood and Marrow Transplantation ( Site 0175)
Brigham & Women's Hospital ( Site 0161)
John Theurer Cancer Center at Hackensack University Med Ctr ( Site 0174)
Memorial Sloan Kettering Cancer Center ( Site 0164)
Duke University Medical Center ( Site 0169)
The University of Texas MD Anderson Cancer Center ( Site 0154)
Fred Hutchinson Cancer Research Center ( Site 0152)
Centre Hospitalier Universitaire Dupuytren ( Site 0182)
Hopital Saint Eloi ( Site 0031)
Centre Hopitalier Lyon Sud ( Site 0039)
CHU Henri Mondor ( Site 0032)
Institut Gustave Roussy ( Site 0038)
CHU Hopital Saint Antoine ( Site 0036)
Universitaetsklinikum Heidelberg-Medizinische Klinik V ( Site 0042)
Universitaetsklinik Koeln ( Site 0041)
Universitaetsklinikum Muenster ( Site 0043)
ASST Spedali Civili di Brescia ( Site 0052)
IRCCS Ospedale San Raffaele ( Site 0051)
Fondazione PTV Policlinico Tor Vergata ( Site 0054)
Policlinico Umberto I ( Site 0056)
Policlinico Universitario Agostino Gemelli ( Site 0055)
Jichi Medical University Hospital ( Site 0123)
Hiroshima Red Cross Hospital & Atomic-bomb Survivors Hospital ( Site 0121)
National Hospital Organization Kumamoto Medical Center ( Site 0122)
Queen Elizabeth University Hospital [Glasgow, UK] ( Site 0096)
1Kings College Hospital ( Site 0091)
UCL Cancer Institute ( Site 0093)
Manchester Royal Infirmary ( Site 0097)
Freeman Hospital Newcastle upon Tyne Foundation NHS Trust ( Site 0092)

Arms of the Study

Arm 1

Arm 2

Arm Type

Experimental

Placebo Comparator

Arm Label

Letermovir

Placebo

Arm Description

Participants who received HSCT transplant and 100 days of LET prophylaxis were randomized to an additional 100 days of LET (480 mg once daily alone or 240 mg once daily for participants on cyclosporin A) treatment.

Participants who received HSCT transplant and 100 days of LET prophylaxis were randomized to an additional 100 days of placebo treatment.

Outcomes

Primary Outcome Measures

Percentage of Participants With Clinically Significant CMV Infection From Week 14 (~100 Days) Post-transplant Through Week 28 (~200 Days) Post-transplant

Clinically significant CMV infection is either the onset of probable or proven CMV end-organ disease or initiation of anti-CMV preemptive therapy (PET) with approved anti-CMV agents (ganciclovir, valganciclovir, foscarnet, and/or cidofovir) based on documented CMV viremia and the clinical condition of the participant. Missing values were handled by the observed failure (OF) approach where failure was defined as all participants who develop clinically significant CMV infection or discontinue prematurely from the study with CMV viremia from week 14 (~100 days) through week 28 post-transplant. It was hypothesized that LET is superior to placebo in the prevention of clinically significant CMV infection when LET prophylaxis is extended from 100 to 200 days.

Secondary Outcome Measures

Percentage of Participants Experiencing ≥1 Adverse Events (AEs) From Week 14 (~100 Days) Post-transplant Through Week 28 (~200 Days) Post-transplant

An adverse event (AE) is any untoward medical occurrence in a clinical study participant, temporally associated with the use of study intervention, whether or not considered related to the study intervention.

Percentage of Participants Withdrawing From Study Drug Due to an AE From Week 14 (~100 Days) Post-transplant Through Week 28 (~200 Days) Post-transplant

An AE is any untoward medical occurrence in a clinical study participant, temporally associated with the use of study intervention, whether or not considered related to the study intervention.

Percentage of Participants With Clinically Significant CMV Infection From Week 14 Post-transplant Through Week 38 Post-transplant

Clinically significant CMV infection is either the onset of probable or proven CMV end-organ disease or initiation of anti-CMV PET with approved anti-CMV agents (ganciclovir, valganciclovir, foscarnet, and/or cidofovir) based on documented CMV viremia and the clinical condition of the participant. Missing values were handled by the OF approach where failure was defined as all participants who develop clinically significant CMV infection or discontinue prematurely from the study with CMV viremia from week 14 (~100 days) through week 38 post-transplant.

Percentage of Participants With Clinically Significant CMV Infection From Week 14 Post-transplant Through Week 48 Post-transplant

Time to Onset of Clinically Significant CMV Infection From Week 14 Post-transplant to Week 28 Post-transplant

Clinically significant CMV infection is either the onset of probable or proven CMV end-organ disease or initiation of anti-CMV PET with approved anti-CMV agents (ganciclovir, valganciclovir, foscarnet, and/or cidofovir) based on documented CMV viremia and the clinical condition of the participant. Time to onset of clinically significant CMV infection is the elapsed time from transplant to the onset of CMV end-organ disease or to the initiation of anti-CMV PET. Time to onset was determined from the Kaplan-Meier method for censored data.

Time to Onset of Clinically Significant CMV Infection From Week 14 Post-transplant to Week 48 Post-transplant

Clinically significant CMV infection is either the onset of probable or proven CMV end-organ disease or initiation of anti-CMV PET with approved anti-CMV agents (ganciclovir, valganciclovir, foscarnet, and/or cidofovir) based on documented CMV viremia and the clinical condition of the participant. Time to onset of clinically significant CMV infection is the elapsed time from transplant to the onset of CMV end-organ disease or to the initiation of anti-CMV PET. Time to onset was determined from the Kaplan-Meier method for censored data.

Percentage of Participants With CMV Viremia Who Started PET From Week 14 Post-transplant to Week 28 Post-transplant

The percentage of participants with CMV viremia who initiated PET of anti-CMV agents (ganciclovir, valganciclovir, foscarnet, and/or cidofovir) was determined. Missing values were handled with the OF approach, where failure was defined as all participants who develop clinically significant CMV infection or discontinue prematurely from the study with CMV viremia from week 14 through week 28 post-transplant.

Percentage of Participants With CMV Viremia Who Started PET From Week 14 Post-transplant to Week 48 Post-transplant

Percentage of Participants With All-cause Mortality From Week 14 Post-transplant to Week 28 Post-transplant

The percentage of participants who died due to any cause (all-cause mortality) from Week 14 to Week 28 was determined.

Percentage of Participants With All-cause Mortality From Week 14 Post-transplant to Week 48 Post-transplant

The percentage of participants who died due to any cause (all-cause mortality) from Week 14 to Week 48 was determined.

Time to All-cause Mortality From Week 14 Post-transplant to Week 28 Post-transplant

Time to all-cause mortality is the time elapsed after Week 14 post-transplant and death due to any cause, and was determined from the Kaplan-Meier method for censored data.

Time to All-cause Mortality From Week 14 Post-transplant to Week 48 Post-transplant

Time to all-cause mortality is the time elapsed after Week 14 post-transplant and death due to any cause, and was determined from the Kaplan-Meier method for censored data.

Full Information

NCT ID

NCT03930615

First Posted

April 26, 2019

Last Updated

October 5, 2022

Sponsor

Merck Sharp & Dohme LLC

1. Study Identification

Unique Protocol Identification Number

NCT03930615

Brief Title

Extension of Letermovir (LET) From Day 100 to Day 200 Post-transplant for the Prevention of Cytomegalovirus (CMV) Infection in Hematopoietic Stem Cell Transplant (HSCT) Participants (MK-8228-040)

Official Title

A Phase 3 Randomized, Double-blind, Placebo-controlled Clinical Trial to Evaluate the Safety and Efficacy of Letermovir (LET) Prophylaxis When Extended From 100 Days to 200 Days Post-transplant in Cytomegalovirus (CMV) Seropositive Recipients (R+) of an Allogenic Hematopoietic Stem Cell Transplant (HSCT)

Study Type

Interventional

2. Study Status

Record Verification Date

October 2022

Overall Recruitment Status

Completed

Study Start Date

June 21, 2019 (Actual)

Primary Completion Date

October 27, 2021 (Actual)

Study Completion Date

March 16, 2022 (Actual)

3. Sponsor/Collaborators

Responsible Party, by Official Title

Sponsor

Name of the Sponsor

Merck Sharp & Dohme LLC

4. Oversight

Studies a U.S. FDA-regulated Drug Product

Yes

Studies a U.S. FDA-regulated Device Product

Data Monitoring Committee

Yes

5. Study Description

Brief Summary

The purpose of this study was to evaluate the safety and efficacy of letermovir (LET) versus placebo when cytomegalovirus (CMV) prophylaxis was extended from 100 days to 200 days post-transplant in CMV seropositive participants who received an allogenic hematopoietic stem cell transplant (HSCT). It was hypothesized that LET is superior to placebo in the prevention of clinically-significant CMV infection when LET prophylaxis is extended from 100 to 200 days.

6. Conditions and Keywords

Primary Disease or Condition Being Studied in the Trial, or the Focus of the Study

Cytomegalovirus Infection

7. Study Design

Primary Purpose

Prevention

Study Phase

Phase 3

Interventional Study Model

Parallel Assignment

Masking

ParticipantCare ProviderInvestigatorOutcomes Assessor

Allocation

Randomized

Enrollment

220 (Actual)

8. Arms, Groups, and Interventions

Arm Title

Letermovir

Arm Type

Experimental

Arm Description

Arm Title

Placebo

Arm Type

Placebo Comparator

Arm Description

Participants who received HSCT transplant and 100 days of LET prophylaxis were randomized to an additional 100 days of placebo treatment.

Intervention Type

Drug

Intervention Name(s)

Letermovir

Other Intervention Name(s)

PREVYMIS™, MK-8228

Intervention Description

LET tablet or intravenous infusion at a total daily dose of 240 mg (when given with cyclosporin A) or 480 mg (when given alone).

Intervention Type

Drug

Intervention Name(s)

Placebo

Intervention Description

Placebo was administered as tablets matched to LET or as inactive (saline or dextrose) intravenous infusion.

Primary Outcome Measure Information:

Title

Percentage of Participants With Clinically Significant CMV Infection From Week 14 (~100 Days) Post-transplant Through Week 28 (~200 Days) Post-transplant

Description

Time Frame

From Week 14 post-transplant to Week 28 post-transplant (approximately 14 weeks)

Secondary Outcome Measure Information:

Title

Percentage of Participants Experiencing ≥1 Adverse Events (AEs) From Week 14 (~100 Days) Post-transplant Through Week 28 (~200 Days) Post-transplant

Description

Time Frame

From Week 14 post-transplant to Week 28 post-transplant (approximately 14 weeks)

Title

Percentage of Participants Withdrawing From Study Drug Due to an AE From Week 14 (~100 Days) Post-transplant Through Week 28 (~200 Days) Post-transplant

Description

An AE is any untoward medical occurrence in a clinical study participant, temporally associated with the use of study intervention, whether or not considered related to the study intervention.

Time Frame

From Week 14 post-transplant to Week 28 post-transplant (approximately 14 weeks)

Title

Percentage of Participants With Clinically Significant CMV Infection From Week 14 Post-transplant Through Week 38 Post-transplant

Description

Time Frame

From Week 14 post-transplant to Week 38 post-transplant (approximately 24 weeks)

Title

Percentage of Participants With Clinically Significant CMV Infection From Week 14 Post-transplant Through Week 48 Post-transplant

Description

Time Frame

From Week 14 post-transplant to Week 48 post-transplant (approximately 34 weeks)

Title

Time to Onset of Clinically Significant CMV Infection From Week 14 Post-transplant to Week 28 Post-transplant

Description

Clinically significant CMV infection is either the onset of probable or proven CMV end-organ disease or initiation of anti-CMV PET with approved anti-CMV agents (ganciclovir, valganciclovir, foscarnet, and/or cidofovir) based on documented CMV viremia and the clinical condition of the participant. Time to onset of clinically significant CMV infection is the elapsed time from transplant to the onset of CMV end-organ disease or to the initiation of anti-CMV PET. Time to onset was determined from the Kaplan-Meier method for censored data.

Time Frame

From Week 14 post-transplant to Week 28 post-transplant (approximately 14 weeks)

Title

Time to Onset of Clinically Significant CMV Infection From Week 14 Post-transplant to Week 48 Post-transplant

Description

Clinically significant CMV infection is either the onset of probable or proven CMV end-organ disease or initiation of anti-CMV PET with approved anti-CMV agents (ganciclovir, valganciclovir, foscarnet, and/or cidofovir) based on documented CMV viremia and the clinical condition of the participant. Time to onset of clinically significant CMV infection is the elapsed time from transplant to the onset of CMV end-organ disease or to the initiation of anti-CMV PET. Time to onset was determined from the Kaplan-Meier method for censored data.

Time Frame

From Week 14 post-transplant to Week 48 post-transplant (approximately 34 weeks)

Title

Percentage of Participants With CMV Viremia Who Started PET From Week 14 Post-transplant to Week 28 Post-transplant

Description

Time Frame

From Week 14 post-transplant to Week 28 post-transplant (approximately 14 weeks)

Title

Percentage of Participants With CMV Viremia Who Started PET From Week 14 Post-transplant to Week 48 Post-transplant

Description

Time Frame

From Week 14 post-transplant to Week 48 post-transplant (approximately 34 weeks)

Title

Percentage of Participants With All-cause Mortality From Week 14 Post-transplant to Week 28 Post-transplant

Description

The percentage of participants who died due to any cause (all-cause mortality) from Week 14 to Week 28 was determined.

Time Frame

From Week 14 post-transplant to Week 28 post-transplant (approximately 14 weeks)

Title

Percentage of Participants With All-cause Mortality From Week 14 Post-transplant to Week 48 Post-transplant

Description

The percentage of participants who died due to any cause (all-cause mortality) from Week 14 to Week 48 was determined.

Time Frame

From Week 14 post-transplant to Week 48 post-transplant (approximately 34 weeks)

Title

Time to All-cause Mortality From Week 14 Post-transplant to Week 28 Post-transplant

Description

Time to all-cause mortality is the time elapsed after Week 14 post-transplant and death due to any cause, and was determined from the Kaplan-Meier method for censored data.

Time Frame

From Week 14 post-transplant to Week 28 post-transplant (approximately 14 weeks)

Title

Time to All-cause Mortality From Week 14 Post-transplant to Week 48 Post-transplant

Description

Time to all-cause mortality is the time elapsed after Week 14 post-transplant and death due to any cause, and was determined from the Kaplan-Meier method for censored data.

Time Frame

From Week 14 post-transplant to Week 48 post-transplant (approximately 34 weeks)

10. Eligibility

Sex

All

Minimum Age & Unit of Time

18 Years

Accepts Healthy Volunteers

Eligibility Criteria

Inclusion Criteria: have documented positive CMV serostatus (CMV immunoglobulin G [IgG] seropositive) for recipient (R+) at the time of transplant has a history of allogeneic HSCT (bone marrow, peripheral blood stem cell, or cord blood transplant) within ~100 days prior to randomization has undetectable CMV deoxyribonucleic acid (DNA) or detectable/not quantifiable CMV DNA from a plasma sample collected within 14 days prior to randomization has received LET as primary prophylaxis that started within 28 days of HSCT and continued through Week 14 post-transplant (± 1 week) prior to randomization is at high risk of CMV disease, defined as meeting one or more of the following criteria: has a related donor with at least 1 mismatch at 1 of the specified 3 human leukocyte antigen (HLA) gene loci (HLA-A, B, or DR) has an unrelated donor with at least one mismatch at one of the specified four HLA gene loci (HLA-A, B, C, and DRB1) has a haploidentical donor has umbilical cord blood as the stem-cell source has ex-vivo T-cell-depleted grafts has received anti-thymocyte globulin has received alemtuzumab has graft versus host disease (GVHD) or other conditions, requiring the use of systemic prednisone (or equivalent) at a dose of ≥1 mg/kg of body weight per day within 6 weeks of randomization for female participants, is not pregnant or breastfeeding, and is either not a woman of childbearing potential (WOCBP) or is a WOBCP who agrees to use acceptable contraception during the treatment period and for ≥28 days after the last dose of study drug. Exclusion Criteria: has a history of CMV end-organ disease or preemptive treatment therapy for CMV after HSCT prior to randomization has a history of >14 days total of LET interruption during the first 100 days post-transplant prior to randomization has suspected or known hypersensitivity to active or inactive ingredients of LET formulations has severe hepatic insufficiency defined as Child-Pugh Class C within 14 days prior to randomization. has serum aspartate aminotransferase (AST) or alanine aminotransferase (ALT) >5× the upper limit of normal (ULN) within 14 days prior to randomization has end-stage renal impairment with a creatinine clearance less than 10 mL/min, as calculated by the Cockcroft-Gault equation using serum creatinine within 14 days prior to randomization has both moderate hepatic insufficiency AND moderate-to-severe renal insufficiency has an uncontrolled infection on the day of enrollment requires mechanical ventilation or is hemodynamically unstable at the time of enrollment has a documented positive result for a human immunodeficiency virus antibody (HIV-Ab) test at any time prior to screening, or for hepatitis C virus antibody (HCV-Ab) with detectable HCV ribonucleic acid (RNA), or hepatitis B surface antigen (HBsAg) within 6 months prior to screening. has active solid tumor malignancies with the exception of localized basal cell or squamous cell skin cancer or the condition under treatment (eg, lymphomas) has received cidofovir or CMV immunoglobulin with 30 days prior to screening is currently participating or has participated in a study with an unapproved investigational compound, monoclonal antibody, or device within 28 days or 5× half-life of the investigational compound or monoclonal antibody, whichever is longer, of initial dosing in this study has previously participated in this study or any other study involving LET, or is currently participating in any study involving administration of a CMV vaccine or another CMV investigational agent, or is planning to participate in a study of a CMV vaccine or another CMV investigational agent during the course of this study is pregnant or expecting to conceive, is breastfeeding, or plans to breastfeed from the time of consent through 28 days after the last dose of study therapy is expecting to donate eggs starting from the time of consent through 28 days after the last dose of study therapy has clinically relevant drug or alcohol abuse within 12 months of screening that may interfere with participant treatment, assessment, or compliance with the protocol as assessed by the investigator has a history or current evidence of any condition, therapy, lab abnormality, or other circumstance that might confound the results of the study, interfere with the participant's participation for the full duration of the study, or would be put at undue risk as judged by the investigator, such that it is not in the best interest of the participant to participate in this study

Overall Study Officials:

First Name & Middle Initial & Last Name & Degree

Medical Director

Organizational Affiliation

Merck Sharp & Dohme LLC

Official's Role

Study Director

Facility Information:

Facility Name

City of Hope National Medical Center ( Site 0158)

City

Duarte

State/Province

California

ZIP/Postal Code

91010

Country

United States

Facility Name

University of California Davis Medical Center ( Site 0156)

City

Sacramento

State/Province

California

ZIP/Postal Code

95817

Country

United States

Facility Name

University of Miami, Sylvester Comprehensive Cancer Center ( Site 0160)

City

Miami

State/Province

Florida

ZIP/Postal Code

33136

Country

United States

Facility Name

Indiana Blood and Marrow Transplantation ( Site 0175)

City

Indianapolis

State/Province

Indiana

ZIP/Postal Code

46237

Country

United States

Facility Name

Brigham & Women's Hospital ( Site 0161)

City

Boston

State/Province

Massachusetts

ZIP/Postal Code

02115

Country

United States

Facility Name

John Theurer Cancer Center at Hackensack University Med Ctr ( Site 0174)

City

Hackensack

State/Province

New Jersey

ZIP/Postal Code

07601

Country

United States

Facility Name

Memorial Sloan Kettering Cancer Center ( Site 0164)

City

New York

State/Province

New York

ZIP/Postal Code

10065

Country

United States

Facility Name

Duke University Medical Center ( Site 0169)

City

Durham

State/Province

North Carolina

ZIP/Postal Code

27710

Country

United States

Facility Name

The University of Texas MD Anderson Cancer Center ( Site 0154)

City

Houston

State/Province

Texas

ZIP/Postal Code

77030

Country

United States

Facility Name

Fred Hutchinson Cancer Research Center ( Site 0152)

City

Seattle

State/Province

Washington

ZIP/Postal Code

98109

Country

United States

Facility Name

Centre Hospitalier Universitaire Dupuytren ( Site 0182)

City

Limoges

State/Province

Haute-Vienne

ZIP/Postal Code

87042

Country

France

Facility Name

Hopital Saint Eloi ( Site 0031)

City

Montpellier

State/Province

Herault

ZIP/Postal Code

34295

Country

France

Facility Name

Centre Hopitalier Lyon Sud ( Site 0039)

City

Pierre Benite

State/Province

Rhone

ZIP/Postal Code

69495

Country

France

Facility Name

CHU Henri Mondor ( Site 0032)

City

Creteil

State/Province

Val-de-Marne

ZIP/Postal Code

94110

Country

France

Facility Name

Institut Gustave Roussy ( Site 0038)

City

Villejuif

State/Province

Val-de-Marne

ZIP/Postal Code

94805

Country

France

Facility Name

CHU Hopital Saint Antoine ( Site 0036)

City

Paris

ZIP/Postal Code

75012

Country

France

Facility Name

Universitaetsklinikum Heidelberg-Medizinische Klinik V ( Site 0042)

City

Heidelberg

State/Province

Baden-Wurttemberg

ZIP/Postal Code

69120

Country

Germany

Facility Name

Universitaetsklinik Koeln ( Site 0041)

City

Koeln

State/Province

Nordrhein-Westfalen

ZIP/Postal Code

50937

Country

Germany

Facility Name

Universitaetsklinikum Muenster ( Site 0043)

City

Muenster

State/Province

Nordrhein-Westfalen

ZIP/Postal Code

48149

Country

Germany

Facility Name

ASST Spedali Civili di Brescia ( Site 0052)

City

Brescia

State/Province

Lombardia

ZIP/Postal Code

25123

Country

Italy

Facility Name

IRCCS Ospedale San Raffaele ( Site 0051)

City

Milano

ZIP/Postal Code

20132

Country

Italy

Facility Name

Fondazione PTV Policlinico Tor Vergata ( Site 0054)

City

Roma

ZIP/Postal Code

00133

Country

Italy

Facility Name

Policlinico Umberto I ( Site 0056)

City

Roma

ZIP/Postal Code

00161

Country

Italy

Facility Name

Policlinico Universitario Agostino Gemelli ( Site 0055)

City

Roma

ZIP/Postal Code

00168

Country

Italy

Facility Name

Jichi Medical University Hospital ( Site 0123)

City

Shimotsuke

State/Province

Tochigi

ZIP/Postal Code

329-0498

Country

Japan

Facility Name

Hiroshima Red Cross Hospital & Atomic-bomb Survivors Hospital ( Site 0121)

City

Hiroshima

ZIP/Postal Code

730-8619

Country

Japan

Facility Name

National Hospital Organization Kumamoto Medical Center ( Site 0122)

City

Kumamoto

ZIP/Postal Code

860-0008

Country

Japan

Facility Name

Queen Elizabeth University Hospital [Glasgow, UK] ( Site 0096)

City

Glasgow

State/Province

Glasgow City

ZIP/Postal Code

G51 4TF

Country

United Kingdom

Facility Name

1Kings College Hospital ( Site 0091)

City

London

State/Province

London, City Of

ZIP/Postal Code

SE5 9RS

Country

United Kingdom

Facility Name

UCL Cancer Institute ( Site 0093)

City

London

State/Province

London, City Of

ZIP/Postal Code

WC1E 6BT

Country

United Kingdom

Facility Name

Manchester Royal Infirmary ( Site 0097)

City

Manchester

ZIP/Postal Code

M13 9WL

Country

United Kingdom

Facility Name

Freeman Hospital Newcastle upon Tyne Foundation NHS Trust ( Site 0092)

City

Newcastle upon Tyne

ZIP/Postal Code

NE7 7DN

Country

United Kingdom

12. IPD Sharing Statement

Plan to Share IPD

Yes

IPD Sharing Plan Description

http://engagezone.msd.com/doc/ProcedureAccessClinicalTrialData.pdf

IPD Sharing URL

http://engagezone.msd.com/ds_documentation.php

Learn more about this trial

Extension of Letermovir (LET) From Day 100 to Day 200 Post-transplant for the Prevention of Cytomegalovirus (CMV) Infection in Hematopoietic Stem Cell Transplant (HSCT) Participants (MK-8228-040)

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