Letermovir Treatment in Pediatric Participants Following Allogeneic Haematopoietic Stem Cell Transplantation (HSCT) (MK-8228-030)

Phase 2

Completed

• Conditions: Cytomegalovirus (CMV) Infection
• Interventions: Drug: Letermovir oral granules; Drug: Letermovir tablet; Drug: Letermovir intravenous

• Registration Number: NCT03940586
• Lead Sponsor: Merck Sharp & Dohme LLC

Brief Summary

The primary objective of this study is to evaluate the pharmacokinetics (PK) of letermovir (LET) in pediatric participants. Participants will be enrolled in the following 3 age groups: Age Group 1: From 12 to \<18 years of age (adolescents); Age Group 2: From 2 to \<12 years of age (children); and Age Group 3: From birth to \<2 years of age (neonates, infants and toddlers). All participants will receive open label LET for 14 weeks (\~100 days) post-transplant, with doses based on body weight and age.

Detailed Description

Not available

Study Timeline

• Study First Submitted: 2019-05-06
• Study First Submitted QC: 2019-05-06
• Study First Posted: 2019-05-07
• Study Start: 2019-08-08
• Primary Completion: 2023-01-04
• Study Completion: 2023-08-25
• Results First Submitted: 2023-11-29
• Results First Submitted QC: 2024-01-05
• Results First Posted: 2024-01-30
• Status Verified: 2024-07
• Last Update Submitted: 2024-07-30
• Last Update Posted: 2024-08-22

Recruitment & Eligibility

• Status: COMPLETED
• Sex: All
• Target Recruitment: 65

Inclusion Criteria

• All participants 12 to <18 years old must have documented positive CMV serostatus (CMV IgG seropositive) for the recipient (R+) within 90 days prior to enrollment. Participants from birth to <12 years old must have documented positive CMV serostatus (CMV IgG seropositive) for the recipient (R+) within 90 days prior to enrollment and/or the donor (D+); the donor serostatus should be documented within 1 year prior to enrollment.
• Is the recipient of a first allogeneic HSCT (bone marrow, peripheral blood stem cell, or cord blood transplant).
• Has undetectable CMV DNA from a plasma or whole blood sample collected within 5 days prior to enrollment.
• Is within 28 days post-HSCT at the time of enrollment.
• Females are not pregnant, not breastfeeding,and is not a woman of childbearing potential (WOCBP); or is a WOCBP who agrees to follow the contraceptive guidance during the treatment period and for at least 28 days after the last dose of study intervention.
• Participants from 2 to <18 years of age must not be on concomitant Cyclosporin A (CsA), and must be able to take LET tablets or the oral granules (either by mouth or via G tube/NG tube), provided the participant does not have a condition that may interfere with the absorption of oral medication (e.g. vomiting, diarrhea, or a malabsorptive condition) from the day of enrollment until the intensive PK sampling is completed in these participants.
• For participants 2 <12 years old their weight should be at least 10 kg; for participants from birth to <2 years old their weight should be at least 2.5 kg and less than or equal to 15 kg at the time of enrollment.

Exclusion Criteria

• Has received a previous allogeneic HSCT (Note: receipt of a previous autologous HSCT is acceptable).
• Has a history of CMV end-organ disease within 6 months prior to enrollment.
• Has evidence of CMV viremia at any time from either signing of the ICF or the HSCT procedure, whichever is earlier, until the time of enrollment.
• Has suspected or known hypersensitivity to active or inactive ingredients of LET formulations.
• Has severe hepatic insufficiency within 5 days prior to enrollment.
• Is a) on renal replacement therapy (eg, hemodialysis, peritoneal dialysis) OR b) has end-stage renal impairment.
• 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 (HIVAb) test at any time prior to enrollment, or for hepatitis C virus antibody (HCV-Ab) with detectable HCV RNA, or hepatitis B surface antigen (HBsAg) within 90 days prior to enrollment.
• Has active solid tumor malignancies with the exception of localized basal cell or squamous cell skin cancer or the condition under treatment (e.g. lymphomas).
• Has a preexisting cardiac condition a) for which the patient is currently being treated or b) which required hospitalization within the last 6 months or c) that may be expected to recur during the course of the trial.
• Has received within 7 days prior to screening any of the following: ganciclovir; valganciclovir; foscarnet; acyclovir; valacyclovir; famciclovir.
• Has received within 30 days prior to screening of any of the following: cidofovir; CMV immunoglobulin; any investigational CMV antiviral agent/biologic therapy; Rifampin and other strong inducers (such as phenytoin, carbamazepine, St John's wort (Hypericum perforatum), rifabutin and phenobarbital) and moderate inducers such as nafcillin, thioridazine, modafinil and bosentan.
• Has received LET at any time prior to enrollment in this study.
• Is currently participating or has participated in a study with an unapproved investigational compound or device within 28 days, or 5X half-life of the investigational compound (excluding monoclonal antibodies), whichever is longer, of initial dosing in this study.
• Has previously participated in this study or any other study involving LET.
• Has previously participated 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 intervention.
• Is expecting to donate eggs starting from the time of consent through 28 days after the last dose of study intervention.
• 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.

Study & Design

• Study Type: INTERVENTIONAL
• Study Design: SINGLE_GROUP

Arm && Interventions

Group	Intervention	Description
Letermovir	Letermovir oral granules	Letermovir administered either orally or intravenously within 28 days post-transplant, once daily through week 14 (approximately 100 days). Dosing will vary based on age, weight, and whether participant takes cyclosporin A as a concomitant medication.
Letermovir	Letermovir tablet	Letermovir administered either orally or intravenously within 28 days post-transplant, once daily through week 14 (approximately 100 days). Dosing will vary based on age, weight, and whether participant takes cyclosporin A as a concomitant medication.
Letermovir	Letermovir intravenous	Letermovir administered either orally or intravenously within 28 days post-transplant, once daily through week 14 (approximately 100 days). Dosing will vary based on age, weight, and whether participant takes cyclosporin A as a concomitant medication.

Primary Outcome Measures

Name	Time	Method
Minimum Concentration of Plasma Letermovir Observed Before Next Dose (Ctrough) Taken as Oral Formulation by Ages 2 - <18 Years	Day 7: 24 hours post-dose	Blood was collected on treatment Day 7 from participants aged 2 - \<18 years in order to determine the Ctrough of plasma letermovir for participants receiving oral formulation. Individual values were natural log transformed and evaluated separately with a linear mixed effects model containing a fixed effect for treatment and a random effect for participant. Participants aged \< 2 years were not presented as their data analysis resulted in a different measure type and method of dispersion.
AUC0-24 of Plasma Letermovir Taken as Oral Formulation by Ages <2 Years	Day 7: Pre-dose, 1, 2.5, 8, and 24 hours post-dose	Blood was collected on treatment Day 7 from participants aged \<2 years in order to determine the AUC0-24 of plasma letermovir for participants receiving oral formulation. Individual values were natural log transformed and evaluated separately with a linear mixed effects model containing a fixed effect for treatment and a random effect for participant. Participants aged 2 - \<18 years were not presented as their data analysis resulted in a different measure type and method of dispersion. The measure of dispersion is not determined when N \<2.
Cmax of Plasma Letermovir Taken as Oral Formulation by Ages 2 to <12 Years	Day 7: Pre-dose, 1, 2.5, 8, and 24 hours post-dose	Blood was collected on treatment Day 7 from participants aged 2 to \<12 years in order to determine Cmax of plasma letermovir for participants receiving oral formulation. Individual values were natural log transformed and evaluated separately with a linear mixed effects model containing a fixed effect for treatment and a random effect for participant. Participants aged \<2 and \>12 years were not presented as their data analysis resulted in a different measure type and method of dispersion.
AUC0-24 of Plasma Letermovir Taken as Intravenous (IV) Formulation by Ages 12 - <18 Years	Day 7: Pre-dose, 1, 2.5, 8, and 24 hours post-dose	Blood was collected on treatment Day 7 from participants aged 12 - \<18 years in order to determine the AUC0-24 of plasma letermovir for participants receiving IV formulation. Individual values were natural log transformed and evaluated separately with a linear mixed effects model containing a fixed effect for treatment and a random effect for participant. Participants aged \< 12 years were not presented as their data analysis resulted in a different measure type and method of dispersion.
Concentration at the End of Infusion (Ceoi) of Plasma Letermovir Taken as IV Formulation by Ages 12 - <18 Years	Day 7: Pre-dose, 1, 2.5, 8, and 24 hours post-dose	Blood was collected on treatment Day 7 from participants aged 12 - \<18 years in order to determine the Ceoi of plasma letermovir for participants receiving IV formulation. As samples were collected outside the collection window Ceoi for these samples were predicted by using a log linear model .Participants aged \< 12 years were not presented as their data analysis resulted in a different measure type and method of dispersion.
Ctrough of Plasma Letermovir Taken as IV Formulation by Ages 12 - <18 Years	Day 7: 24 hours post-dose	Blood was collected on treatment Day 7 from participants aged 12 - \<18 years in order to determine the Ctrough of plasma letermovir for participants receiving IV formulation. Individual values were natural log transformed and evaluated separately with a linear mixed effects model containing a fixed effect for treatment and a random effect for participant. Participants aged \< 12 years were not presented as their data analysis resulted in a different measure type and method of dispersion.
Cmax of Plasma Letermovir Taken as Oral Formulation by Ages < 2 Years	Day 7: Pre-dose, 1, 2.5, 8, and 24 hours post-dose	Blood was collected on treatment Day 7 from participants aged \<2 years in order to determine the Cmax of plasma letermovir for participants receiving oral formulation. Individual values were natural log transformed and evaluated separately with a linear mixed effects model containing a fixed effect for treatment and a random effect for participant. Participants aged 2 - \<18 years were not presented as their data analysis resulted in a different measure type and method of dispersion. The measure of dispersion is not determined when N \<2
Ceoi of Plasma Letermovir Taken as IV Formulation by Ages s 2 to <12 Years	Day 7: Pre-dose, 1, 2.5, 8, and 24 hours post-dose	Blood was collected on treatment Day 7 from participants aged 2 to \<12 years in order to determine the Ceoi of plasma letermovir for participants receiving IV formulation. As samples were collected outside the collection window Ceoi for these samples were predicted by using a log linear model. Participants aged \> 2 years were not presented as their data analysis resulted in a different measure type and method of dispersion. A measure of dispersion is not determined when N \<2.
Ctrough of Plasma Letermovir Taken as IV Formulation by Ages <2 Years	Day 7: Pre-dose, 1, 2.5, 8, and 24 hours post-dose	Blood was collected on treatment Day 7 from participants aged \<2 years in order to determine the Ctrough of plasma letermovir for participants receiving IV formulation. Individual values were natural log transformed and evaluated separately with a linear mixed effects model containing a fixed effect for treatment and a random effect for participant. Participants aged \> 2 years were not presented as their data analysis resulted in a different measure type and method of dispersion. The measure type is Geometric Mean, and a measure of dispersion is not determined when N \<2.
Ctrough of Plasma Letermovir Taken During Sparse PK as IV Formulation	Day 7: 24 hours post-dose	Blood was collected on treatment Day 7 in order to determine the Ctrough of plasma letermovir for participants receiving IV formulation during sparse PK. Individual values were natural log transformed and evaluated separately with a linear mixed effects model containing a fixed effect for treatment and a random effect for participant.
AUC0-24 of Plasma Letermovir Taken as Oral Formulation by Ages 2 to <12 Years	Day 7: Pre-dose, 1, 2.5, 8, and 24 hours post-dose	Blood was collected on treatment Day 7 from participants aged 2 to \<12 years in order to determine the AUC0-24 of plasma letermovir for participants receiving oral formulation. Individual values were natural log transformed and evaluated separately with a linear mixed effects model containing a fixed effect for treatment and a random effect for participant. Participants aged \<2 and \>12 years were not presented as their data analysis resulted in a different measure type and method of dispersion.
Ctrough of Plasma Letermovir Taken as Oral Formulation by Ages 2 to <12 Years	Day 7: Pre-dose, 1, 2.5, 8, and 24 hours post-dose	Blood was collected on treatment Day 7 from participants aged 2 to \<12 years in order to determine Ctrough of plasma letermovir for participants receiving oral formulation. Individual values were natural log transformed and evaluated separately with a linear mixed effects model containing a fixed effect for treatment and a random effect for participant. Participants aged \<2 and \>12 years were not presented as their data analysis resulted in a different measure type and method of dispersion.
Ctrough of Plasma Letermovir Taken as Oral Formulation by Ages < 2 Years	Day 7: 24 hours post-dose	Blood was collected on treatment Day 7 from participants aged \<2 years in order to determine the Ctrough of plasma letermovir for participants receiving oral formulation. Individual values were natural log transformed and evaluated separately with a linear mixed effects model containing a fixed effect for treatment and a random effect for participant. Participants aged 2 - \<18 years were not presented as their data analysis resulted in a different measure type and method of dispersion. The measure of dispersion is not determined when N \<2.
AUC0-24 of Plasma Letermovir Taken as IV Formulation by Ages 2 to <12 Years	Day 7: Pre-dose, 1, 2.5, 8, and 24 hours post-dose	Blood was collected on treatment Day 7 from participants aged 2 to \<12 years in order to determine the AUC0-24 of plasma letermovir for participants receiving IV formulation. Individual values were natural log transformed and evaluated separately with a linear mixed effects model containing a fixed effect for treatment and a random effect for participant. Participants aged \> 2 years were not presented as their data analysis resulted in a different measure type and method of dispersion. The measure of dispersion is not determined when N \<2.
AUC0-24 of Plasma Letermovir Taken as IV Formulation by Ages <2 Years	Day 7: Pre-dose, 1, 2.5, 8, and 24 hours post-dose	Blood was collected on treatment Day 7 from participants aged \<2 years in order to determine the AUC0-24 of plasma letermovir for participants receiving IV formulation. Individual values were natural log transformed and evaluated separately with a linear mixed effects model containing a fixed effect for treatment and a random effect for participant. Participants aged \> 2 years were not presented as their data analysis resulted in a different measure type and method of dispersion. The measure of dispersion is not determined when N \<2.
Ceoi of Plasma Letermovir Taken as IV Formulation by Ages 2 to <12 Years	Day 7: Pre-dose, 1, 2.5, 8, and 24 hours post-dose	Blood was collected on treatment Day 7 from participants aged 2 to \<12 years in order to determine the Ceoi of plasma letermovir for participants receiving IV formulation. As samples were collected outside the collection window Ceoi for these samples were predicted by using a log linear model. Participants aged \< 2 years and \> 12 years were not presented as their data analysis resulted in a different measure type and method of dispersion.
Ceoi of Plasma Letermovir Taken as IV Formulation by Ages <2 Years	Day 7: Pre-dose, 1, 2.5, 8, and 24 hours post-dose	Blood was collected on treatment Day 7 from participants aged \<2 years in order to determine the Ceoi of plasma letermovir for participants receiving IV formulation. As samples were collected outside the collection window Ceoi for these samples were predicted by using a log linear model. Participants aged \> 2 years were not presented as their data analysis resulted in a different measure type and method of dispersion. A measure of dispersion is not determined when N \<2.
Ctrough of Plasma Letermovir Taken During Sparse PK for Oral Formulation	Day 7: 24 hours post-dose	Blood was collected on treatment Day 7 in order to determine the Ctrough of plasma letermovir during sparse PK for participants receiving oral formulation. Individual values were natural log transformed and evaluated separately with a linear mixed effects model containing a fixed effect for treatment and a random effect for participant.
Area Under the Concentration-time Curve From Time 0 to 24 Hours Post-dose (AUC0-24) of Plasma Letermovir Taken as Oral Formulation by Ages 2 - <18 Years	Day 7: Pre-dose, 1, 2.5, 8, and 24 hours post-dose	Blood was collected on treatment Day 7 from participants aged 2 - \<18 years in order to determine the AUC0-24 of plasma letermovir for participants receiving oral formulation. Individual values were natural log transformed and evaluated separately with a linear mixed effects model containing a fixed effect for treatment and a random effect for participant. Participants aged \< 2 years were not presented as their data analysis resulted in a different measure type and method of dispersion.
Maximal Concentration (Cmax) of Plasma Letermovir Taken as Oral Formulation by Ages 2 - <18 Years	Day 7: Pre-dose, 1, 2.5, 8, and 24 hours post-dose	Blood was collected on treatment Day 7 from participants aged 2 - \<18 years in order to determine the Cmax of plasma letermovir for participants receiving oral formulation. Individual values were natural log transformed and evaluated separately with a linear mixed effects model containing a fixed effect for treatment and a random effect for participant. Participants aged \< 2 years were not presented as their data analysis resulted in a different measure type and method of dispersion.
Ctrough of Plasma Letermovir Taken as IV Formulation by Ages 2 to <12 Years	Day 7: Pre-dose, 1, 2.5, 8, and 24 hours post-dose	Blood was collected on treatment Day 7 from participants aged \<2 years in order to determine the Ctrough of plasma letermovir for participants receiving IV formulation. Individual values were natural log transformed and evaluated separately with a linear mixed effects model containing a fixed effect for treatment and a random effect for participant. Participants aged \> 2 years were not presented as their data analysis resulted in a different measure type and method of dispersion. The measure of dispersion is not determined when N \<2.

Secondary Outcome Measures

Name	Time	Method
Percentage of Participants Who Discontinued Study Medication Due to an AE.	Up to Week 14 post-transplant (up to 18 weeks)	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. An AE can therefore be any unfavorable and unintended sign (including an abnormal laboratory finding), symptom, or disease (new or exacerbated) temporally associated with the use of a study intervention. The 95% CI is based on the exact binomial method proposed by Clopper and Pearson.
Number of Participants Receiving Oral Granules With Palatability Response, Based on Taste of Medication on the First Day of Administration of Oral Formulation	Day 1 of administration of oral formulation up to Week 14 post-transplant (up to 18 weeks)	Palatability was measured by response to a questionnaire on the taste of medication , with responses from very good, good, neither good nor bad, bad or very bad.
Percentage of Participants With One or More Adverse Event (AE)	Up to Week 48 post-transplant (up to 52 weeks)	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. An AE can therefore be any unfavorable and unintended sign (including an abnormal laboratory finding), symptom, or disease (new or exacerbated) temporally associated with the use of a study intervention. The 95% confidence interval (CI) is based on the exact binomial method proposed by Clopper and Pearson.
Percentage of Participants With Clinically Significant CMV Infection Through Week 14 Post-transplant	Up to Week 14 post-transplant (up to 18 weeks)	Clinically significant cytomegalovirus (CMV) infection is defined as CMV end organ disease (proven or probable) or initiation of pre-emptive therapy (PET) based on documented CMV viremia and the clinical condition of the participant. The 95% confidence interval (CI) was based on the exact binomial method proposed by Clopper and Pearson. Missing values: were handled by the Non-Completer=Failure (NC=F) approach. where failure was defined as all participants who developed clinically significant CMV infection or prematurely discontinued from the study or had a missing outcome through week 14 post-transplant visit window.
Number of Participants Receiving Oral Granules With Palatability Response, Based on Taste of Medication on the Eighth Day of Administration of Oral Formulation	Day 8 of administration of oral formulation up to Week 14 post-transplant (up to 18 weeks)	Palatability was measured by response to a questionnaire on the taste of medication , with responses from very good, good, neither good nor bad, bad or very bad.
Percentage of Participants With Clinically Significant CMV Infection Through Week 24 Post-transplant	Up to Week 24 post-transplant (up to 28 weeks)	Clinically significant CMV infection is defined as CMV end organ disease (proven or probable) or initiation of PET based on documented CMV viremia and the clinical condition of the participant. The 95% confidence interval (CI) was based on the exact binomial method proposed by Clopper and Pearson. Missing values: were handled by the Non-Completer=Failure (NC=F) approach. where failure was defined as all participants who developed clinically significant CMV infection or prematurely discontinued from the study or had a missing outcome through week 24 post-transplant visit window.

Trial Locations

Locations (40)

Seattle Childrens Hospital ( Site 0248); 🇺🇸 Seattle, Washington, United States

UCSF Benioff Children's Hospital San Francisco ( Site 0245); 🇺🇸 San Francisco, California, United States

Pediatric Hemato Oncology Safra Children's Hospital, Sheba Medical Center ( Site 0123); 🇮🇱 Ramat Gan, Israel

Royal Childrens Hospital Melbourne ( Site 0181); 🇦🇺 Parkville, Victoria, Australia

Rambam Medical Center ( Site 0121); 🇮🇱 Haifa, Israel

Schneider Children's Medical Center ( Site 0122); 🇮🇱 Petah Tikva, Israel

Saitama Children's Medical Center ( Site 0202); 🇯🇵 Saitama, Japan

Hospital Infantil de Mexico ( Site 0221); 🇲🇽 Mexico City, Distrito Federal, Mexico

Boston Children's Hospital ( Site 0243); 🇺🇸 Boston, Massachusetts, United States

Uniwersytecki Szpital Kliniczny im. Jana Mikulicza-Radeckieg-Klinika Transplantacji Szpiku, Onkolog; 🇵🇱 Wrocław, Dolnoslaskie, Poland

Acibadem Adana Hastanesi ( Site 0162); 🇹🇷 Adana, Turkey

Fundacion Valle del Lili ( Site 0212); 🇨🇴 Cali, Valle Del Cauca, Colombia

Centro Medico Imbanaco de Cali S.A ( Site 0211); 🇨🇴 Cali, Valle Del Cauca, Colombia

Instituto Nacional de Pediatria ( Site 0224); 🇲🇽 Mexico City, Distrito Federal, Mexico

Szpital Uniwersytecki nr 1 im. Dr. Antoniego Jurasza w Bydgoszczy ( Site 0141); 🇵🇱 Bydgoszcz, Kujawsko-pomorskie, Poland

Akdeniz University Faculty of Medicine ( Site 0161); 🇹🇷 Antalya, Turkey

Ege Univ.Tip Fakultesi Cocuk Has ( Site 0163); 🇹🇷 Izmir, Turkey

City of Hope Comprehensive Cancer Center ( Site 0251); 🇺🇸 Duarte, California, United States

Children's Hospital of Orange County ( Site 0241); 🇺🇸 Orange, California, United States

University Of Chicago School Of Medicine ( Site 0253); 🇺🇸 Chicago, Illinois, United States

Cincinnati Children's Hospital Medical Center ( Site 0244); 🇺🇸 Cincinnati, Ohio, United States

Memorial Sloan Kettering Cancer Center ( Site 0254); 🇺🇸 New York, New York, United States

Children's Hospital of Pittsburgh of UPMC ( Site 0258); 🇺🇸 Pittsburgh, Pennsylvania, United States

Children's Medical Center ( Site 0257); 🇺🇸 Dallas, Texas, United States

Duke University Health System ( Site 0252); 🇺🇸 Durham, North Carolina, United States

The Children s Hospital at Westmead ( Site 0185); 🇦🇺 Westmead, New South Wales, Australia

Lady Cilento Children s Hospital ( Site 0182); 🇦🇺 South Brisbane, Queensland, Australia

Universitaetsklinikum Muenster ( Site 0114); 🇩🇪 Muenster, Nordrhein-Westfalen, Germany

Instituto De Cancerologia S.A. ( Site 0213); 🇨🇴 Medellin, Antioquia, Colombia

Universitaetsklinikum Frankfurt ( Site 0112); 🇩🇪 Frankfurt, Hessen, Germany

Hôpital Universitaire Necker Enfants Malades-, Unite d'Immunologie-Hematologie et Rhumatologie Pedi; 🇫🇷 Paris, France

Charite Universitaetsmedizin Berlin - Campus-Virchow-Klinikum ( Site 0113); 🇩🇪 Berlin, Germany

Universitatsklinikum Hamburg-Eppendorf ( Site 0111); 🇩🇪 Hamburg, Germany

National Center for Child Health and Development ( Site 0201); 🇯🇵 Tokyo, Japan

Nuevo Hospital Civil Dr Juan I Menchaca ( Site 0223); 🇲🇽 Guadalajara, Jalisco, Mexico

Hospital Universitario "Dr. Jose Eleuterio Gonzalez" ( Site 0222); 🇲🇽 Monterrey, Nuevo Leon, Mexico

H. de la Santa Creu I Sant Pau ( Site 0155); 🇪🇸 Barcelona, Spain

Hospital Universitari Vall d Hebron ( Site 0154); 🇪🇸 Barcelona, Spain

Hospital Infantil Universitario Nino Jesus ( Site 0151); 🇪🇸 Madrid, Spain

Hospital Universitario La Paz ( Site 0153); 🇪🇸 Madrid, Spain