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NCT01379703 Clinical Trial

Multicountry, Multicenter Post-Marketing Observational Study of Clinical, Biological and Virological Outcomes, Compliance and Tolerability of Kaletra® in Routine Clinical Use

HIV-1 Patients Clinical Trial

KaleEAST

Official title:
Multicountry, Multicenter Post-Marketing Observational Study of Clinical, Biological and Virological Outcomes, Compliance and Tolerability of Kaletra® in Routine Clinical Use

Clinical Trial Details — Status: Completed

Administrative data
NCT number NCT01379703
Other study ID # PMOS-EAST-04-1
Secondary ID
Status Completed
Phase N/A
First received June 22, 2011
Last updated October 10, 2011
Start date February 2004
Est. completion date February 2010

Study information
Verified date October 2011
Source Abbott
Contact n/a
Is FDA regulated No
Health authority Romania: Ethics CommitteeRomania: National Medicines AgencyPoland: Office for Registration of Medicinal Products, Medical Devices and Biocidal ProductsSerbia: Ethics CommitteeIsrael: Ethics CommissionIsrael: Ministry of HealthSlovenia: Ethics CommitteeSlovak Republic: Ethics CommitteeCzech Republic: State Institute for Drug ControlLatvia: Institutional Review BoardLatvia: State Agency of MedicinesLithuania: Bioethics CommitteeLithuania: State Medicine Control Agency - Ministry of Health
Study type Observational

Clinical Trial Summary

KaleEAST is a non-interventional, post-marketing observational study (PMOS) in which lopinavir/ritonavir is prescribed in the usual manner in accordance with the terms of the local marketing authorization with regards to dose, population and indication. No additional procedures (other than the standard of care) are to be applied to the patients.

The KaleEAST PMOS was conducted in a prospective, single-arm, multicountry, multicenter format. The study was carried out in two (2) parts: the first part was initiated in 2004 with the lopinavir/ritonavir capsule formulation, the second part started in 2006 after the lopinavir/ritonavir tablets had become available in the participating countries.

The aim of this post-marketing observational study was to obtain further data on clinical, biological, and virological outcomes, compliance and tolerability of Kaletra®-containing regimen during routine clinical use in the participating countries.

Description:

As this study is observational in nature, subject follow-up was not specified by the protocol but was left to the judgment of each physician within the 18 months period, which defines the survey for each participant. For indicative purposes, follow-up of each participant should enable approximately 7 visits during this period. These visits will take place at average intervals of 3 months, apart from the first visit following inclusion (usually at the end of the first treatment month) and apart from visits required because of intercurrent events. Participant visits were assigned as follows: Baseline/Day 0 (start of lopinavir/ritonavir treatment), Month 1 (day 1 to day 45), Month 3 (day 46 to day 136), Month 6 (day 137 to day 228), Month 9 (day 229 to day 319), Month 12 (day 320 to day 410), Month 15 (day 411 to day 501), Month 18 (day 502 to day 593). Each participant is planned to be observed during his/her lopinavir/ritonavir capsule containing treatment regimen for a maximum period of 18 months, and each participant is planned to be observed during his/her lopinavir/ritonavir tablet containing treatment regimen for a maximum period of 9 months.

Recruitment information / eligibility
Status Completed
Enrollment 2288
Est. completion date February 2010
Est. primary completion date February 2010
Accepts healthy volunteers No
Gender Both
Age group 2 Years and older
Eligibility Inclusion Criteria:

Patients infected by HIV-1 infection who are either:

- Antiretroviral treatment (ART) naive or

- Had failed or had been intolerant to one previous combined antiretroviral treatment (cART), not including a Protease inhibitor (PI) (first-line pretreated without a Protease inhibitor) or

- Had failed or had been intolerant to one previous antiretroviral treatment ART, including one Protease inhibitor (first-line pretreated with a Protease Inhibitor).

A ritonavir-boosted Protease inhibitor PI is considered as treatment with one Protease inhibitor PI.

Exclusion Criteria:

- Treatment with drugs at risk for interactions with lopinavir/ritonavir

- Uncontrolled AIDS defining disease

- Two or more previous Protease inhibitors (PIs)

- Participation in another study or clinical trial

Study Design

Time Perspective: Prospective

Related Conditions & MeSH terms

Locations
Country Name City State
Czech Republic Site Ref # / Investigator 57102 Brno
Czech Republic Site Ref # / Investigator 57054 Ceske Budejovice
Czech Republic Site Ref # / Investigator 57055 Hradec Kralove
Czech Republic Site Ref # / Investigator 57056 Ostrava
Czech Republic Site Ref # / Investigator 57052 Plzen
Czech Republic Site Ref # / Investigator 5344 Prague 8
Czech Republic Site Ref # / Investigator 57053 Usti nad Labem
Georgia Site Ref # / Investigator 7576 Tbilisi
Israel Site Ref # / Investigator 57050 Beer-Sheva
Israel Site Ref # / Investigator 57048 Haifa
Israel Site Ref # / Investigator 57049 Jerusalem
Israel Site Ref # / Investigator 6124 Kfar Saba
Israel Site Ref # / Investigator 57047 Rechovot
Israel Site Ref # / Investigator 57051 Tel-Hashomer
Latvia Site Ref # / Investigator 7578 Riga
Lithuania Site Ref # / Investigator 6127 Vilnius
Poland Site Ref # / Investigator 6190 Bialystok
Poland Site Ref # / Investigator 56885 Bydgoszcz
Poland Site Ref # / Investigator 56887 Chorzow
Poland Site Ref # / Investigator 56883 Gdansk
Poland Site Ref # / Investigator 56888 Krakow
Poland Site Ref # / Investigator 56889 Lodz
Poland Site Ref # / Investigator 56884 Poznan
Poland Site Ref # / Investigator 56886 Szczecin
Poland Site Ref # / Investigator 56882 Warsaw
Poland Site Ref # / Investigator 56890 Wroclaw
Romania Site Ref # / Investigator 57064 Brasov
Romania Site Ref # / Investigator 57062 Bucharest
Romania Site Ref # / Investigator 6194 Bucharest
Romania Site Ref # / Investigator 57063 Constanta
Romania Site Ref # / Investigator 57067 Craiova
Romania Site Ref # / Investigator 57068 Iasi
Romania Site Ref # / Investigator 57065 Targu Mures
Romania Site Ref # / Investigator 57066 Timisoara
Russian Federation Site Ref # / Investigator 57022 Barnaul
Russian Federation Site Ref # / Investigator 56918 Chelyabinsk
Russian Federation Site Ref # / Investigator 56963 Chita
Russian Federation Site Ref # / Investigator 56903 Ekaterinburg
Russian Federation Site Ref # / Investigator 56923 Ekaterinburg
Russian Federation Site Ref # / Investigator 56921 Irkutsk
Russian Federation Site Ref #/Investigator 57104 Irkutsk
Russian Federation Site Ref # / Investigator 57028 Ivanovo
Russian Federation Site Ref # / Investigator 57036 Izhevsk
Russian Federation Site Ref # / Investigator 56945 Kaliningrad
Russian Federation Site Ref # / Investigator 56909 Kazan
Russian Federation Site Ref # / Investigator 57037 Kemerovo
Russian Federation Site Ref #/Investigator 57105 Kemerovo
Russian Federation Site Ref # / Investigator 56948 Khabarovsk
Russian Federation Site Ref # / Investigator 56932 Khanty-Mansiysk
Russian Federation Site Ref #/Investigator 57107 Kirov
Russian Federation Site Ref # / Investigator 57030 Kostroma
Russian Federation Site Ref # / Investigator 56943 Krasnodar
Russian Federation Site Ref # / Investigator 56928 Krasnoyarsk
Russian Federation Site Ref #/Investigator 57106 Krasnoyarsk
Russian Federation Site Ref # / Investigator 57021 Kurgan
Russian Federation Site Ref # / Investigator 57025 Lipetsk
Russian Federation Site Ref # / Investigator 56944 Magnitogorsk
Russian Federation Site Ref # / Investigator 56902 Moscow
Russian Federation Site Ref # / Investigator 56904 Moscow
Russian Federation Site Ref # / Investigator 6209 Moscow
Russian Federation Site Ref # / Investigator 57024 Murmansk
Russian Federation Site Ref # / Investigator 56907 Nizhniy Novgorod
Russian Federation Site Ref # / Investigator 56964 Norilsk
Russian Federation Site Ref # / Investigator 56929 Novokuznetsk
Russian Federation Site Ref # / Investigator 56942 Novosibirsk
Russian Federation Site Ref # / Investigator 56926 Noyabrsk
Russian Federation Site Ref # / Investigator 56915 Orenburg
Russian Federation Site Ref # / Investigator 57031 Orenburg
Russian Federation Site Ref # / Investigator 56930 Perm
Russian Federation Site Ref # / Investigator 56911 Rostov-on-Don
Russian Federation Site Ref # / Investigator 56905 Saint Petersburg
Russian Federation Site Ref # / Investigator 56906 Saint Petersburg
Russian Federation Site Ref # / Investigator 56931 Samara
Russian Federation Site Ref # / Investigator 56913 Saratov
Russian Federation Site Ref # / Investigator 56920 St. Petersburg
Russian Federation Site Ref # / Investigator 57033 St. Petersburg
Russian Federation Site Ref # / Investigator 57038 St. Petersburg
Russian Federation Site Ref # / Investigator 56908 Surgut
Russian Federation Site Ref # / Investigator 56962 Togliatti
Russian Federation Site Ref # / Investigator 57034 Tula
Russian Federation Site Ref # / Investigator 56947 Tver
Russian Federation Site Ref # / Investigator 57035 Tver
Russian Federation Site Ref # / Investigator 56910 Tyumen
Russian Federation Site Ref # / Investigator 56919 Tyumen
Russian Federation Site Ref # / Investigator 57029 Ufa
Russian Federation Site Ref # / Investigator 56949 Ulan-Ude
Russian Federation Site Ref # / Investigator 56914 Ulyanovsk
Russian Federation Site Ref # / Investigator 57027 Vladimir
Russian Federation Site Ref # / Investigator 56916 Volgograd
Russian Federation Site Ref #/Investigator 57103 Vologda
Russian Federation Site Ref # / Investigator 56946 Yakutsk
Russian Federation Site Ref # / Investigator 57026 Yaroslavl
Serbia Site Ref # / Investigator 7579 Belgrade
Slovakia Site Ref # / Investigator 6208 Bratislava
Slovenia Site Ref # / Investigator 6199 Ljubljana
Ukraine Site Ref # / Investigator 57042 Dnepropetrovsk
Ukraine Site Ref # / Investigator 57043 Donetsk
Ukraine Site Ref # / Investigator 57045 Kyiv
Ukraine Site Ref # / Investigator 57046 Kyiv
Ukraine Site Ref # / Investigator 6191 Kyiv
Ukraine Site Ref # / Investigator 57044 Mykolaiv
Ukraine Site Ref # / Investigator 57039 Odessa
Ukraine Site Ref # / Investigator 57040 Simferopol

Sponsors (1)
Lead Sponsor Collaborator
Abbott

Countries where clinical trial is conducted

Czech Republic,  Georgia,  Israel,  Latvia,  Lithuania,  Poland,  Romania,  Russian Federation,  Serbia,  Slovakia,  Slovenia,  Ukraine, 

Outcome
Type Measure Description Time frame Safety issue
Primary CD4 Count CD4 lymphocyte count is a measure of a participant's immunologic health. Participants' CD4-positive (CD4+) T-lymphocyte counts were assessed by measuring the number of CD4+ cells at baseline. Baseline No
Primary Changes in CD4 Count Increases in CD4 count are a biomarker for antiretroviral treatment effectiveness in restoring immunologic function. Changes in participants' CD4-positive (CD4+) T-lymphocyte counts were assessed by measuring the change from Baseline in the number of CD4+ cells at scheduled study visits. Baseline to 1 month No
Primary Changes in CD4 Count Increases in CD4 count are a biomarker for antiretroviral treatment effectiveness in restoring immunologic function. Changes in participants' CD4-positive (CD4+) T-lymphocyte counts were assessed by measuring the change from Baseline in the number of CD4+ cells at scheduled study visits. Baseline to 3 months No
Primary Changes in CD4 Count Increases in CD4 count are a biomarker for antiretroviral treatment effectiveness in restoring immunologic function. Changes in participants' CD4-positive (CD4+) T-lymphocyte counts were assessed by measuring the change from Baseline in the number of CD4+ cells at scheduled study visits. Baseline to 6 months No
Primary Changes in CD4 Count Increases in CD4 count are a biomarker for antiretroviral treatment effectiveness in restoring immunologic function. Changes in participants' CD4-positive (CD4+) T-lymphocyte counts were assessed by measuring the change from Baseline in the number of CD4+ cells at scheduled study visits. Baseline to 9 months No
Primary Changes in CD4 Count Increases in CD4 count are a biomarker for antiretroviral treatment effectiveness in restoring immunologic function. Changes in participants' CD4-positive (CD4+) T-lymphocyte counts were assessed by measuring the change from Baseline in the number of CD4+ cells at scheduled study visits. Baseline to 12 months No
Primary Changes in CD4 Count Increases in CD4 count are a biomarker for antiretroviral treatment effectiveness in restoring immunologic function. Changes in participants' CD4-positive (CD4+) T-lymphocyte counts were assessed by measuring the change from Baseline in the number of CD4+ cells at scheduled study visits. Baseline to 15 months No
Primary Changes in CD4 Count Increases in CD4 count are a biomarker for antiretroviral treatment effectiveness in restoring immunologic function. Changes in participants' CD4-positive (CD4+) T-lymphocyte counts were assessed by measuring the change from Baseline in the number of CD4+ cells at scheduled study visits. Baseline to 18 months No
Primary Viral Load Viral load is a direct measure of the viral burden by providing a count of the number of HIV-RNA copies in blood (plasma). The number of HIV-RNA copies in the blood was measured at baseline. Baseline No
Primary Viral Load Viral load (number of HIV-RNA copies in the blood) was measured at baseline and scheduled study visits. A decrease in viral load is a measure used to assess the effectiveness of antiviral treatments. 1 month No
Primary Viral Load Viral load (number of HIV-RNA copies in the blood) was measured at baseline and scheduled study visits. A decrease in viral load is a measure used to assess the effectiveness of antiviral treatments. 3 months No
Primary Viral Load Viral load (number of HIV-RNA copies in the blood) was measured at baseline and scheduled study visits. A decrease in viral load is a measure used to assess the effectiveness of antiviral treatments. 6 months No
Primary Viral Load Viral load (number of HIV-RNA copies in the blood) was measured at baseline and scheduled study visits. A decrease in viral load is a measure used to assess the effectiveness of antiviral treatments. 9 months No
Primary Viral Load Viral load (number of HIV-RNA copies in the blood) was measured at baseline and scheduled study visits. A decrease in viral load is a measure used to assess the effectiveness of antiviral treatments. 12 months No
Primary Viral Load Viral load (number of HIV-RNA copies in the blood) was measured at baseline and scheduled study visits. A decrease in viral load is a measure used to assess the effectiveness of antiviral treatments. 15 months No
Primary Viral Load Viral load (number of HIV-RNA copies in the blood) was measured at baseline and scheduled study visits. A decrease in viral load is a measure used to assess the effectiveness of antiviral treatments. 18 months No
Primary Laboratory Parameter Blood Glucose Blood glucose laboratory values were assessed at baseline and scheduled study visits. Normal ranges are based on the standards for individual facilities in each country. Baseline, 9 months, 18 months No
Primary Laboratory Parameter Transaminases Serum aspartate aminotransferase (AST) and alanine aminotransferase (ALT) laboratory values were assessed at baseline and scheduled study visits. Normal ranges are based on the standards for individual facilities in each country. Baseline, 9 months, 18 months No
Primary Laboratory Parameter Lipids A blood lipid panel consisting of total cholesterol, triglyceride, high-density lipoprotein (HDL), and low-density lipoprotein (LDL) levels was performed at baseline and scheduled study visits. Normal ranges are based on the standards for individual facilities in each country. Baseline, 9 months, 18 months No
Secondary Reasons for Discontinuation of Lopinavir/Ritonavir For participants who discontinued lopinavir/ritonavir treatment, the reasons for discontinuation are provided. 9 months No
Secondary Reasons for Discontinuation of Lopinavir/Ritonavir For participants who discontinued lopinavir/ritonavir treatment, the reasons for discontinuation are provided. 18 months No
Secondary Compliance With Lopinavir/Ritonavir Participants reported whether they had missed doses of their antiretroviral treatment. 9 months No
Secondary Compliance With Lopinavir/Ritonavir Participants reported whether they had missed any doses of their antiretroviral treatment. 18 months No
Secondary Adverse Events Observed on Treatment With Lopinavir/Ritonavir. Total number of adverse events with causal relationship (rated by Investigator as probably or possibly related) to lopinavir/ritonavir treatment.
All serious adverse events and non serious adverse events (0.2% or greater frequency) are summarized in the "Reported Adverse Events" section of this record.		 18 months No