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Pharmacogenomic Biomarker Study for Recombinant Human Activated Protein C Treatment in Severe Sepsis

5 декабря 2011 г. обновлено: Sirius Genomics Inc.

A Multicenter Pharmacogenomic Biomarker Study in Matched Patients With Severe Sepsis Treated With or Without Recombinant Human Activated Protein C [Xigris®, Drotrecogin Alfa (Activated)]

The overall purpose of the study is to determine whether either of the Improved Response Polymorphisms (IRPs) individually predicts a differential DrotAA treatment effect in patients with severe sepsis and high risk of death. This will be an international, multicenter, "prospective-retrospective", nonrandomized, controlled, outcome-blinded, genotype-blinded, matched-patients study. No prospective enrollment or treatment of patients will occur under this protocol. Retrospectively collected clinical data and DNA samples will be analyzed for existing cohorts of patients with severe sepsis who were previously treated with DrotAA (treatment group) or not (control group) as part of their standard care in an ICU.

Обзор исследования

Статус

Неизвестный

Условия

Подробное описание

This will be a multicenter, "prospective-retrospective", controlled, matched-patients study. Retrospective phenotypic data and DNA samples will be obtained from patient registries and clinical trials where the study hypotheses were not related to DrotAA treatment. The prospective aspect of this study will be the statistical testing of prespecified hypotheses regarding the IRP genotype as a predictive biomarker for differential DrotAA treatment effects.

To control for differences in standard of care in different countries and medical centers, the selection of matched control patients will be performed within each cohort. Control patients will be selected to match the DrotAA-treated patients using an algorithm that matches on baseline demographic and disease characteristics that may have influenced the decision to give DrotAA or that may impact survival. A propensity score (the likelihood for having received DrotAA treatment) will be derived using the matching variables that are common in all cohorts. The number of matched control patients for each treated patient will be variable, up to a maximum of 3.

The selection of the control patients via the matching algorithm will be conducted by an independent clinical research organization (CRO) in a blinded manner - specifically without knowledge of survival outcome, other outcome data, and genotype. A two-phase transfer of data from each center will be implemented to ensure that the selection of matched control patients is implemented in a blinded manner. The first step will involve the transfer of the baseline data for all variables needed to conduct the matching. Once the control patients have been identified for each cohort, the outcomes data will be transferred to the CRO in the second phase of data transfer.

Centralized genotyping using a validated Taqman®-based analytical method will be conducted on the DNA samples for all matched patients. The genotyping laboratory will be blinded to treatment and outcome.

The total number of patients in the available cohorts is >23,000, with approximately 800 who have received DrotAA as part of their standard ICU-based care. After applying eligibility criteria to all patients and selecting the matched control patients, it is expected that the final analysis will include approximately 3000 patients.

Тип исследования

Наблюдательный

Регистрация (Ожидаемый)

3000

Контакты и местонахождение

В этом разделе приведены контактные данные лиц, проводящих исследование, и информация о том, где проводится это исследование.

Места учебы

Канада
- British Columbia
  - Vancouver, British Columbia, Канада, V6Z 1Y6
    - University of British Columbia and Providence Health Care, St. Paul's Hospital
Соединенное Королевство
- - London, Соединенное Королевство, W6 8RF
    - Imperial College London, Charing Cross Hospital
Соединенные Штаты
- Georgia
  - Atlanta, Georgia, Соединенные Штаты, 30322
    - Emory University School of Medicine
- Maryland
  - Baltimore, Maryland, Соединенные Штаты, 21224
    - Johns Hopkins University, Bayview Medical Center
- Massachusetts
  - Boston, Massachusetts, Соединенные Штаты, 02115
    - Harvard University School of Public Health
- Tennessee
  - Nashville, Tennessee, Соединенные Штаты, 73232-2650
    - Vanderbilt University Schoo of Medicine
Франция
- - Garches, Франция, 92380
    - University of Versailles, Hospital Raymond Poincaré (AP-HP)
  - Paris, Франция, 75014
    - Université Paris Descartes, Sorbonne Paris Cité, Cochin Hotel-Dieu University Hospital

Критерии участия

Исследователи ищут людей, которые соответствуют определенному описанию, называемому критериям приемлемости. Некоторыми примерами этих критериев являются общее состояние здоровья человека или предшествующее лечение.

Критерии приемлемости

Возраст, подходящий для обучения

18 лет и старше (Взрослый, Пожилой взрослый)

Принимает здоровых добровольцев

Нет

Полы, имеющие право на обучение

Все

Метод выборки

Невероятностная выборка

Исследуемая популяция

The indicated-patients population (INDICATED) population will be the primary population for this study and it will include those DrotAA-treated patients who have documented severe sepsis and high risk of death, defined in keeping with the regulatory approvals in the EU and US, and their matched controls. Documented organ dysfunction will be defined according to published criteria. A secondary severe sepsis population (SEVSEP) will have had documented severe sepsis, but not necessarily a high risk of death. The INDICATED population will be a subset within the broader SEVSEP population.The SEVSEP population will be analyzed only if at least 10% larger than the INDICATED population.

Описание

Inclusion Criteria for INDICATED population:

Age ≥ 18 years
Severe sepsis (must meet a, b, and c below)
- Suspected or proven infection
- Systemic Inflammatory Response Syndrome (SIRS)(must meet 2 of 4 criteria)
  - Temperature < 36°C or > 38°C
  - Heart rate > 90 beats/minute
  - Respiratory rate > 20 breaths/minute or PaC02 < 32 mm Hg) or on mechanical ventilation
  - White blood cell count < 4,000/mm3 or > 12,000/mm3
- At least one organ dysfunction due to sepsis based on definitions of clinically significant organ dysfunction
  - Cardiovascular dysfunction [must meet one of (1), (2), or (3) below]:
    - Systolic blood pressure ≤ 90 mmHg and pH ≤ 7.3
    - Mean arterial pressure ≤ 70 mmHg and pH ≤ 7.3
    - Reported use of a vasopressor alone is sufficient evidence of shock
  - Pulmonary dysfunction: PaO2/FiO2 ≤ 300 mmHg
  - Central Nervous System dysfunction: Glasgow Coma Scale ≤ 12
  - Coagulation dysfunction: platelets ≤ 80,000/mm3
  - Renal dysfunction: creatinine ≥ 2.0 mg/dL
  - Hepatic dysfunction: bilirubin ≥ 2.0 mg/dL
High risk of death (one of a, b, or c below)
- APACHE II ≥ 25
- SAPS II ≥ 54
- Multiple organ dysfunction - two or more clinically significant organ dysfunctions (as defined above), which have occurred within 2 days of each other
Platelet counts ≥ 30,000/mm3
DrotAA status known

Exclusion Criteria:

Patients with no DNA
Patients enrolled in local cohort more than 2 years before Xigris [drotrecogin alfa activated)] was commercially available

A secondary analysis population with severe sepsis will be defined by Inclusion Criteria 1, 2, 4, and 5 above, and the Exclusion Criteria. This will be referred to as the SEVSEP population.

Учебный план

В этом разделе представлена подробная информация о плане исследования, в том числе о том, как планируется исследование и что оно измеряет.

Как устроено исследование?

Детали дизайна

Количество групп / когорт

Когорты и вмешательства

Группа / когорта
DrotAA Treatment Group Patients with severe sepsis at high risk of death (INDICATED patients) who received treatment with drotrecogin alfa (activated (DrotAA) as part of standard care in ICU. The standard dosing regimen for DrotAA is 96 hours of continuous infusion at a dose of 24 ug/kg/hour. DrotAA is also known as recombinant human activated protein C.
Control Group (non-DrotAA treated) Patients with severe sepsis at high risk of death (INDICATED patients) who did not receive DrotAA treatment as part of their standard care in an ICU. The Control group patients will be selected to match the DrotAA-treated patients based on numerous clinical covariates, including propensity score (for DrotAA treatment).

Что измеряет исследование?

Первичные показатели результатов

Мера результата	Мера Описание	Временное ограничение
In-hospital mortality through Day 28 Временное ограничение: Through Day 28.	All cause in-hospital mortality up to Day 28 or discharge, whichever comes first. Day 1 is the day when patient meets eligibility criteria for this study.	Through Day 28.

Вторичные показатели результатов

Мера результата	Мера Описание	Временное ограничение
Time to death in hospital Временное ограничение: Through Day 28	Time to death (any cause) in hospital, censored by the competing risk of discharge from hospital	Through Day 28
Time to death Временное ограничение: Through Day 60	Time to death (any cause), censored at Day 60 or last evaluation. Will be evaluated using data from centers where follow-up extended beyond hospital discharge.	Through Day 60
Mechanical ventilator-free days through Day 28 Временное ограничение: Through Day 28	Number of days alive and free of mechanical ventilation from Day 1 through Day 28.	Through Day 28
ICU-free days through Day 28 Временное ограничение: Through Day 28	Number of days alive and free of ICU from Day 1 through Day 28.	Through Day 28
Hospital-free days through Day 28 Временное ограничение: Through Day 28	Number of days alive and free of hospitalization from Day 1 through Day 28.	Through Day 28
ICU length of stay Временное ограничение: Through Day 180		Through Day 180
Hospital length of stay Временное ограничение: Through Day 180		Through Day 180

Соавторы и исследователи

Здесь вы найдете людей и организации, участвующие в этом исследовании.

Спонсор

Sirius Genomics Inc.

Следователи

Главный следователь: Djillali Annane, MD, PhD, University of Versailles
Директор по исследованиям: Alexandra DJ Mancini, MSc, Sirius Genomics Inc.

Публикации и полезные ссылки

Лицо, ответственное за внесение сведений об исследовании, добровольно предоставляет эти публикации. Это может быть что угодно, связанное с исследованием.

Общие публикации

Annane D, Mira JP, Ware LB, Gordon AC, Hinds CJ, Christiani DC, Sevransky J, Barnes K, Buchman TG, Heagerty PJ, Balshaw R, Lesnikova N, de Nobrega K, Wellman HF, Neira M, Mancini ADJ, Walley KR, Russell JA. Pharmacogenomic biomarkers do not predict response to drotrecogin alfa in patients with severe sepsis. Ann Intensive Care. 2018 Jan 31;8(1):16. doi: 10.1186/s13613-018-0353-2.

Даты записи исследования

Эти даты отслеживают ход отправки отчетов об исследованиях и сводных результатов на сайт ClinicalTrials.gov. Записи исследований и сообщаемые результаты проверяются Национальной медицинской библиотекой (NLM), чтобы убедиться, что они соответствуют определенным стандартам контроля качества, прежде чем публиковать их на общедоступном веб-сайте.

Изучение основных дат

Начало исследования

1 октября 2011 г.

Первичное завершение (Ожидаемый)

1 апреля 2012 г.

Завершение исследования (Ожидаемый)

1 апреля 2012 г.

Даты регистрации исследования

Первый отправленный

2 декабря 2011 г.

Впервые представлено, что соответствует критериям контроля качества

5 декабря 2011 г.

Первый опубликованный (Оценивать)

6 декабря 2011 г.

Обновления учебных записей

Последнее опубликованное обновление (Оценивать)