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Clinical Trial Details — Status: Terminated

Administrative data

NCT number NCT01567956
Other study ID # ST261DM11006
Secondary ID 2011-004770-28
Status Terminated
Phase Phase 3
First received March 28, 2012
Last updated November 4, 2016
Start date April 2012
Est. completion date January 2014

Study information

Verified date April 2014
Source sigma-tau i.f.r. S.p.A.
Contact n/a
Is FDA regulated No
Health authority Germany: Federal Institute for Drugs and Medical Devices
Study type Interventional

Clinical Trial Summary

The aim of the trial is to test safety, tolerability and efficacy of Propionyl-L-carnitine modified release tablets 1g/die in reducing the symptoms of the disease with respect to the proportion of patients with disease remission at the end of the 8 weeks of treatment. It will also aim to investigate capability of the treatment in the maintenance of remission after four weeks of treatment interruption; histological changes will be also evaluated and finally, improvement in the overall quality of life as measured by the Short Inflammatory Bowel Disease Questionnaire (SIBDQ) will be investigated.


Description:

Although it seems clear that an abnormal function of the colonic epithelium is the central problem causing inflammation and the unusual immunological response to the normal gut flora in inflammatory bowel disease (IBD), the actual causes of these dysfunctions are still unknown. Short Chain Fatty Acids (SCFA) are the main fuel of the colonic epithelium, and are normally produced by the bacterial flora by fermentation of the complex carbohydrates forming non soluble fibers usually introduced with everyday diet. Butyrate alone contributes 70% of the normal colonocyte energy. Studies done using animal models and colonic mucosa biopsies from patients suffering form ulcerative colitis (UC) have consistently shown that a metabolic change occurs in diseased colonic mucosa, with an impairment of butyrate oxidation (and of beta-oxidation) and an energy shortage that is only incompletely compensated by oxidation of glucose and other substrates such as glutamine. It is also well known that matrix metalloproteases production is highly increased in IBD and that serum transglutaminase activity is significantly reduced in patients with IBD. Transglutaminases are enzymes contributing to the crosslinking of matrix proteins and the reduction seen in patients affected by IBD correlates well with the endoscopic and histopathologic grading in UC, meaning that part of the circulating enzyme is sequestered in the injured colonic tissue in the effort to re-build the extracellular matrix during the healing process. Propionyl-L-carnitine Hydrochloride (PLC) is a molecule that has already been shown to reduce membrane lipid peroxidation in endothelial cells from bovine aorta and coronary vessels, to reduce the effects of hypoxia in coronary endothelial cells, and to play a role in the cardiac metabolic abnormalities that contribute to the mechanical dysfunctions leading to heart failure. Given these properties of Propionyl-L-carnitine Hydrochloride (ST 261) and given the peroxidative damage suffered by colonocytes in UC together with their metabolic impairment, the use of this molecule for the treatment of UC seemed to be appropriate and sound, in particular as a carrier of a propionate moiety that, once transformed into succinate, enters the Kreb cycle, acting as an extra burst fuel improving the balance of energy production inside tissues. Previous clinical experience has shown that PLC promoted complete or nearly complete regression of cutaneous trophic ulcers in a large number of vasculopathic patients refractory to all other therapies. As far as the UC pathology is concerned, the effects of ST 261, given orally or intrarectally, were investigated at different dosages, in preclinical experimentation, either after a single trinitrobenzene sulphonic acid (TNBS) administration (acute colitis) or after repeated TNBS administrations (reactivated colitis). The results showed a reduction in the damaged colon area both in acute model and reactivated colitis, even if the beneficial effect of restoration of TNBS-induced alterations of tissue morphology is more evident in the reactivated colitis model, particularly after oral administration. Based on the above-described results a development plan in humans started to investigate the activity of PLC in the treatment of ulcerative colitis.


Recruitment information / eligibility

Status Terminated
Enrollment 150
Est. completion date January 2014
Est. primary completion date October 2013
Accepts healthy volunteers No
Gender Both
Age group 18 Years to 75 Years
Eligibility Inclusion Criteria:

- Have read the Information for the Patient and signed the Informed Consent Form.

- Diagnosis of active ulcerative colitis since at least 4 weeks as confirmed endoscopically and histologically.

- Disease Activity Index comprised between 3 and 6, inclusive (mild ulcerative colitis), with rectal bleeding sub-score of at least 1.

- Stable background oral aminosalicylates (mesalazine, balsalazide, olsalazine) or sulfasalazine standard therapy for greater than or equal to 4 weeks prior to screening assessments.

- If female, not pregnant or nursing. For women of childbearing potential, willingness to avoid a pregnancy during the treatment period and for at least 4 weeks from the last dose of drug and utilization of an efficient method of birth control for the entire duration of the trial and until the first menses after a 30-day period after the last dose of trial medication.

Exclusion Criteria:

- Crohn's disease and indeterminate colitis.

- Current or previous (in the last 10 days preceding the screening) use of systemic corticosteroids.

- Use of systemic antibiotics in the last 10 days preceding the screening.

- Use of systemic Nonsteroidal anti-inflammatory drugs on a repeat basis in the last 10 days preceding the screening.

- Use of probiotics started within 10 days preceding the screening. A stable regimen from at least 10 days prior to screening is allowed but the patient must be willing to continue up to the end of the study.

- Use of immunosuppressants or biological agents within the last 6 weeks preceding the screening.

- Treatment with L-carnitine or its esters derivatives within the last 3 months.

- Stool culture positive for enteric pathogens (eg, Shigella, Salmonella, Yersinia, Campylobacter) or toxins (C.difficile).

- Significantly impaired liver, renal, pulmonary or cardiovascular function as assessed by the investigator.

- History of colon resection.

- Diverticulitis, symptomatic diverticulosis.

- Active peptic ulcer disease.

- Proctitis (extent of inflammation < 15 cm from the anus).

- Bleeding disorders

- Rectal therapy with any therapeutic enemas or suppositories with the exception of those required for endoscopy during the 10 days preceding the screening.

- Active or chronic infection(s) or malignancies.

- Known hypersensitivity to the active ingredient and excipients of the study drug

- Patients treated with L-Carnitine or its esters derivatives during the 3 months preceding the screening phase.

Study Design

Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Treatment


Related Conditions & MeSH terms


Intervention

Drug:
Propionyl-L-Carnitine
500 mg modified release tablets, 500 mg bid; treatment duration 8 weeks
Placebo
500 mg inert substances modified release tablets, 500 mg bid; treatment duration 8 weeks

Locations

Country Name City State
Austria Landeskrankenhaus-Universitätskliniken Innsbruck - Klinische Abteilung für Gastroenterologie und Hepatologie Innsbruck
Austria Krankenhaus der Barmherzigen Brüder - Abteilung für Innere Medizin Salzburg
Austria Ordinationszentrum Döbling Vienna
Austria Allgemeines Krankenhaus Wien - Universitätsklinik Klinik für Innere Medizin III Wien
France Centre Hospitalier Intercommunal Créteil 40 avenue de Verdun Creteil
France Centre Hospitalier Universitaire Hôpital Nord - Service D'Hépato-Gastro-Entérologie Marseille
France Centre Hospitalier Universitaire Hotel Dieu Service d'hépato-gastroentérologie Nantes
France Hôpital de I´Archet 2 Service d'Hépato-Gastroentérologie et de Nutrition Clinicque, Pôle Digestif Nice cedex 3
France Hôpital Nord - Dept. of Gastroenterology Picardie
France Hôpital Robert Debré Service et Consultation d'Hépato-Gastro-Entérologie Reims cedex
France Hopital Nord - CHU de Saint-Etienne Service de Gastro-Entérologie Saint-Etienne
France Hôpital Rangueil Service de gastro-enterologie Toulouse Cedex 4
France Hôpital Brabois Service de gastro-enterologie Vandoeuvre Les Nancy Cedex
Germany Charité Universitätsmedizin Berlin Universitätsklinik Charité, Campus Mitte Medizinische Poliklinik Berlin
Germany Saint Josef Hospital Ruhr Universitaet Bochum Gudrunstraße 56 Bochum
Germany Klinikum Braunschweig Braunschweig
Germany Universitätsklinikum Dresden Medizinische Klinik und Poliklinik I Dresden
Germany Universtätsklinikum Schleswig-Holstein Gastroenterologie Lübeck
Germany Universitätsklinikum Magdeburg A.ö.R. Klinik für Gastroenterologie, Hepatologie und Infektiologie Magdeburg
Germany Universitätsmedizin Mannheim II. Medizinische Klinik Mannheim
Germany Praxis Prof. Dr. med. Herbert Kellner München
Germany Gastroenterologische Fachpraxis am Germania Campus Münster
Germany Universitätklinikum Münster Medizinische Klinik und Poliklinik für Innere Medizin Münster
Germany Elbe Klinikum Stade Innere Medizin, Abteilung Gastroenterology Stade
Hungary Fovárosi Önkormányzat Péterfy Sándor Utcai Kórház Budapest
Hungary Pannónia Magánorvosi Centrum Kft. Budapest
Hungary Semmelweis Egyetem 1st Internal Dept. Budapest
Hungary Semmelweis Egyetem II. sz. Belgyógyászati Klinika Budapest
Hungary Békés Megyei Képviselotestület Pándy Kálmán Kórháza Semmelweis ulica 1 Gyula
Hungary Kaposi Mór Megyei Oktató Kórhaz Belgyógyászati Osztály Kaposvár
Hungary Borsod Abaúj Zemplén Megyei Kórház és Egyetemi Oktató Kórház II. sz. Belgyógyászati Osztály Miskolc
Hungary Karolina Kórház Rendelointézet Belgyógyászat- Gasztroenterológiai Osztály Mosonmagyaróvar
Hungary Clinfan Kft. SMO Szekszárd
Hungary CRU Hungary Kft. Szikszó
Latvia Daugavpils Central Regional Hospital Daugavpils
Latvia Digestive Disease Center GASTRO Riga
Latvia Latvian Maritime Medicine Centre Riga
Latvia Paula Stradina Clinical University Hospital Gastroenterology Centre Riga
Lithuania Lietuvos sveikatos mokslu universiteto ligonine VšI Kauno klinikos Gastroenterologijos skyrius Kaunas
Lithuania Klaipedos jurininku ligonine Diagnostikos skyrius Klaipeda
Lithuania VšI Mykolo Marcinkeviciaus ligonines Vilnius
Lithuania Vilniaus universiteto ligonine Santariškiu klinikos Hepatologijos, gastroenterologijos ir dietologijos centras Vilnius
Poland Centrum Opieki Zdrowotnej Orkan-Med Stec-Michalska Sp.J Ksawerów
Poland SPZOZ Uniwersytecki Szpital Kliniczny Nr 1 im. Norberta Barlickiego Oddzial Gastroenterologii Ogólnej i Onkologicznej Lódz
Poland Wojewódzki Szpital Specjalistyczny w Olsztynie Oddzial Gastroenterologii Olsztyn
Poland Endoskopia Sp. z o.o. Sopot
Poland Nzoz Vivamed Warszawa
Poland Akademicki Szpital Kliniczny im. Jana Mikulicza-Radeckiego we Wroclawiu Klinika Gastroenterologii i Hepatologii Wroclaw
Poland ARS MEDICA s.c., Rybak Maria, Rybak Zbigniew Wroclaw
Poland LexMedica Wroclaw
Poland Wojewodzki Szpital Specjalistyczny im. J. Gromkowskiego we Wroclawiu Oddzial Gastroenterologii Wroclaw
Spain Fundación Hospital de Alcorcón Servicio de Gastroenterología Alcorcón
Spain Centro Medico Teknon Servicio de Aparato Disgestivo Barcelona
Spain Hospital Universitario Virgen de la Arrixaca Servicio de Digestivo El Palmar
Spain Hospital Universitario La Paz Servico de Gastroenterologia Madrid
Spain Hospital Universitario La Princesa Unidad de Hepatología, Servicio de Gastroenterologia Madrid
Spain Corporació Sanitaria Parc Taulí Servicio de Digestivo Sabadell
Spain Hospital Universitario Marques de Valdecilla Servicio de Digestivo Santander

Sponsors (2)

Lead Sponsor Collaborator
sigma-tau i.f.r. S.p.A. PRA Health Sciences

Countries where clinical trial is conducted

Austria,  France,  Germany,  Hungary,  Latvia,  Lithuania,  Poland,  Spain, 

Outcome

Type Measure Description Time frame Safety issue
Primary Proportion of clinical/endoscopic remissions Remission will be defined according with the overall modified Mayo score (Disease Activity Index). A score = 2 with rectal bleeding sub-score = 0 and no other individual sub-score >1 will be considered necessary to classify the patient in remission state. End of treatment (week 8) No
Secondary Change from baseline in Rectal bleeding evaluation Evaluation will be performed by means of Disease Activity Index (DAI) sub-score (from 0 to 3). At week 2, 6 and 8 of treatment and after 4 week follow-up No
Secondary Change from baseline in stool frequency evaluation Evaluations will be performed by means of Disease Activity Index (DAI) sub-score (from 0 to 3). At week 2, 6 and 8 of treatment and after 4 week follow-up No
Secondary Histological response to the treatment Evaluated as an improvement of the histological index of at least 1 point End of treatment (week 8) No
Secondary Change from baseline in C-reactive protein (CRP) and Fibrinogen End of the treatment (week 8) and after 4 week follow-up No
Secondary Improvement of patients quality of life A validated specific questionnaire, the SIBDQ by McMaster university will be administered to evaluate changes in patients' quality of life End of treatment period (week8) and after 4 week follow-up No
Secondary Haematology Haemoglobin, Haematocrit, RBC, WBC and differential count. Baseline and end of treatment (week8) Yes
Secondary Electrocardiogram Standard intervals (PR, RR, QRS, QT) will be collected plus all rhythm abnormalities At baseline and at the end of treatment period (week8) Yes
Secondary Adverse Events collection 12 weeks Yes
Secondary Serum Chemistry Standard evaluation including renal and liver function, electrolytes and blood glucose At baseline and at the end of treatment period (week8) Yes
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