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Comparative Study to Evaluate Microbial Versus Porcine Pancreatic Enzyme Therapy in Chronic Pancreatitis (NP-PERT)

5 juillet 2026 mis à jour par: Rupjyoti Talukdar, Asian Institute of Gastroenterology, India

A Randomised, Double-Blind, Non-Inferiority Trial Comparing Microbial and Porcine Pancreatic Enzyme Replacement Therapy in Chronic Pancreatitis

Background: Chronic pancreatitis (CP) is a progressive inflammatory disorder causing irreversible pancreatic damage, eventually resulting in pancreatic exocrine insufficiency (PEI). This may lead to malabsorption, malnutrition, weight loss, and impaired quality of life. Pancreatic enzyme replacement therapy (PERT) is the standard treatment for PEI and is predominantly derived from porcine sources. However, religious, ethical, dietary, and supply-related concerns highlight the need for effective non-porcine alternatives. Microbial (fungal)-based pancreatic enzymes have shown promising safety and efficacy in preliminary studies, but evidence in CP remains limited.

Objective: To compare the efficacy and safety of non-porcine microbial (fungal)-based pancreatin with standard porcine-based pancreatin in patients with PEI secondary to CP.

Methods: This investigator-initiated, randomized, double-blind, single-center, non-inferiority trial will enroll 134 adults with CP-associated PEI (defined as having a fecal elastase <100 µg/g). After a two-week washout period, participants will be randomized 1:1 to receive either microbial-based or porcine-based pancreatin for 12 weeks. The primary outcome is the change from baseline in the Pancreatic Exocrine Insufficiency Questionnaire (PEI-Q) score at 12 weeks. Secondary outcomes include nutritional status, anthropometric measures, gastrointestinal symptoms, pain scores, stool consistency, glycaemic parameters, laboratory markers, and quality of life.

Discussion: This study aims to evaluate whether microbial-based pancreatin is non-inferior to porcine-based therapy and may provide a culturally acceptable and sustainable alternative for managing CP-related PEI.

Aperçu de l'étude

Description détaillée

Chronic pancreatitis (CP) is a complex inflammatory disorder of the pancreas. It is characterized by persistent inflammation that progressively damages the pancreatic tissue, leading to irreversible fibrotic changes. The dominant clinical manifestation of is abdominal pain and ongoing parenchymal injury leads to a gradual decline in both exocrine and endocrine function. However, the onset of pancreatic exocrine insufficiency (PEI) and diabetes is not universal, as a subset of individuals with CP retains sufficient exocrine reserve to avoid clinically significant malabsorption. When functional decline advances, however, patients may ultimately develop PEI and diabetes. In the absence of disease-modifying treatments, the current primary goal of management is early recognition and management of these complications. Treatment includes pain management, digestive support with pancreatic enzyme supplementation and nutrition, and endocrine management with oral antidiabetic medications and/or insulin.

In PEI, insufficient secretion of pancreatic enzymes leads to inadequate digestion and absorption of nutrients, resulting in weight loss, malnutrition, metabolic bone disease, and deficiencies of fat-soluble vitamins and minerals. PEI develops frequently in patients with CP, with a prevalence ranging from 30%-85% within 10-15 years after diagnosis.

Large cohort studies report an overall PEI prevalence of 50%-75%, particularly in patients with alcohol-related CP and longer disease duration. Management of PEI secondary to CP is important to improve nutritional status and quality of life. Pancreatic enzyme replacement therapy (PERT) is the mainstay of treatment for PEI. According to two meta-analyses, supportive treatment with pancreatic enzyme replacement showed significant improvement in the symptoms and consequences of PEI in patients with CP.

Currently available PERT preparations are primarily derived from porcine pancreas. Although clinically effective, porcine-derived PERT has certain limitations, including concerns related to its animal origin. Additionally, some patients may avoid such supplements due to lifestyle or ethical choices, such as vegetarians and vegans, while others, particularly followers of Islam and Judaism, may refrain from porcine-derived products due to religious dietary restrictions. Importantly, there is an increased lack of supplies due to the increasing prevalence of CP and other diseases associated with PEI. Therefore, new formulations of PERT are an unmet need.

Advances in biotechnology have led to the development of non-porcine microbial (fungal) based pancreatic enzymes that have been shown to have a good safety profile and efficacy in several conditions. Animal studies and human pilot studies have also shown benefit in CP. While the use of porcine PERT is well-established in CP, the utilization of non-porcine microbial-based PERT and its efficacy in CP is unclear.

HYPOTHESIS:

We hypothesize that non-porcine PERT will be as efficacious as the porcine based pancreatic enzymes in nutrient digestion. Hence, the aim of this study is to evaluate the clinical efficacy of non-porcine, microbial-based pancreatic enzymes compared with the current standard of care porcine enzymes, as a supportive therapy for patients with PEI secondary to CP.

REPORTING:

The study protocol will reported in accordance with the Standard Protocol Items: Recommendations for Interventional Trials (SPIRIT) 2025 guidelines.

MONITORING:

The conduct of the study will be monitored by a Data Safety Monitoring Board (DSMB).

STUDY DESIGN AND DURATION:

This is a multi-center, randomized, double-blind, parallel-group (1:1), placebo-controlled, non-inferior trial. The trial duration is 3 months (including enrolment and follow-up period). The study will be conducted in three independent branches of AIG hospitals, at Gachibowli, Somajiguda, and Banjara Hills, Hyderabad, India. The main branch at Gachibowli will be the coordinating center. Ethical approval has already been procured in the coordinating center (Asian Institute of Gastroenterology, Gachibowli).

FOLLOW-UP PLAN The patients will be provided with a structured diary wherein they will record their body weight every week using the same weighing machine for all measurements to ensure consistency. They will also record their medication intake, new symptoms, need for hospital visits, and any deviation in their diet regimen. A research coordinator will make a telephone call to each patient after weeks 4, 6, and 8 to collect any data that the patient recorded over the weeks. At the same time, the coordinator will also ensure and encourage compliance with the treatment. At the end of the study, the patient will visit the study centers where all the baseline measurements will be repeated. The patients will be directed to bring the study medicine containers, and a pill count will be done.

RANDOMIZATION, BLINDING, AND PERT ALLOCATION:

After obtaining written informed consent by the designated research coordinator, eligible participants who satisfy the inclusion criteria and complete the 2-week wash-out period will be randomized in a 1:1 ratio to either the non-porcine microbial (fungal)-based pancreatin group or the porcine-based standard-of-care pancreatin group. A block randomization method with a block size of 8 will be used to ensure equal allocation between the two groups. Randomization will be performed using a sealed envelope randomization software (https://www.sealedenvelope.com/power/continuous-noninferior/) by a statistician who is not involved in patient interaction, study interventions, or data analysis. Treatment allocation and blinding will be managed by an independent research coordinator not involved in the conduct of the study or patient care.

The principal investigator (PI), co-investigators, study staff, outcome assessors, and participants will remain blinded to treatment allocation throughout the study to ensure unbiased treatment administration and outcome assessment.

Unblinding will be permitted only in the event of a medical emergency or serious adverse event where knowledge of the assigned intervention is essential for clinical management. The PI will authorize unblinding and access the allocation code for the specific participant through the secure randomization system. The reason and date of unblinding will be documented, and the Institutional Ethics Committee will be notified as per regulatory requirements. Unblinding will be restricted to the affected participant and will not compromise the overall blinding of the trial.

STUDY AND ASSESSMENT METHOD:

Once the initial screening is completed by the PI and participant allocation is performed by an independent research coordinator, the designated co-investigators and research team from each center will systematically assess and record clinical, radiological (baseline), biochemical, and treatment-related details.

SAMPLE SIZE CALCULATION:

The study is designed as a non-inferiority trial comparing non-porcine microbial (fungal)based with porcine-based standard of care pancreatin on the primary continuous outcome measured by the PEI-Q total score (range 0-72). Non inferiority will be concluded if the upper bound of the one-sided 97.5% confidence interval for the mean difference does not exceed a pre-specified non-inferiority margin of 10 units, which is considered the minimal clinically important difference for the PEI-Q based on expert consensus. Sample size and power calculations for a range of non-inferiority margins (Δ = 5, 7.5, 10, 12.5, and 15 units), assuming a common standard deviation of 15 units and n = 60 participants per group, indicate that the study has approximately 94% power to demonstrate non-inferiority for a margin of 10 units, with higher power for larger margins and lower power for smaller margins. To adjust for 10% drop-outs, we will increase to sample size to 67 patients in each group adding up to a total of 134 patients.

STATISTICAL ANALYSIS A centralized database will be developed in RedCAP. Data will be uploaded from the three study centers and curated at the monitoring center in Aalborg, Denmark. All analyses will be conducted at the University of Aalborg, who will be blinded to treatment allocation and randomization.

Continuous variables will be expressed as mean with standard deviation (SD) or median with interquartile range (IQR), as appropriate. Categorical variables will be presented as frequencies and proportions.

A linear mixed-effects model will be used to assess changes in PEI-Q scores across all assessment time points. Summary statistics with corresponding 95% confidence intervals (CI) will be reported with the between group-difference at 12 weeks being the primary endpoint.

Continues secondary outcomes, including changes in nutritional parameters, SARC-F score, stool consistency, gastrointestinal symptom severity, quality of life, endocrine function, fecal elastase-1 levels, and body composition, will be analyzed using mixed-effects regression models for normally distributed variables and quantile regression models for non-normally distributed variables. Categorical outcomes will be analyzed using risk differences between groups with corresponding 95% confidence intervals.

Missing data will be handled using multiple imputation techniques. A two-tailed p-value of <0.05 will be considered statistically significant.

Type d'étude

Interventionnel

Inscription (Estimé)

134

Phase

  • Phase 3

Contacts et emplacements

Cette section fournit les coordonnées de ceux qui mènent l'étude et des informations sur le lieu où cette étude est menée.

Coordonnées de l'étude

Sauvegarde des contacts de l'étude

  • Nom: Abdul Rasheed, PharmD

Critères de participation

Les chercheurs recherchent des personnes qui correspondent à une certaine description, appelée critères d'éligibilité. Certains exemples de ces critères sont l'état de santé général d'une personne ou des traitements antérieurs.

Critère d'éligibilité

Âges éligibles pour étudier

  • Adulte
  • Adulte plus âgé

Accepte les volontaires sains

Non

La description

Inclusion Criteria:

  • CP fulfilling the M-ANNHEIM criteria 11 with documented PEI (defined as fecal elastase <100 µg/g stool on the background of morphological changes of CP).
  • Willingness to undergo a 2-week wash-out period without pancreatic enzyme therapy before enrolment.
  • Willing and able to provide written informed consent.

Exclusion Criteria:

  • Major psychiatric illness impairing study participation.
  • Systemic illness affecting digestion or study outcomes.
  • Any condition deemed unsuitable for study participation by the investigator.
  • Concurrent acute exacerbation of the CP at the time of screening.

Plan d'étude

Cette section fournit des détails sur le plan d'étude, y compris la façon dont l'étude est conçue et ce que l'étude mesure.

Comment l'étude est-elle conçue ?

Détails de conception

  • Objectif principal: Traitement
  • Répartition: Randomisé
  • Modèle interventionnel: Affectation parallèle
  • Masquage: Quadruple

Armes et Interventions

Groupe de participants / Bras
Intervention / Traitement
Expérimental: Non-porcine microbial (fungal) based pancreatic enzyme preparation
The non-porcine microbial enzyme preparation will contain amylase (6650 DU), lipase (13000 FIP), and protease (7120 HUT, 15 SAPU, 3000 PC)
Dietary Supplement: Pancreatic enzyme preparation from microbial (fungal) source that contains amylase (6650 DU), lipase (13000 FIP), and protease (7120 HUT, 15 SAPU, 3000 PC).
Comparateur actif: Standard of care porcine pancreatic enzyme
The standard of care porcine-based enzyme preparation will contain amylase (8000 U), lipase (25000 U), and protease (1000 U)
Standard of care porcine pancreatic enzyme preparation: amylase (8000 U), lipase (25000 U), and protease (1000 U)

Que mesure l'étude ?

Principaux critères de jugement

Mesure des résultats
Description de la mesure
Délai
Change in Pancreatic Exocrine Insufficiency Questionnaire (PEI-Q) score
Délai: 3 months
The PEI-Q is a validated questionnaire that captures several symptoms related to exocrine pancreatic insufficiency and the result is presented as a composite score.
3 months

Mesures de résultats secondaires

Mesure des résultats
Description de la mesure
Délai
Changement de la qualité de vie
Délai: 3 mois

La qualité de vie sera évaluée par l'outil Short Form (SF)-36. Il s'agit d'un outil de notation standardisé et validé basé sur un questionnaire qui contient 36 questions portant sur 8 domaines de la qualité de vie.

Le score le plus bas de cet outil est 0 et le score le plus élevé est 100, un score plus élevé indiquant une meilleure qualité de vie.

3 mois
Changement de l'état nutritionnel : Anthropométrie
Délai: 3 mois
Circonférence musculaire du bras mi-supérieur (CMB) en cm.
3 mois
Changement de l'état nutritionnel : Anthropométrie
Délai: 3 mois
Surface musculaire du bras médian (MAMA) en centimètres carrés.
3 mois
Modification de l'état nutritionnel : Évaluation biochimique
Délai: 3 mois
Hémoglobine en g/dL
3 mois
Modification de l'état nutritionnel : Évaluation biochimique
Délai: 3 mois
Vitamine D
3 mois
Changement de l'état nutritionnel : Évaluation biochimique
Délai: 3 mois
Vitamine B12
3 mois
Changement de composition corporelle (analyse par bio-impédance) : Masse grasse (kg)
Délai: 3 mois
La masse grasse totale sera évaluée à l'aide de l'analyse d'impédance bioélectrique (BIA). Il s'agit d'une méthode non invasive qui fonctionne en envoyant un courant électrique de faible intensité, imperceptible, à travers le corps. La fourchette normale est de 10 à 20 kg.
3 mois
Changement de la composition corporelle (analyse par bio-impédance) : Eau corporelle totale (litres)
Délai: 3 mois
L'eau corporelle totale sera quantifiée à l'aide de l'analyse par bioimpédance (BIA). Il s'agit d'une méthode non invasive qui fonctionne en envoyant un courant électrique de faible intensité et imperceptible à travers le corps.
3 mois
Modification de la composition corporelle (analyse par bio-impédance) : Angle de phase à 50 kHz (degrés)
Délai: 3 mois
L'intégrité de la membrane cellulaire sera évaluée en utilisant la fonction d'angle de phase de l'analyse de bio-impédance (BIA). Il s'agit d'une méthode non invasive qui fonctionne en envoyant un courant électrique de faible intensité, imperceptible, à travers le corps.
3 mois
Changement de la composition corporelle (analyse par bio-impédance) : Niveau de graisse viscérale (unité numérique ; plage normale (1-12).
Délai: 3 mois
Le niveau de graisse viscérale sera évalué par analyse d'impédance bioélectrique (BIA). Il s'agit d'une méthode non invasive qui fonctionne en envoyant un courant électrique de faible intensité, imperceptible, à travers le corps. La plage normale est de 1 à 12, une valeur plus basse indiquant une graisse viscérale plus faible et une valeur plus élevée indiquant une graisse viscérale plus importante.
3 mois
Change in nutritional status: Subjective global assessment
Délai: 3 months
Subjective global assessment (SGA) is a composite semi-quantitative tool that provides the degree of nutrition of an individual in three categories such as SGA A (Normal nutrition), SGA B (moderate malnutrition) and SGA C (Severe malnutrition).
3 months
Change in nutritional status: Body weight
Délai: 3 months
Percent change in body weight (kg)
3 months
Change in nutritional status: Anthropometry
Délai: 3 months
Mid-arm circumference (MAC) in cm.
3 months
Change in nutritional status: Anthropomentry
Délai: 3 months
Triceps skin fold thickness (TSF) in cms.
3 months
Change in nutritional status: Biochemical assessment
Délai: 3 months
Serum pre albumin (mg/dl)
3 months
Change in endocrine status
Délai: 3 months
HbA1c
3 months
Change in endocrine function
Délai: 3 months
Fasting blood glucose (mg/dl)
3 months
Change in endocrine function
Délai: 3 months
C-peptide
3 months
Change in body composition (Bioimpedence analysis): Skeletal muscle mass (kg)
Délai: 3 months
Skeletal muscle mass will be assessed using Bioimpedence analysis (BIA) This is a non-invasive method that operates by sending a low-level, imperceptible electrical current through the body
3 months
Stool consistency
Délai: 3 months
Bristol stool scale [Type 1 (separate hard lumps, indicating constipation) to Type 7 (watery stool, indicating diarrhea].
3 months
Change in gastrointestinal symptoms
Délai: 3 months
Patient Assessment of Upper Gastrointestinal Disorders - Symptom Severity Index (PAGI-SYM)
3 months
Change in sarcopenia score
Délai: 3 months
SARC-F Questionnaire (Score of =/>4 is considered to have sarcopenia)
3 months
Change in patient's global impression of change (PGIC)
Délai: 3 months
This will be evaluated using the Patient's Global Impression of Change (PGIC). The score ranges from 1-7, with a score of 1 indicating very much improved and 7 indicating very much worse
3 months
Change in quality of life (QOL)
Délai: 3 months
QOL will be assessed using the EORTC-QLQ c30 with PAN-28.
3 months
Change in pain severity
Délai: 3 months.
Range of 0-10 in the Visual Analog Scale (VAS). A score of 0 indicates no pain, while 10 is maximum pain.
3 months.
Change in pain severity
Délai: 3 months
Pain-related symptoms and characteristics will be assessed using the Short-form Comprehensive Pain Assessment Tool (COMPAT-SF).
3 months
Readmission during the study period
Délai: 3 months
Number of admissions during the study period
3 months
Change in functional mobility during the study period.
Délai: 3 months.
This will be performed using the using the Timed Up and Go (TUG) test.
3 months.

Collaborateurs et enquêteurs

C'est ici que vous trouverez les personnes et les organisations impliquées dans cette étude.

Collaborateurs

Les enquêteurs

  • Chercheur principal: Rupjyoti Talukdar, MD, Asian Institute of Gastroenterology

Publications et liens utiles

La personne responsable de la saisie des informations sur l'étude fournit volontairement ces publications. Il peut s'agir de tout ce qui concerne l'étude.

Publications générales

Dates d'enregistrement des études

Ces dates suivent la progression des dossiers d'étude et des soumissions de résultats sommaires à ClinicalTrials.gov. Les dossiers d'étude et les résultats rapportés sont examinés par la Bibliothèque nationale de médecine (NLM) pour s'assurer qu'ils répondent à des normes de contrôle de qualité spécifiques avant d'être publiés sur le site Web public.

Dates principales de l'étude

Début de l'étude (Estimé)

1 août 2026

Achèvement primaire (Estimé)

1 juin 2027

Achèvement de l'étude (Estimé)

1 septembre 2027

Dates d'inscription aux études

Première soumission

5 juillet 2026

Première soumission répondant aux critères de contrôle qualité

5 juillet 2026

Première publication (Réel)

13 juillet 2026

Mises à jour des dossiers d'étude

Dernière mise à jour publiée (Réel)

13 juillet 2026

Dernière mise à jour soumise répondant aux critères de contrôle qualité

5 juillet 2026

Dernière vérification

1 juillet 2026

Plus d'information

Termes liés à cette étude

Plan pour les données individuelles des participants (IPD)

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INDÉCIS

Informations sur les médicaments et les dispositifs, documents d'étude

Étudie un produit pharmaceutique réglementé par la FDA américaine

Non

Étudie un produit d'appareil réglementé par la FDA américaine

Non

Ces informations ont été extraites directement du site Web clinicaltrials.gov sans aucune modification. Si vous avez des demandes de modification, de suppression ou de mise à jour des détails de votre étude, veuillez contacter register@clinicaltrials.gov. Dès qu'un changement est mis en œuvre sur clinicaltrials.gov, il sera également mis à jour automatiquement sur notre site Web .

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