# Porcine Protease (Sus scrofa domesticus)

**Canonical URL:** https://ingredients.hermeticasuperfoods.com/ingredients/porcine-protease
**Data Source:** Hermetica Superfoods Ingredient Encyclopedia
**Updated:** 2026-03-29
**Evidence Score:** 2 / 10
**Category:** Enzyme
**Also Known As:** Pig protease, Swine protease, Porcine pancreatic protease, Sus scrofa protease, Domestic pig protease, Porcine digestive enzyme, Pig pancreatic enzyme, Porcine endopeptidase, Swine pancreatic protease

## Overview

Porcine protease is a [digestive enzyme](/ingredients/condition/gut-health) derived from pig (Sus scrofa domesticus) pancreatic or gastric tissue, containing serine proteases such as trypsin and chymotrypsin that cleave peptide bonds in dietary proteins. These enzymes hydrolyze proteins into absorbable amino acids and peptides by targeting specific amino acid sequences, supporting protein digestion particularly when endogenous enzyme output is insufficient.

## Health Benefits

• Enhanced protein digestion - Based on animal studies showing improved amino acid digestibility in pigs (preliminary evidence only)
• Potential improved nutrient absorption - In vitro studies demonstrate enhanced soybean meal digestibility (no human evidence)
• May support [digestive health](/ingredients/condition/gut-health) - Proteolytic enzymes facilitate protein hydrolysis and peptide bond cleavage (theoretical benefit, no human trials)
• Possible anti-oxidative effects - Hydrolyzed peptides from porcine sources show anti-oxidative activity in laboratory studies (preliminary evidence)
• Could aid in protein utilization - Animal feeding trials show improved protein breakdown and productivity in pigs (no human data available)

## Mechanism of Action

Porcine protease preparations contain serine endopeptidases—primarily trypsin, chymotrypsin, and elastase—that cleave internal peptide bonds at specific residues: trypsin targets lysine and arginine residues, while chymotrypsin cleaves after aromatic amino acids such as phenylalanine, tyrosine, and tryptophan. These enzymes function optimally in the neutral-to-alkaline pH range (pH 7–9) of the small intestine, where they activate a proteolytic cascade that reduces large polypeptides into di- and tripeptides and free amino acids ready for enterocyte absorption via peptide transporter PEPT1. Exogenous supplementation may compensate for reduced endogenous pancreatic protease secretion, as occurs in conditions like exocrine pancreatic insufficiency (EPI).

## Clinical Summary

The evidence base for porcine protease supplementation in humans is limited, with most data derived from animal models and in vitro studies. Pig feeding trials have demonstrated measurable improvements in ileal amino acid digestibility when porcine protease is added to soybean-meal-based diets, with digestibility coefficients improving by approximately 3–8% in controlled swine studies. In vitro [digestion](/ingredients/condition/gut-health) models show enhanced hydrolysis of plant proteins, particularly soy and wheat gluten, but these findings have not been replicated in randomized controlled trials in humans. Clinically, porcine-derived pancreatin preparations (which include proteases alongside lipase and amylase) have stronger evidence in EPI management, but isolated porcine protease as a standalone supplement lacks peer-reviewed human trial data establishing efficacy or optimal dosage.

## Nutritional Profile

Porcine Protease is an enzyme preparation derived from Sus scrofa domesticus (domestic pig), not a nutritional ingredient in the traditional macronutrient sense. As an enzyme, it contributes negligible caloric value (<1 kcal per typical supplemental dose of 50–500 mg). Macronutrient composition: Protein constitutes the primary structural component at approximately 85–95% dry weight (enzyme is itself a protease protein, predominantly serine protease and/or metalloprotease subtypes). Fat content is negligible (<1%). Carbohydrates are absent or trace (<1%). Bioactive compounds: The primary bioactive component is the proteolytic enzyme itself, characterized by active serine residues or zinc-coordinated metalloprotease domains capable of cleaving peptide bonds. Enzymatic activity is typically expressed in units such as HUT (Hemoglobin Units on a Tyrosine basis) or USP units, with commercial preparations ranging from 10,000–100,000 HUT per gram. Micronutrients: Trace zinc may be present in metalloprotease variants as a cofactor (approximately 1–4 mg/g of enzyme protein). Trace calcium may be present as a stabilizing cofactor in some preparations. Bioavailability notes: The enzyme itself is largely denatured and hydrolyzed in the gastrointestinal tract, meaning systemic absorption of intact enzyme protein is minimal; functional activity occurs primarily in the gastrointestinal lumen prior to denaturation by stomach acid (optimal pH activity range: 6.0–8.0 for most porcine proteases). Enteric-coated formulations may extend functional activity into the small intestine. No significant vitamin content is contributed by this ingredient.

## Dosage & Preparation

No clinically studied human dosages are available. Animal feed studies used unspecified inclusion levels without detailing exact doses, standardization, or activity units. No data exists for human dosing ranges in extract, powder, or standardized forms. Consult a healthcare provider before starting any new supplement.

## Safety & Drug Interactions

Porcine protease supplements are generally considered low-risk at typical dietary supplement doses, but individuals with pork allergies or sensitivities must avoid them due to the risk of allergic reactions, including anaphylaxis in severe cases. High doses of exogenous proteolytic enzymes may cause gastrointestinal side effects including nausea, cramping, and diarrhea, and oral mucosal irritation has been reported with chewable protease formulations. Porcine protease may theoretically enhance the absorption of certain oral medications by altering gut mucosal permeability or degrading protein-bound drug complexes, and caution is warranted alongside anticoagulants such as warfarin due to possible additive effects on fibrin degradation. Safety during pregnancy and lactation has not been established through clinical research, and use should be avoided unless directed by a healthcare provider; individuals with a history of pancreatitis should also exercise caution.

## Scientific Research

No human clinical trials, RCTs, or meta-analyses were identified for porcine protease as a biomedical supplement. Available evidence is limited to animal studies, including controlled feeding trials in pigs showing enhanced amino acid digestibility (PMID 39506561) and in vitro [digestion](/ingredients/condition/gut-health) assays demonstrating improved soybean meal digestibility.

## Historical & Cultural Context

No evidence of historical or traditional medicinal use was found in any traditional medicine systems. Porcine protease appears to be a modern industrial extract primarily developed for animal feed applications and protein hydrolysis, without documented traditional therapeutic context.

## Synergistic Combinations

Bromelain, Papain, Betaine HCl, Pepsin, Pancreatin

## Frequently Asked Questions

### What is porcine protease and how is it different from other digestive enzymes?

Porcine protease refers to protease enzymes—primarily trypsin, chymotrypsin, and elastase—extracted from pig (Sus scrofa domesticus) pancreatic or gastric tissue. Unlike plant-derived proteases such as bromelain (from pineapple) or papain (from papaya), porcine proteases have a pH activity profile closely matching human pancreatic enzymes, functioning optimally between pH 7 and 9 in the small intestine. This makes them structurally and functionally closer to the body's own digestive enzymes compared to most botanical alternatives.

### Is there human clinical evidence that porcine protease improves protein digestion?

As of current literature, robust human randomized controlled trials specifically evaluating isolated porcine protease are lacking; the most compelling data comes from swine feeding studies and in vitro digestion models. Animal trials have shown ileal amino acid digestibility improvements of roughly 3–8% with protease supplementation in soybean-meal diets. Porcine pancreatin blends (containing proteases plus lipase and amylase) have demonstrated clinical benefit in human exocrine pancreatic insufficiency, but isolated protease evidence in healthy adults remains preliminary.

### Can people with pork allergies take porcine protease supplements?

No—individuals with confirmed pork or porcine-derived ingredient allergies should not take porcine protease supplements, as residual porcine proteins can trigger IgE-mediated allergic responses ranging from hives and gastrointestinal distress to anaphylaxis in sensitized individuals. Those with alpha-gal syndrome, a tick-bite-associated allergy to the mammalian carbohydrate galactose-alpha-1,3-galactose found in pork and other red meats, may also react adversely. Consulting an allergist before use is strongly recommended for anyone with a history of meat or porcine product sensitivity.

### What is the typical dosage of porcine protease in supplements?

There is no established standardized human dosage for isolated porcine protease supplements, as clinical dose-finding trials in humans are absent. In porcine pancreatin pharmaceutical products used for exocrine pancreatic insufficiency, protease activity is typically measured in USP units, with therapeutic doses ranging from 25,000 to 40,000 USP protease units per meal. Over-the-counter digestive enzyme supplements containing porcine protease vary widely—from 10,000 to 100,000 HUT (Hemoglobin Unit Tyrosine basis) per serving—and manufacturers' dosing recommendations should be followed in the absence of clinical guidance.

### Does porcine protease interact with any medications?

Porcine protease may interact with anticoagulant medications such as warfarin or heparin, as systemic proteolytic enzyme activity has been associated with fibrinolytic effects that could theoretically potentiate bleeding risk, though direct interaction data for isolated porcine protease in humans is limited. There is also a theoretical concern that enhanced intestinal permeability from high protease activity could alter absorption kinetics of narrow-therapeutic-index drugs. Individuals taking immunosuppressants, blood thinners, or drugs with protein-binding pharmacokinetics should consult a healthcare provider before adding porcine protease supplementation.

### Is porcine protease safe for pregnant or breastfeeding women?

There is limited clinical safety data on porcine protease use during pregnancy and breastfeeding. Women in these populations should consult their healthcare provider before supplementing, as the effects on fetal development and infant exposure have not been adequately studied. Standard digestive enzyme use is generally considered low-risk, but individualized medical advice is warranted.

### What is the quality of evidence supporting porcine protease benefits in humans?

Currently, human clinical trials on porcine protease are limited or absent; most evidence comes from animal studies in pigs and in vitro laboratory experiments. The existing research shows promise for improved protein digestion in animal models, but these results have not been reliably replicated in rigorous human studies. Until larger, well-controlled human trials are conducted, benefits should be considered preliminary rather than conclusively proven.

### How does porcine protease bioavailability compare to plant-based protease supplements?

Porcine protease and plant-based proteases (such as bromelain or papain) differ in their enzymatic specificity and pH stability, which may affect their bioavailability and effectiveness in different parts of the digestive tract. Porcine protease is optimized for acidic stomach conditions, while some plant enzymes work better in neutral intestinal pH environments. Direct comparative studies measuring absorption and efficacy between these sources in humans are limited, making definitive bioavailability claims difficult.

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*Source: Hermetica Superfoods Ingredient Encyclopedia — https://ingredients.hermeticasuperfoods.com*
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