Pancragen 20 mg peptide vial with white lyophilized powder, labeled Batch No.007, dated 05-01-2026, pharmaceutical glass vial with rubber stopper and metal seal.

Pancragen 20mg vial

€40,00 EUR
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Pancragen 20 mg peptide vial with white lyophilized powder, labeled Batch No.007, dated 05-01-2026, pharmaceutical glass vial with rubber stopper and metal seal.
Pancragen 20mg vial

Pancragen 20mg vial

€40,00 EUR
Inkl. skatter.

                                         NOT FOR HUMAN CONSUMPTION

Pancragen is an ultrashort tripeptide bioregulator most commonly identified by the amino-acid sequence
EDP (Glu–Asp–Pro).

It is positioned within the Khavinson peptide-bioregulator framework as a pancreas-targeted regulatory peptide, conceptually derived from pancreatic tissue peptide fractions and later reproduced as a defined synthetic tripeptide for research and bioregulator product lines.

Regulatory status:
Pancragen is not FDA/EMA-approved as a therapeutic drug. In practice it is marketed as a bioregulator or research peptide, not as a regulated pharmaceutical with standardized indications, PK, or safety labeling.

2) Biological rationale: why a pancreatic tripeptide?

The bioregulator paradigm proposes that very short peptides (2–4 amino acids) can:

  • penetrate cells (and in some studies, nuclei),

  • interact with DNA/chromatin or transcriptional machinery, and

  • modulate gene-expression programs in a tissue-biased manner.

Within this framework, EDP (Pancragen) is classified as a pancreas-specific regulatory peptide, with proposed relevance to:

  • β-cell maintenance and renewal,

  • regulation of islet endocrine function,

  • pancreatic stress-response and aging biology, and

  • exocrine pancreatic cellular homeostasis.

The scientific anchor for these claims is primarily class-level mechanistic literature on ultrashort peptides and gene regulation, rather than modern randomized clinical trials specific to Pancragen.

3) Molecular mechanism of action

(evidence-weighted, non-receptor model)

3.1 Pharmacodynamic framing

Pancragen is not described as a ligand for a classical receptor (GPCR, RTK, etc.). Instead, it is framed as a gene-program modulator, based on three recurring mechanistic ideas in the ultrashort-peptide literature:

  1. Cellular and nuclear penetration
    Ultrashort peptides have been shown in multiple experimental systems to enter cytoplasm and nuclei, giving them physical access to transcriptional machinery.

  2. DNA / promoter-interaction hypothesis
    Computational docking and in-vitro interaction studies across this peptide class suggest that short peptides can bind specific DNA motifs or promoter regions, biasing transcription of selected genes.

  3. Epigenetic/transcriptional normalization
    By shifting transcriptional programs, peptides like EDP are proposed to “normalize” cellular phenotype under conditions of stress, metabolic overload, or aging.

3.2 Downstream biology (conceptual map)

Domain Reported / Proposed Effect Context
β-cell survival ↑ stress resistance, ↓ apoptosis inferred from pancreatic bioregulator positioning
β-cell renewal possible ↑ proliferative capacity class-level bioregulator claims
Insulin secretion normalization under stress brochure + framework-level claims
Exocrine pancreas improved cellular homeostasis organ-specific positioning
Gene-expression programs measurable transcriptional shifts supported by ultrashort-peptide literature

Interpretation constraint:
The most defensible scientific anchor is not pancreas-specific clinical outcomes, but the general ability of ultrashort peptides to modulate gene expression and cell differentiation programs.

4) Chemistry and identity

  • Sequence: Glu–Asp–Pro (EDP)

  • Molecule class: unmodified tripeptide

  • Charge profile: acidic (two negatively charged residues)

  • Molecular weight: ~345 Da

Identity caveat (practical):
“Pancragen” is sometimes used interchangeably to mean:

  • the defined tripeptide EDP, or

  • a branded pancreatic peptide complex.

For scientific or product-grade claims, identity should be confirmed by COA + MS/HPLC.

5) Pharmacokinetics and exposure constraints

There is no drug-label PK for Pancragen. As an unmodified tripeptide, general peptide principles apply:

  • likely rapid enzymatic degradation without stabilization,

  • short systemic half-life expected,

  • strong dependence on route and formulation (oral/sublingual vs parenteral vs intranasal are not interchangeable).

Because the mechanistic hypothesis hinges on intracellular/nuclear effects, any credible translation requires:

  • demonstration of tissue exposure, and

  • a reproducible PD signature (e.g., transcriptomic or protein-expression biomarkers).

6) Evidence base

6.1 Mechanistic / preclinical (stronger)

The strongest scientific foundation is class-level rather than Pancragen-specific:

  • Systematic reviews describe how ultrashort peptides (including EDP-like sequences) regulate gene expression and differentiation programs in multiple tissues.

  • Experimental and in-silico work across this class supports DNA-binding / promoter-interaction as a plausible physical mechanism.

These findings make the pancreatic-gene-modulation hypothesis biologically plausible, but not clinically proven.

6.2 Human clinical evidence (weaker / not drug-grade)

  • Product brochures and secondary summaries claim benefits in diabetes, pancreatic insufficiency, and metabolic stress states.

  • These materials generally do not present transparent RCT-grade datasets (randomization, blinding, prespecified endpoints, adverse-event accounting).

Bottom line:
There is no widely indexed, high-quality human RCT demonstrating clinically meaningful pancreatic or glycemic outcomes for Pancragen itself.

7) Safety and tolerability

(risk-based, not label-based)

Because Pancragen is not an approved medicine:

  • No standardized contraindications or interactions exist.

  • Dominant real-world risks relate to:

    • identity and purity variability,

    • contamination/sterility (especially for injectable “research peptide” formats),

    • unknown dose–response relationships.

Mechanism-based uncertainty:
Any agent proposed to modulate transcription may carry a risk of off-target gene-network effects, which cannot be bounded without controlled PK/PD and human safety studies.

8) Regulatory landscape

Pancragen is marketed as a bioregulator / research peptide, not as a regulated pharmaceutical.
It has no FDA or EMA marketing authorization.

9) How Pancragen fits into the broader bioregulator landscape

Peptide Sequence Target system Strongest mechanistic anchor
Vesugen KED Vascular Ki-67 / endothelial aging biology
Cortagen AEDP Nervous system gene-expression microarray effects
Pancragen EDP Pancreas gene-regulation framework
Testagen KEDG Gonadal nuclear localization / gene regulation
Bronchogen AEDL Lung mucin/surfactant gene activation

Pancragen is therefore best understood as a pancreatic member of a gene-regulatory peptide family, not as a hormone-like drug.

10) Future directions: what would make Pancragen “clinical-grade”

To move Pancragen from concept to evidence-based therapy, the decisive steps would be:

  1. Definitive molecular identity
    Confirm EDP vs peptide-complex formats; publish MS/HPLC and impurity profiles.

  2. Human PK/PD bridging
    Demonstrate exposure and target-engagement biomarkers (islet transcriptomics, stress markers, β-cell turnover signatures).

  3. Mechanism resolution
    Replace docking with modern chromatin-interaction assays (ChIP-seq, ATAC-seq shifts).

  4. Controlled clinical trials
    Defined populations (prediabetes, early T2D, pancreatic insufficiency) with validated endpoints (C-peptide, HOMA-β, CGM metrics, imaging biomarkers).