VIP Peptide | Buy Research-Grade Vasoactive Intestinal Peptide in Europe | ≥99% Purity

VIP (Vasoactive Intestinal Peptide) is a 28 amino acid endogenous neuropeptide and immunomodulatory hormone, available to buy in Europe for laboratory research into neuroimmune regulation, gut motility biology, pulmonary physiology, circadian rhythm signalling, and VPAC receptor pharmacology.

Laboratories and research institutions across the EU can order verified, research-grade VIP with fast international dispatch to Europe, full batch documentation, and ≥99% purity confirmed by HPLC and Mass Spectrometry.

✅ ≥99% Purity — HPLC & Mass Spectrometry Verified

✅ Batch-Specific Certificate of Analysis (CoA)

✅ Sterile Lyophilised Powder | GMP Manufactured

✅ Fast Dispatch to EU & Europe | Tracked Shipping

What is VIP Peptide?

VIP (Vasoactive Intestinal Peptide) is a 28 amino acid neuropeptide and peptide hormone belonging to the glucagon/secretin superfamily — a structurally related class of signalling peptides sharing a conserved helical backbone that includes PACAP, glucagon, GLP-1, secretin, and PHI. First isolated from porcine intestine in 1970 by Said and Mutt, VIP is now understood to be one of the most widely distributed and pleiotropic neuropeptides in the body — expressed throughout the enteric nervous system, central and peripheral nervous system, immune tissues, respiratory tract, and reproductive organs.

VIP exerts its biological effects through two G-protein coupled receptors — VPAC1 and VPAC2 — both of which signal primarily through Gs-coupled cAMP/PKA pathways and are expressed in a wide range of tissues including intestinal smooth muscle, immune cells, lung, brain, pancreas, and cardiovascular tissue. A third receptor — PAC1 — preferentially binds PACAP but shows some VIP affinity at higher concentrations, adding further complexity to VIP’s receptor pharmacology. Through these receptors, VIP coordinates an extraordinarily broad range of physiological functions — earning its characterisation in the research literature as one of the most multifunctional neuropeptides known.

VIP’s biological roles span gut motility regulation, vasodilation and bronchodilation, immune tolerance induction, circadian clock synchronisation in the suprachiasmatic nucleus, neurotransmission, exocrine and endocrine secretion, and reproductive biology — making it a research tool of relevance across gastroenterology, immunology, pulmonology, chronobiology, and neuroscience. Its potent anti-inflammatory and immunomodulatory properties have attracted particular research attention — with studies establishing VIP as a key mediator of immune tolerance through effects on T regulatory cell induction, Th1/Th2 balance, and innate immune cell cytokine suppression. These properties have made VIP one of the most actively researched immunomodulatory neuropeptides in European pre-clinical research settings.

What Does VIP Peptide Do in Research?

In laboratory settings, VIP is studied across an exceptionally broad range of physiological systems and research applications — reflecting its wide tissue distribution and pleiotropic receptor pharmacology. EU and European researchers working with VIP typically focus on:

• VPAC receptor pharmacology — VIP is the primary endogenous ligand for VPAC1 and VPAC2 receptors, making it the reference compound for studying VPAC receptor biology — including receptor binding kinetics, downstream cAMP/PKA signalling, receptor subtype distribution across tissues, and comparative pharmacology with PACAP and synthetic VPAC ligands.
• Immunomodulation and immune tolerance research — VIP is one of the most potent endogenous immunomodulatory neuropeptides characterised — suppressing pro-inflammatory cytokine production, inducing regulatory T cell differentiation, shifting immune responses toward tolerogenic profiles, and modulating innate immune cell activation. Studies use VIP to examine neuroimmune regulatory mechanisms and the contribution of neuropeptide signalling to immune homeostasis.
• Gut motility and enteric nervous system research — VIP is a major inhibitory neurotransmitter of the enteric nervous system — driving intestinal smooth muscle relaxation, regulating peristalsis, and coordinating gut motility patterns. It is used extensively in gastrointestinal research examining enteric neurotransmission, intestinal smooth muscle pharmacology, and the neural regulation of gut function.
• Gut inflammation and intestinal immunity research — studies have examined VIP’s anti-inflammatory effects in intestinal inflammation models — including effects on mucosal cytokine profiles, epithelial barrier function, and gut immune cell regulation — making it a research tool relevant to inflammatory bowel disease biology alongside KPV and BPC-157.
• Pulmonary biology and bronchodilation research — VIP is expressed in pulmonary neurons and acts on airway smooth muscle VPAC receptors to produce bronchodilation and anti-inflammatory effects in lung tissue. Studies use VIP to examine airway pharmacology, pulmonary neuroimmune regulation, and the role of neuropeptide signalling in respiratory biology.
• Circadian rhythm and suprachiasmatic nucleus research — VIP is the primary neurotransmitter coordinating circadian rhythm synchronisation between neurons of the suprachiasmatic nucleus (SCN) — the brain’s master circadian clock. It is used in chronobiology research examining how SCN VIP/VPAC2 signalling maintains circadian rhythm coherence and synchronises peripheral clocks throughout the body.
• Neuroprotection and neuroinflammation research — studies have characterised VIP’s neuroprotective and anti-neuroinflammatory effects — including suppression of microglial activation, reduction of neuroinflammatory cytokine production, and protection of neurons against excitotoxic and inflammatory injury — making it relevant to CNS inflammatory disease research.
• Autoimmune disease models — VIP’s immune tolerance-inducing properties have been examined in pre-clinical autoimmune models — including rheumatoid arthritis, multiple sclerosis, inflammatory bowel disease, and lupus models — where its effects on Treg induction, Th17 suppression, and inflammatory cytokine reduction have been characterised.
• Cardiovascular biology research — VIP acts as a vasodilator and cardiac chronotrope through VPAC receptor activation in vascular smooth muscle and cardiac tissue — making it relevant to research examining neuropeptide contributions to cardiovascular regulation, vascular tone, and cardiac function parameters.
• Pancreatic biology and insulin secretion research — VPAC receptors are expressed on pancreatic beta cells, and VIP acts as an incretin-like potentiator of glucose-stimulated insulin secretion — connecting it to metabolic biology research alongside GLP-1 and other incretin peptides.
• Reproductive biology research — VIP is expressed in reproductive tissues and has been characterised in studies examining neuropeptide regulation of reproductive function — including effects on uterine contractility, ovarian biology, and reproductive neuroendocrine regulation.
• Neurotransmission and synaptic biology — VIP functions as a neurotransmitter and neuromodulator in multiple CNS and peripheral nervous system circuits — and is used in neuroscience research examining peptidergic neurotransmission, synaptic plasticity, and the role of neuropeptide co-transmission in neural circuit function.

All research applications are for in vitro and pre-clinical use only.

What Do Studies Say About VIP Peptide?

VIP has one of the most extensive research literatures of any neuropeptide — with over five decades of investigation spanning gastroenterology, immunology, neuroscience, pulmonology, and chronobiology establishing it as a pleiotropic signalling molecule of fundamental physiological importance.

Immunomodulatory profile: A large and well-established body of research has characterised VIP as a potent anti-inflammatory and immunomodulatory neuropeptide — documenting suppression of TNF-α, IL-6, IL-12, and IL-1β production in stimulated macrophages and dendritic cells, induction of IL-10 and TGF-β tolerogenic cytokines, promotion of regulatory T cell differentiation, and inhibition of Th1 and Th17 inflammatory responses. These findings have established VIP as one of the primary mediators of neuroimmune anti-inflammatory regulation and have driven substantial European research interest in VIP as a model immunomodulatory neuropeptide.

Autoimmune disease pre-clinical research: Studies examining VIP in pre-clinical autoimmune models have documented beneficial effects across multiple disease systems — including reductions in joint inflammation and cartilage damage in collagen-induced arthritis models, improvements in neurological parameters in EAE multiple sclerosis models, and reductions in intestinal inflammation in colitis models. These findings have characterised VIP’s therapeutic research potential across autoimmune biology and have positioned it as a reference neuropeptide immunomodulator in European pre-clinical research.

Circadian biology: Research has established VIP as the essential neurotransmitter for synchronising circadian rhythms between SCN neurons — with studies documenting that VIP/VPAC2 signalling maintains the coherent circadian oscillation of the SCN clock network that drives daily rhythms in physiology and behaviour. Studies using VIP knockout and VPAC2 knockout models have comprehensively characterised the consequences of disrupted VIP signalling for circadian rhythm organisation — establishing VIP as an indispensable research tool in chronobiology.

Enteric nervous system research: Decades of research have characterised VIP as a major inhibitory neurotransmitter of the enteric nervous system — with studies documenting its role in descending inhibition during peristalsis, non-adrenergic non-cholinergic (NANC) relaxation of intestinal smooth muscle, and coordination of gut motility patterns. This foundational gastrointestinal neuroscience literature has established VIP as the reference compound for studying inhibitory enteric neurotransmission.

Pulmonary research: Studies have characterised VIP expression in pulmonary neurons and its bronchodilatory and anti-inflammatory effects in airway tissue — with research documenting VPAC receptor-mediated smooth muscle relaxation, inhibition of mast cell activation, and suppression of airway inflammatory responses. Reduced VIP expression has been documented in asthmatic airways in some research, connecting VIP biology to inflammatory respiratory disease research.

Neuroprotection research: Studies have characterised VIP’s neuroprotective effects in models of CNS injury and neurodegeneration — documenting protection against excitotoxic, ischaemic, and inflammatory neuronal injury through mechanisms including BDNF upregulation, anti-apoptotic signalling, and microglial activation suppression. These findings have established VIP as a research tool for studying neuropeptide-mediated CNS protection.

VPAC receptor signalling characterisation: Research has comprehensively characterised VPAC1 and VPAC2 receptor distribution, binding kinetics, downstream cAMP/PKA signalling cascades, and differential tissue expression — with VIP serving as the primary pharmacological tool for these studies. This receptor biology literature provides the mechanistic foundation for interpreting VIP’s diverse physiological effects across different tissue systems.

VIP vs Related Neuropeptide and Immunomodulatory Research Compounds

Compound	Type	Primary Receptors	Key Research Application
VIP	28aa endogenous neuropeptide	VPAC1 + VPAC2	Neuroimmune regulation, gut motility, circadian biology, pulmonary research
PACAP-38	38aa neuropeptide — VIP superfamily	PAC1 + VPAC1 + VPAC2	Neuroprotection, stress biology, comparative VPAC/PAC1 pharmacology
PACAP-27	27aa PACAP truncation	PAC1 + VPAC1 + VPAC2	Comparative PACAP biology, receptor selectivity research
Secretin	27aa — VIP superfamily	Secretin receptor	Pancreatic secretion, gut biology
KPV	α-MSH C-terminal tripeptide	Melanocortin pathway / NF-κB	Gut inflammation, anti-inflammatory biology
Thymosin β4	43aa thymic peptide	Pleiotropic repair signalling	Tissue repair, immune regulation

Buying VIP Peptide in Europe — What’s Included

Every order of VIP peptide dispatched to EU and European research institutions includes:

• Batch-Specific Certificate of Analysis (CoA)
• HPLC Chromatogram
• Mass Spectrometry Confirmation
• Sterility and Endotoxin Testing Reports
• Reconstitution Protocol
• Technical Research Support

Frequently Asked Questions — VIP Peptide EU

Can I Buy VIP Peptide in the EU and Europe?

Yes. We supply research-grade Vasoactive Intestinal Peptide with fast tracked international dispatch to all EU member states and wider European destinations including Germany, France, Netherlands, Spain, Italy, Poland, and beyond. Packaging is designed to maintain peptide integrity throughout transit and all orders include full batch documentation. VIP is supplied strictly for laboratory research use only.

What Are VPAC1 and VPAC2 Receptors and How Do They Differ?

VPAC1 and VPAC2 are both G-protein coupled receptors that bind VIP and PACAP with comparable affinity — signalling primarily through Gs-coupled cAMP/PKA pathways. They differ in their tissue distribution and physiological roles. VPAC1 is widely expressed — found in lung, intestine, liver, immune cells, and throughout the CNS — and is considered the primary mediator of VIP’s immunomodulatory effects given its expression on T cells, macrophages, and dendritic cells. VPAC2 has a more restricted distribution — expressed prominently in the suprachiasmatic nucleus, smooth muscle, pancreas, and specific brain regions — and is the primary receptor mediating VIP’s circadian rhythm synchronisation function in the SCN. These distinct distributions make VPAC1 and VPAC2 research targets of interest in different biological contexts, with VIP serving as the reference non-selective agonist for both.

What is the Difference Between VIP and PACAP in Research?

VIP and PACAP (Pituitary Adenylate Cyclase-Activating Polypeptide) are closely related members of the glucagon/secretin superfamily with overlapping but distinct receptor pharmacology. Both bind VPAC1 and VPAC2 with comparable affinity, but PACAP additionally binds PAC1 — a receptor with much higher affinity for PACAP than VIP — through which it exerts many of its most characterised neuroprotective and stress biology effects. VIP’s research profile is more centred on immunomodulation, gut biology, and circadian rhythm regulation — reflecting its high expression in enteric neurons, immune tissues, and the SCN. PACAP’s research profile emphasises neuroprotection, stress response biology, and CNS signalling — reflecting PAC1 receptor expression in brain regions involved in these functions. The two are studied as complementary tools for dissecting the shared VPAC1/VPAC2 pharmacology from the PACAP-selective PAC1 receptor biology.

How Does VIP Regulate Circadian Rhythms in the SCN?

The suprachiasmatic nucleus (SCN) — the brain’s master circadian clock — contains approximately 20,000 neurons that must synchronise their individual circadian oscillations to produce a coherent population-level rhythm driving daily physiological cycles. VIP, released by a subset of SCN neurons, binds VPAC2 receptors on neighbouring neurons to synchronise their circadian clocks through cAMP/PKA signalling — maintaining the phase coherence of the SCN network. Research using VIP knockout and VPAC2 knockout mice has documented severe circadian rhythm fragmentation and arrhythmicity — establishing VIP/VPAC2 signalling as essential for SCN network synchronisation. VIP is therefore the primary research tool for studying the neurotransmitter mechanisms underlying circadian clock network organisation.

What Makes VIP an Important Tool in Autoimmune Disease Research?

VIP’s immunomodulatory profile makes it one of the most pharmacologically interesting endogenous anti-inflammatory neuropeptides for autoimmune disease research. Its effects include suppression of pro-inflammatory cytokines through VPAC1 on immune cells, promotion of regulatory T cell differentiation, inhibition of Th17 inflammatory responses, and induction of tolerogenic dendritic cell phenotypes — collectively shifting immune responses toward tolerance. In pre-clinical autoimmune models including arthritis, multiple sclerosis, and inflammatory bowel disease, VIP administration has produced measurable reductions in disease parameters. These findings position VIP as a reference neuropeptide immunomodulator for studying neuroimmune regulation and as a research model for peptide-based immune tolerance strategies.

What is the Relationship Between VIP and Gut Motility Research?

VIP is one of the primary inhibitory neurotransmitters of the enteric nervous system — released from inhibitory motor neurons to drive relaxation of intestinal smooth muscle through VPAC receptor-mediated cAMP elevation and downstream smooth muscle hyperpolarisation. It plays an essential role in the descending inhibition component of the peristaltic reflex — where intestinal contents trigger relaxation ahead of the advancing bolus — and in non-adrenergic non-cholinergic (NANC) relaxation of gut smooth muscle. VIP-containing enteric neurons are among the most well-characterised in gut neuroscience, and VIP is used as the reference inhibitory enteric neurotransmitter in research examining intestinal smooth muscle pharmacology, peristaltic reflex mechanisms, and enteric nervous system circuit biology.

How Do I Reconstitute VIP Peptide for Laboratory Use?

Allow the vial to reach room temperature before opening. Add sterile water or an appropriate laboratory buffer slowly down the vial wall and swirl gently — do not shake. VIP is a 28 amino acid peptide that reconstitutes in aqueous buffers — prepare at your protocol’s required concentration and consider adding a carrier protein such as BSA at low concentrations to minimise adsorption losses. Aliquot and store at -80°C to minimise freeze-thaw degradation. Standard peptide handling protocols apply. VIP is susceptible to enzymatic degradation — prepare working solutions fresh and handle on ice during experimental procedures.

How Quickly is VIP Delivered to Europe?

Orders are dispatched promptly via tracked international courier. Delivery to EU and European destinations typically takes 3–7 working days depending on location, with packaging designed to protect peptide stability throughout transit.

Product Specifications

Parameter	Detail
Full Name	Vasoactive Intestinal Peptide
Type	Endogenous 28 Amino Acid Neuropeptide — Glucagon/Secretin Superfamily
Primary Receptors	VPAC1 + VPAC2 (Gs-coupled cAMP/PKA signalling)
Molecular Weight	3326.8 g/mol
Primary Research Interest	Neuroimmune regulation, gut motility, circadian biology, pulmonary research, autoimmune models
Purity	≥99%
Verification	HPLC & Mass Spectrometry
Form	Sterile Lyophilised Powder
Solubility	Sterile water or laboratory buffer — BSA carrier recommended at low concentrations
Storage	-20°C, protected from light and moisture
Intended Use	Research use only

Research Disclaimer

VIP (Vasoactive Intestinal Peptide) is supplied exclusively for legitimate scientific research conducted within licensed laboratory environments. This product is not approved for human consumption, self-administration, or any therapeutic, clinical, or veterinary application. It must be handled solely by qualified researchers in compliance with applicable EU regulations, national legislation, and institutional ethics guidelines. By purchasing, you confirm this compound will be used exclusively for approved in vitro or pre-clinical research purposes.