VIP5 (Vasoactive Intestinal Peptide Fragment)
VIP5 is a short peptide fragment derived from vasoactive intestinal peptide (VIP), a naturally occurring neuropeptide involved in cellular communication, vascular signaling, and immune-related pathways. In research settings, VIP5 is studied for its ability to model selective aspects of VIP-related signaling while offering a more focused and simplified peptide structure.
In laboratory research, VIP5 is valued for its interaction with VIP-associated receptor pathways. VIP receptors are widely distributed across nervous, immune, and vascular systems, making VIP-derived fragments relevant for studying cross-system cellular communication.
One of the defining characteristics of VIP5 is its reduced peptide length compared to full-length VIP. This allows researchers to isolate and examine specific signaling behaviors without the complexity of the parent peptide, supporting precision-based experimental design.
VIP5 is frequently examined in neurobiology research focused on neuromodulation and neurotransmitter signaling. VIP-related pathways are known to influence neural communication balance, and VIP5 provides insight into how smaller peptide sequences contribute to these effects.
The peptide is also studied in immune signaling research. VIP pathways are associated with immune cell communication and inflammatory signaling modulation, making VIP5 useful for exploring how peptide fragments influence immune response coordination in controlled models.
In vascular and endothelial research, VIP5 is examined for its relevance to cellular signaling involved in vasodilation-related mechanisms. This allows researchers to investigate how peptide-mediated signals influence vascular cell behavior at the molecular level.
VIP5’s compact structure supports stability and predictable behavior in laboratory environments. This reliability contributes to reproducible results and makes it suitable for comparative peptide signaling studies.
Researchers often include VIP5 in structure–function investigations to better understand how truncation of larger neuropeptides alters receptor interaction and downstream signaling pathways.
Unlike full-length VIP, VIP5 is studied for its selective signaling potential rather than broad systemic activity. This targeted approach allows for focused examination of specific biological mechanisms.
VIP5 is also of interest in gut–brain axis research, where VIP-related signaling plays a role in communication between the nervous system and gastrointestinal cellular networks.
Because VIP signaling intersects multiple biological systems, VIP5 is commonly used in systems-based research rather than isolated pathway studies, supporting broader insight into peptide-mediated coordination.
The peptide’s well-defined sequence makes it a useful reference compound in neuropeptide and immune-modulation research.
As peptide science continues to evolve, VIP5 remains a valuable research tool for studying how short peptide fragments contribute to complex biological signaling networks.
Its focused design, stability, and relevance to VIP-related pathways make VIP5 an important compound for advanced cellular communication research.
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VIP5 (Vasoactive Intestinal Peptide Fragment) 10mg
$145.00
VIP5 is a short peptide fragment derived from vasoactive intestinal peptide (VIP), a naturally occurring neuropeptide involved in cellular communication, vascular signaling, and immune-related pathways. In research settings, VIP5 is studied for its ability to model selective aspects of VIP-related signaling while offering a more focused and simplified peptide structure.
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