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GLI PRO XL21080 Dual 10


GLI PRO XL21080 Dual 10″ 800W Professional PA Speaker System Great Quality!


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Gli Pro PVX5000 5,000 Watt 2 Channel Bridgable Power Amplifier DJ Rack Amp


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GLI PRO XL1540 15


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GLI Pro (ZX-18200) 1200W Max, 18


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GLi Pro PVX - 2000 Professional Power Amplifier - High Definition


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Gli Pro Xpa-7B 4,000 Watt 2 Channel Bridgeable Power Amplifier With USB/SD Input


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GLI PRO GLQ-420C MIC/AV/KARAOKE MIXER RACK MOUNTABLE


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GLI PRO XPA-7 4,000 WATT DJ POWER AMPLIFIER + USB STICK


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GLI Pro Power-99 2000W Karaoke Receiver/Amplifier w/ Microphone Pre-Amp+Tuner


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NEW GLI PRO SL-2500 DIRECT DRIVE TURNTABLE / S TONEARM


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 GLI pro digital dual 42 band amplifier sistem!!


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New GLI PRO GLX-3990 3 Channel DJ Mixer W/ USB Input


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Gli PRO  F-12BT


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Gli Pro Xpa-9 5,000 Watt 2 Channel Bridgeable Power Amplifier With USB/SD Inputs


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GLI PRO PVX3000 3,000 WATT POWER AMPLIFIER DJ RACK AMP


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(2) GLI PRO XL1880 18


(2) GLI PRO XL1880 18″ 1600 Watt 7-Way PA Speakers With Oversized Horns


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Gli Pro Xpa-7Y 4,000 Watt 2 Channel Bridgeable Power Amplifier With USB/SD Input


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GLI Pro XL-850 8


GLI Pro XL-850 8″ 300 Watt 8 Ohms DJ Speaker


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GLI PRO PVX9000 10,000 WATT POWER AMPLIFIER DJ RACK AMP


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GLI PRO XL1880 18


GLI PRO XL1880 18″ 800 Watt 7-Way PA Speaker With Oversized Horn


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Gli Pro Xpa-9 5,000 Watt 2 Channel Bridgeable Power Amplifier + 8GB USB Drive


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Gli Pro Xpa-7Y 4,000 Watt 2 Channel Bridgeable Power Amplifier + 8 GB USB Drive


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Pair GLI Pro XL-850 8


Pair GLI Pro XL-850 8″ 600 Watt 8 Ohms DJ Speakers


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Pair (2) GLI PRO XL1895 18


Pair (2) GLI PRO XL1895 18″ 1,000 Watt Passive PA/DJ Speaker Monitors


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GLI PRO SL-2100 Belt Drive DJ Turntables S-Tonearms


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GLI PRO XL1895 18


GLI PRO XL1895 18″ 1,000 Watt Passive PA/DJ Speaker Monitor


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Pair (2) GLI PRO SL-2100 Belt Drive DJ Turntables S-Tonearms


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GLI Pro XA5500 3500 Watt Power Amplifier DJ/Pro Audio Stereo 2U Rack Mount Amp


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aFe Pro5R Air Intake 06-08 VW Jetta GLI 2.0L L4 Turbo


aFe Pro5R Air Intake 06-08 VW Jetta GLI 2.0L L4 Turbo


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aFe Pro Dry Air Intake 06-08 VW Jetta GLI 2.0L L4 Turbo


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Gli Pro CX-750 -3 Way Stereo Crossover


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Gli Pro  Scratch 8 Dual CD Player w/USB & SD Card Slot


Gli Pro Scratch 8 Dual CD Player w/USB & SD Card Slot


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Gli Pro Scratch 11.0 Professional Dual CD/USB/SD Slot


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GLI Pro XL-1080   10


GLI Pro XL-1080 10″ Carpeted Speaker w/Full Grill


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Gli Pro SE-908 Sound Effects Machine


Gli Pro SE-908 Sound Effects Machine


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GLI Pro Gooseneck light for Mixer


GLI Pro Gooseneck light for Mixer


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GLI Pro Wire/Wireless Microphone WM-6501


GLI Pro Wire/Wireless Microphone WM-6501


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Gli PRO  PUNCH 10  USB Professional 10


Gli PRO PUNCH 10 USB Professional 10″ Powered Speaker


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Gli PRO  PUNCH 12 USB Professional 12


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Gli PRO  PUNCH 15  Professional 15


Gli PRO PUNCH 15 Professional 15″ Powered Speaker


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Gli Pro Xpa7yellow Glipro 19


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Pair Of GLI Pro SL-2500 Direct Drive Professional Turntables / S Tonearms


Pair Of GLI Pro SL-2500 Direct Drive Professional Turntables / S Tonearms


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GLI Pro 800S 3800 Watt Rack Mount Pro Audio DJ Stereo Power Amplifier + USB/SD


GLI Pro 800S 3800 Watt Rack Mount Pro Audio DJ Stereo Power Amplifier + USB/SD


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4 GLI PRO ZX-18200 18


4 GLI PRO ZX-18200 18″ 4800 Watt Raw DJ Subwoofers SUBS


$339.95

Physalaemin-Like Peptides

Definition
Physalaemin-like peptides group is represented in the amphibian skin by the following three members – Physalaemin, Phyllomedusin and Uperolein. Two important physalaemin-like peptides occur outside the amphibian skin: eledoisin and substance P (SP).

Discovery
Physalaemin, the prototype of the group, first isolated in a pure form from methanol extracts of the skin of Physalaemus bigilonigerus (fuscumaculatus) and is also present in skin extracts of other Physalaemus species as well (Physalaemus centralis, Physalaemus bresslaui)1. Phyllomedusin, isolated from methanol extracts of the skin of the Amazonian hylid frog Phyllomedusa bicolor 2. Uperolein, found in the skin of Australian amphibians belonging to the genera Uperoleia and probably also Taudactylus. Eledoisin was discovered in the salivary glands of certain Mediterranean species of octopus3. SP was discovered in 1931 by von Euler and Gaddum as a tissue extract that caused intestinal contraction in vitro4.

Structural Charachterisics
Physalaemin-like peptide belong to tachykinin (TKs) peptide family. Bio-assay and chemical analysis showed that physalaemin is closely related to elodoisin, both from a biological and chemical point of view5. Two physalaemin (PHY)-like immunoreactive peptides reflects homology at amino acid residues 1, 3, 4 and 5 for the mammalian and amphibian residues 6. Uperolein which is an  physalaemin-like endecapeptide, has been shown to be selective for Neurokinin 1 receptor. Analysis of NMR data indicates that the global fold of Uperolein can be explained in terms of equilibrium between 310-helix and alpha-helix from residues 5 to 11. An extended highly flexible N-terminus displays some degree of order and a possible turn structure. A comparison between the structures of Uperolein and SP, a prototype and endogenous Neurokinin 1 receptor agonist, indicates several common features in the distribution of hydrophobic and hydrophilic residues. Both the peptides show an amphiphilic character towards the middle region. The similarities suggest that the molecules interact with the receptor in an analogous manner7.

The sequence of physalaemin is Pyr-Ala-Asp-Pro-Asn-Lys-Phe-Tyr-Gly-Leu-Met-NH2.

The sequence of Phyllomedusin is Pyr-Asn-Pro-Asn-Arg-Phe-Ile-Gly-Leu-Met-NH2

The sequence of Uperolein is Pyr-Pro-Asp-Pro-Asn-Ala-Phe-Tyr-Gly-Leu-Met-NH2.

The sequence of Eledoisin is Pyr-Pro-Ser-Lys-Asp-Ala-Phe-Ile-Gly-Leu-Met-NH2

The sequence of SP is Arg-Pro-Lys-Pro-Gln-Gln-Phe-Phe-Gly-Leu-Met-NH2

Mode of action
The striking hypotensive effects of the tachykinins observed in some animal species, as a consequence of intense vasodilation in several peripheral vascular beds, must be considered a direct effect of the peptides on the blood vessel wall.  The site of action of the tachykinins is endothelium of the blood vessel. Thus tachykinins may act to promote the release of endogenous factors from the endothelium that is able to reduce the tone of the arterial smooth muscle fibers. The SP receptor is a G protein-coupled receptor, in many respects similar to other well-studied receptors in psychiatry, particularly monoamine receptors .  The interaction of SP with its receptor activates Gq, which in turn activates phospholipase C to break down phosphatidyl inositol bisphosphate into inositol trisphosphate (IP3) and diacylglycerol (DAG). IP3 acts on specific receptors in the sarcoplasmic reticulum to release intracellular stores of Ca2+, while DAG acts via protein kinase C to open L-type calcium channels in the plasma membrane. The rise in intracellular [Ca2+] induces the tissue response. With an array of actions as diverse as that seen with SP, there is scope for numerous therapeutic possibilities 8.

Functions
TKs display a number of potent pharmacological actions in the periphery and in the central nervous system. Eledoisin, kassinin, and, to a lesser extent, physalaemin caused release of vasopressin, with ensuing antidiuresis. In dogs Physalaemin was very effective in antagonizing the pressor effects of noradrenaline and angiotensin II given at doses 100 and 10 times higher, respectively.In human volunteers, eledoisin given by rapid intravenous injection (threshold 15–20 pmol/kg) decreased blood pressure, caused spinal fluid hypertension, increased the rate of respiration and caused skin vasodilation, particularly in the head. Physalaemin and, to a considerably lesser extent eledoisin and SP (Losay et al., 1977) displayed a very potent vasodilator action9. Eledoisin infused intravenously in the dog at 0.01 nmol/kg/min decreased cerebral blood flow (−22%), with an increase (+20%) in vascular resistance (Beretta Anguissola et al., 1966)10.

References
1.Anastasi A, Erspamer V, Cei JM (1964). Isolation and amino acid sequence of physalaemin, the main active polypeptide of the skin of Physalaemus fuscumaculatus. Arch Biochem Biophys., 108:341-348.
2.Anastasi A, Erspamer GF (1970). Occurrence of phyllomedusin, a physalaemin-like decapeptide, in the skin of Phyllomedusa bicolor. Experientia., 26(8):866-867.
3.Jaeger W (1988). Treatment of a severe course of keratoconjunctivitis sicca with eledoisin. Klin Monbl Augenheilkd.,192(2)163-166.
4.    Senba E, Tohyama M (1985). Origin and fine structure of substance P-containing nerve terminals in the facial nucleus of the rat:an immunohistochemical study. Exp Brain Res., 57(3):537-546.
5.Bernardi L, Bosisio G, Goffredo O, De Castiglione R (1964). Synthesis of physalaemin. Experientia., 20(9):490-492.
6.Dike A, Cowsik SM (2006). Solution structure of amphibian tachykinin Uperolein bound to DPC micelles. J Struct Biol., 156(3):442-52.
7.Wilson WE, Harvan DJ, Hamm C, Lazarus LH, Klapper DG, Yajima H, Hayashi Y (1986). Physalaemin-like immunoreactive peptides from rabbit stomach. Int J Pept Protein Res. 28(1):58-66.
8.Severini C, Improta G, Falconieri-Erspamer G, Salvadori S, Erspamer V (2002). The tachykinin peptide family. Pharmacol Rev., 54(2):285-322.
9.   Losay J, Mroz E, Tregear GW, Leeman SE, Gamble WJ (1977. Action of substance P on the coronary blood flow in the isolated dog heart. in Substance P. Raven Press, New York, 287–293.
10. Beretta Anguissola A, Feruglio FS, Campus S, Chiandussi L, Pandolfo G, Berti G (1966). The effects of eledoisin and bradykinin on the general and visceral circulation. in Hypotensive Peptides, Springer-Verlag, New York, 430–440.

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My GLi Pro SL-2500 Turntable, “Frankencart” And 175 45s

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