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Pramlintide

Pramlintide Struktur
CAS-Nr.
Englisch Name:
Pramlintide
Synonyma:
CBNumber:
CB61171802
Summenformel:
Molgewicht:
0
MOL-Datei:
Mol file

Pramlintide Eigenschaften

Sicherheit

Pramlintide Chemische Eigenschaften,Einsatz,Produktion Methoden

Beschreibung

Pramlintide is an analogue of amylin in which proline has replaced the normal amino acids at positions 25, 28, and 29, as indicated above. The result of these substitutions is an increase in water solubility and a reduced tendency for self-aggregation.

Verwenden

Antidiabetic.

Allgemeine Beschreibung

Pramlintide is the 25-L-proline-28-L-proline-29-L-prolinetrisubstitution product of human amylin. The marketedformulation (Symlin) is an acetate salt, the exactcomposition of which may not be public-domain knowledge,although salts containing up to four acetic acidmolecules per pramlintide molecule would be possible byvirtue of the free amino terminus andLys1, Arg11, andHis18 residues. The carboxyl terminus of pramlintide, as inamylin, is amidated, and there are no appreciably acidicmoities in the structure; thus, in solution at the pH of bloodand tissues pramlintide would be present almost entirely asone or the other of two significant molecular species, onehaving a +3 charge (histidine imidazole deprotonated anduncharged) predominating modestly over the quadruplyprotonated (+4) species.

Mechanism of action

Amylin receptors have been identified in distinct areas of the brain, including the nucleus accumbens and the dorsal vagal complex. Stimulation of these receptors reduces food intake and depresses GI motility. It is assumed that pranlintide stimulates these receptors, leading to the reported benefits of the drug in patients with diabetes, although the exact mechanism is still poorly understood. Pranlintide causes a moderate reduction in HbA1c and postprandial glucose levels when used in combination with insulin, which has benefits in normalizing fluctuations of circulating glucose levels.

Pharmakokinetik

Pramlintide is administered via subcutaneous injection immediately before meals, reaches maximum circulating concentrations within 20 minutes, and has a half-life of 29 minutes. The drug is eliminated from the body primarily through the kidney. The plasma concentrations are similar to those seen with postprandial amylin. Because the drug is formulated at pH 4.0, it is potentially incompatible with insulin (pH 7.8) if administered within the same syringe, although one study of pramlintide combined with Novolin or Humulin did not show changes in the pharmacokinetics of either drugs.

Clinical Use

Pramlintide’s effects upon administration to patients almostcertainly arise in significant measure from directAMY-mediated actions within the brainstem. Amylin receptorsare abundant in the circumventricular organs, includingthe subfornical organ (where AMY1(a) receptors areknown to be expressed in relative abundance), the organumvasculosum lateralis terminalis, and the area postrema(AMY3(a)

), where the action of pramlintide (or of -cell–secretedamylin) is not precluded by a diffusional BBB.Amylin receptors are also expressed in various other brainareas, in particular the nucleus accumbens, but neitheramylin or pramlintide circulating in the bloodstream arelikely to exert any action at these BBB-shielded locations.Direct amylin receptor–mediated actions of pramlintide in the periphery, if any, remain poorly characterized.Unsurprisingly, though, the appetite-suppressing actions,and benefits of pramlintide and amylin agonists in general,are receiving significant clinical and scientific attention.

Nebenwirkungen

The major side effects reported for pramlintide consist of mild to moderate nausea, with severe nausea appearing in patients using large doses of the drug. The nausea may decrease on continued use of the drug. The rate of hypoglycemia appears to be quite low.

Pramlintide Upstream-Materialien And Downstream Produkte

Upstream-Materialien

Downstream Produkte


Pramlintide Anbieter Lieferant Produzent Hersteller Vertrieb H?ndler.

Global( 23)Lieferanten
Firmenname Telefon E-Mail Land Produktkatalog Edge Rate
Shanghai HongTide Biotechnology Co.,Ltd. 19961912513
sales@hongtide.com China 4595 58
Beijing HuaMeiHuLiBiological Chemical 010-56205725
waley188@sohu.com China 12335 58
Chengdu Youngshe Chemical Co., Ltd. +86-17380623303 +86-17380623303
Caroline@youngshechem.com China 4844 58
Hangzhou Go Top Peptide Biotech 0571-88211921 13355716090
Sales@gotopbio.com China 2858 58
Shaoxing Junyu Biotechnology Co., LTD 0571-88211921 15572296305
sales4@gotopbio.com China 5128 58
Hangzhou Baige Pharmaceutical Technology Co. , Ltd. 0571-85350119 15888826472
15888826472@163.com China 2729 58
Combio (Suzhou) Ltd. 0512-51886999 17706251929
office@combiosz.com China 3000 58
Zhejiang Jiekun Biotechnology Co., Ltd 0571-88211951 13735575465
sales1@gotopbio.com China 4904 58
Guangzhou Xinyanze Biotechnology Co., LTD 18120340188
3239311947@qq.com China 278 58
Baoji Didu Pharmaceutical and Chemical Co., Ltd 02961856358 15829046862
1035@dideu.com China 10011 58

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