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6-(Dimethylamino)purine структурированное изображение

6-(Dimethylamino)purine

  • английское имя6-Dimethylaminopurine
  • CAS №938-55-6
  • CBNumberCB0421579
  • ФормулаC7H9N5
  • мольный вес163.18
  • EINECS213-344-3
  • номер MDLMFCD00005573
  • файл Mol938-55-6.mol
химическое свойство
Температура плавления 259-262 °C(lit.)
Температура кипения 162 °C (50 mmHg)
плотность 1.1407 (rough estimate)
показатель преломления 1.6380 (estimate)
Fp 110 °C
температура хранения -20°C
растворимость methanol: 0.1 g/mL, clear
форма prilled
пка 9.38±0.20(Predicted)
цвет off-white to yellow
БРН 7634
ИнЧИКей BVIAOQMSVZHOJM-UHFFFAOYSA-N
Справочник по базе данных CAS 938-55-6(CAS DataBase Reference)
Рейтинг продуктов питания EWG 1
FDA UNII 649SA4S2CV
Справочник по химии NIST 1H-Purin-6-amine, N,N-dimethyl-(938-55-6)
Заявления об опасности и безопасности
Коды опасности
WGK Германия 3
RTECS UO7440636
кода HS 29335990

рисовальное письмо(GHS)

  • рисовальное письмо(GHS)

    GHS hazard pictograms

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6-(Dimethylamino)purine MSDS

6-(Dimethylamino)purine химические свойства, назначение, производство

Химические свойства

white to light yellow crystal powder

Использование

6-Dimethylaminopurine is a serine threonine protein kinase inhibitor. It inhibits the germinal vesicle breakdown and the meiotic maturation of oocytes. It can be used to rtificially lengthen the pre-maturation period of oocyte growth, in vitro, by inhibiting germinal vesicle breakdown in mouse and human oocytes.

прикладной

6-(Dimethylamino)purine has been used:
as a supplement in GR-1 aa medium (bovine medium) for parthenogenetic activation of bovine oocytes to study its potential for embryo development.
in the activation step during the production of nuclear transfer embryos.
as a supplement in HCR2aa medium to activate interspecies embryos derived from interspecies somatic cell nuclear transfer (iSCNT) technique.
A purine antagonist.
In the benzodiazepine receptor (BZR) binding assay, it inhibits the binding of 1.5 nM [3H]diazepam at 100uM in rat brains.

Подготовка

6-Dimethylaminopurine synthesis: 2-Methylmercapto-4-amino-6-dimethylaminopyrimidine (VI) was smoothly nitrosated in 10% acetic acid to the 5-nitrosopyrimidine (V) in 95% yield. Reduction of V with sodium hydrosulfite to the triamine (IV), followed by formylation gave the 5-formamidopyrimidine (VII) in 76% over-all yield for the two steps. Reductive formylation of V directly to VI1 with zinc and formic acid, although more rapid, was less efficient (50% yield). Ring closure of VII to 2-methyhercapto-6-dimethylaminopurine (X) was best done on a small scale by short fusion at 250°(99% yield), although boiling quinoline, formamide, or dilute alcoholic sodium hydroxide could also be employed. The latter reagent was most efficient on a large scale. Desulfurization of X with Raney nickel (7) in 1 N sodium hydroxide at 100° afforded the final product, 6-dimethylaminopurine (XII) in 43% yield.This compound was identical in all respects with the C7H9N5 moiety from puromycin (2).
synthesis of 6-Dimethylaminopurine

Определение

ChEBI: 6-Dimethylaminopurine is a tertiary amine that is adenine substituted at N-6 by geminal methyl groups. It is functionally related to an adenine.

Общее описание

6-(Dimethylamino)purine (6-DMAP) is a purine-based metabolite with two condensed heterocyclic rings and two methyl groups linked to the amino group of the purine unit of adenine.

Биохимия/физиол Действия

6-(Dimethylamino)purine (6-DMAP) is a protein kinase and cyclin-dependent kinase inhibitor. It acts as a secondary metabolite and mediates RNA modification. 6-DMAP is a potent cytokinetic inhibitor and is used in parthenogenesis and meiosis studies. It is also used to promote pronuclei formation in mammalian oocytes. 6-DMAP is a dual fluorescence molecule according to femtosecond fluorescence up-conversion spectroscopy studies.

Методы очистки

It is purified by recrystallisation from H2O, EtOH (0.32g in 10mL) or CHCl3. [Albert & Brown J Chem Soc 2060 1954, UV: Mason J Chem Soc 2071 1954.] The monohydrochloride crystallises from EtOH/Et2O, m 2 5 3o(dec) [Elion et al. J Am Chem Soc 74 411 1952], the dihydrochloride has m 225o(dec) and the picrate has m 245o (235-236.5o) [Fryth et al. J Am Chem Soc 80 2736 1958]. [Beilstein 26 III/IV 3566.]

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