ピリメサミン

ピリメサミン 化学構造式
58-14-0
CAS番号.
58-14-0
化学名:
ピリメサミン
别名:
チンズリン;ジアミノピリタミン;ピリメシダン;5-(4-クロロフェニル)-6-エチル-2,4-ピリミジンジアミン;クロリジン;5-(4-クロロフェニル)-6-エチルピリミジン-2,4-ジアミン;ピリメサミン;ダラプラム;ダラクロル;ピリメタミン/ダプソン,(12.5mg:100mg);エルバプレリナ;チンデュリン;マラシド;2,4-ジアミノ-5-(p-クロロフェニル)-6-エチルピリミジン;5-(4-クロロフェニル)-2,4-ジアミノ-6-エチルピリミジン;5-(p-クロロフェニル)-6-エチル-2,4-ピリミジンジアミン;2,4-ジアミノ-5-(4-クロロフェニル)-6-エチルピリミジン;マロシド;ダラプリム;マロプリム
英語名:
Pyrimethamine
英語别名:
Daraprim;Fansidar;Chloridine;PYRIMETHAMIN;Pirimetamina;Pyremethamine;wr2978;bw50-63;RP 4753;WR 2978
CBNumber:
CB8461315
化学式:
C12H13ClN4
分子量:
248.71
MOL File:
58-14-0.mol
MSDS File:
SDS

ピリメサミン 物理性質

融点 :
233-234°C
沸点 :
393.35°C (rough estimate)
比重(密度) :
1.2171 (rough estimate)
屈折率 :
1.6110 (estimate)
貯蔵温度 :
Keep in dark place,Inert atmosphere,Room temperature
溶解性:
0.25 g を 1 容量のメタノール R と 3 容量のジクロロメタン R の混合物に溶解し、同じ溶媒で 10 mL に希釈しました。溶液は透明であり (2.2.1)、参照溶液 BY6 (2.2.2、方法 II) より暗くはありませんでした。
酸解離定数(Pka):
pKa 7(t=20.0) (Uncertain)
色:
ホワイトからオフホワイト
水溶解度 :
<0.01 g/100 mL で 21 ºC
極大吸収波長 (λmax):
276nm(lit.)
Merck :
14,7985
BRN :
219864
BCS Class:
2 (CLogP), 4 (LogP),3
安定性::
安定していますが、光に敏感です。可燃性。強力な酸化剤とは相容れない。
CAS データベース:
58-14-0(CAS DataBase Reference)
IARC:
3 (Vol. 13, Sup 7) 1987
NISTの化学物質情報:
Pyrimethamine(58-14-0)
EPAの化学物質情報:
Pyrimethamine (58-14-0)
安全性情報
  • リスクと安全性に関する声明
  • 危険有害性情報のコード(GHS)
主な危険性  Xn
Rフレーズ  22-36
Sフレーズ  26
RIDADR  3249
WGK Germany  3
RTECS 番号 UV8140000
国連危険物分類  6.1(b)
容器等級  III
HSコード  29335990
有毒物質データの 58-14-0(Hazardous Substances Data)
毒性 LD50 oral in rat: 440mg/kg
化審法 (9)-539, (9)-696, (9)-1124, (9)-270
絵表示(GHS) GHS hazard pictograms
注意喚起語 警告
危険有害性情報
コード 危険有害性情報 危険有害性クラス 区分 注意喚起語 シンボル P コード
H302 飲み込むと有害 急性毒性、経口 4 警告 GHS hazard pictograms P264, P270, P301+P312, P330, P501
注意書き
P264 取扱い後は皮膚をよく洗うこと。
P264 取扱い後は手や顔をよく洗うこと。
P270 この製品を使用する時に、飲食または喫煙をしないこ と。
P301+P312 飲み込んだ場合:気分が悪い時は医師に連絡する こと。
P501 内容物/容器を...に廃棄すること。

ピリメサミン 価格 もっと(16)

メーカー 製品番号 製品説明 CAS番号 包装 価格 更新時間 購入
富士フイルム和光純薬株式会社(wako) W01W0116-1863 ピリメタミン標準品 99.0+% (HPLC)99.0+% (After Drying)(Titration)
Pyrimethamine Standard 99.0+% (HPLC)99.0+% (After Drying)(Titration)
58-14-0 200mg ¥12200 2024-03-01 購入
富士フイルム和光純薬株式会社(wako) W01MPB02194180 ピリメサミン
Pyrimethamine
58-14-0 1g ¥18900 2024-03-01 購入
富士フイルム和光純薬株式会社(wako) W01MPB02194180 ピリメサミン
Pyrimethamine
58-14-0 5g ¥23400 2024-03-01 購入
東京化成工業 P2037 ピリメタミン >98.0%(HPLC)(T)
Pyrimethamine >98.0%(HPLC)(T)
58-14-0 1g ¥3900 2024-03-01 購入
東京化成工業 P2037 ピリメタミン >98.0%(HPLC)(T)
Pyrimethamine >98.0%(HPLC)(T)
58-14-0 5g ¥12900 2024-03-01 購入

ピリメサミン 化学特性,用途語,生産方法

外観

白色~わずかにうすい褐色, 結晶~粉末

溶解性

酢酸に溶け、水にほとんど溶けない。

解説

ピリメサミン,化学的に合成される。結晶性。融点 233~234℃。水に不溶。エチルアルコールにわずかに可溶。

ブリタニカ国際大百科事典 小項目事典 ブリタニカ

用途

抗マラリア薬で,葉酸と拮抗作用をもつ。副作用は貧血。

効能

抗マラリア薬

化学的特性

White Solid

使用

For the treatment of toxoplasmosis and acute malaria; For the prevention of malaria in areas non-resistant to pyrimethamine.
Pyrimethamine is a dihydrofolate reductase inhibitor, like the biguanides, and is structurally related to trimethoprim. It is seldom used alone. Pyrimethamine in fixed combinations with dapsone or sulfadoxine is used for treatment and prophylaxis of chloroquine-resistant falciparum malaria. The synergistic activities of pyrimethamine and sulfonamides are similar to those of trimethoprim/sulfonamide combinations. Resistant strains of Plasmodium falciparum have appeared world wide. Prophylaxis against falciparum malaria with pyrimethamine alone is therefore not recommended. Most strains of Plasmodium vivax have remained sensitive. Pyrimethamine is also used in combination with a sulfonamide for the treatment of Toxoplasmosis. It is slowly absorbed from the gastrointestinal tract with peak plasma levels 4–6 hours after dosing. Pyrimethamine is bound to plasma proteins and is extensively metabolized before excretion. Its elimination half-life is 3–5 days.

定義

ChEBI: An aminopyrimidine that is pyrimidine-2,4-diamine which is substituted at position 5 by a p-chlorophenyl group and at position 6 by an ethyl group. It is a folic acid antagonist used as an antimalarial or with a sulfonamide to treat toxoplasmo is.

適応症

Pyrimethamine (Daraprim) is the best of a number of 2,4- diaminopyrimidines that were synthesized as potential antimalarial and antibacterial compounds. Trimethoprim (Proloprim) is a closely related compound.
Pyrimethamine is well absorbed after oral administration, with peak plasma levels occurring within 3 to 7 hours. An initial loading dose to saturate nonspecific binding sites is not required, as it is with chloroquine. However, the drug binds to tissues, and therefore, its rate of renal excretion is slow. Pyrimethamine has a half-life of about 4 days. Although the drug does undergo some metabolic alterations, the metabolites formed have not been totally identified.

一般的な説明

Odorless white crystalline powder. Tasteless. An antimalarial drug.

空気と水の反応

Pyrimethamine is a diaminopyrimidine which is structurally related to trimethoprim. It is effective against erythrocytic stage of Plasmodium (P) falciparum and less so against P. vivax, P. ovale and P. malariae. Pyrimethamine also inhibits the sporogony in the mosquito, resulting in a decrease of transmission of the infection within the community[1].
The mechanism of action of pyrimethamine is related to its inhibition of dihydrofolic reductase necessary for the folic acid synthesis in the parasite. Pyrimethamine acts slowly and is not recommended as monotherapy for acute malaria attacks. Resistance to pyrimethamine developed soon when the drug was used on a large scale as monoprophylaxis [1]. In resistant strains, the enzyme dihydrofolic reductase binds to pyrimethamine several hundred times less than in sensitive strains [2]. This high grade resistance is probably a onestep mutation and cannot be overcome by increasing the dose. However, when combined with long-acting sulphonomides (sulphadoxine), the effect of pyrimethamine is potentiated and the risk of developing resistant strains is far less.

反応プロフィール

Pyrimethamine together with sulphadoxine (Fansidar) is used in the treatment of P. falciparum malaria (cf. Sulphadoxine: Indications). Pyrimethamine is also valuable in the treatment of toxoplasmosis.

火災危険

Pyrimethamine in combination with sulphadoxine (Fansidar) can cause severe cutaneous adverse reactions (cf. Sulphadoxine: Side effects). Agranulocytosis occurs quite frequently (1/2000) and fatalities have been reported when pyrimethamine is combined with dapsone [3]. When given alone, life-threatening adverse reactions are very rare and the drug is generally well tolerated. Megaloblastic anaemia may, however, occur during long-term treatment with high doses (i.e. for toxoplasmosis) and can be prevented by folinic acid supplementation [4].

生物活性

During long-term treatment with high doses, folinic acid supplement is usually given.

作用機序

The combination of pyrimethamine with a long-acting sulfonamide, sulfadoxine, which blocks dihydrofolate synthesis by blocking incorporation of PABA into the dihydrofolate, is called Fansidar, which produces sequential blockage of tetrahydrofolate synthesis similar to that reported for treatment of bacterial infections. Plasmodium enzymes catalyzing folic acid synthesis differ from those enzymes found in other organisms. A single bifunctional protein present in Plasmodium sp. catalyzes the phosphorylation of 6-hydroxymethyl-7,8-hydropterin (a pyrophosphokinase) and the incorporation of PABA into dihydropteroic acid. A second bifunctional enzyme catalyzes the reduction of dihydropteroic acid and thymidylic acid synthesis. As a result, the drug combination (Fansidar) appears to have improved drug-mediated disruption of folic acid in Plasmodium sp.. This combination has been used with quinine for the treatment and prevention of chloroquine-resistant malaria (Plasmodium falciparum, Plasmodium ovale, Plasmodium vivax, and Plasmodium malaria). The combination therapy (Fansidar) has the added advantage of being inexpensive, which is essential for successful therapy in developing countries. When used on its own, pyrimethamine is a blood schizonticide without effects on the tissue stage of the disease.

臨床応用

Pyrimethamine has been recommended for prophylactic use against all susceptible strains of plasmodia; however, it should not be used as the sole therapeutic agent for treating acute malarial attacks. As mentioned previously, sulfonamides should always be coadministered with pyrimethamine (or trimethoprim), since the combined antimalarial activity of the two drugs is significantly greater than when either drug is used alone. Also, resistance develops more slowly when they are used in combination. Sulfonamides exert little or no effect on the blood stages of P. vivax, and resistance to the dihydrofolate reductase inhibitors is widespread.
In addition to its antimalarial effects, pyrimethamine is indicated (in combination with a sulfonamide) for the treatment of toxoplasmosis.The dosage required is 10 to 20 times higher than that employed in malarial infections.

副作用

Relatively few side effects are associated with the usual antimalarial dosages. However, signs of toxicity are evident at higher dosages, particularly those used in the management of toxoplasmosis. Many of these reactions reflect the interference of pyrimethamine with host folic acid metabolism, especially that occurring in rapidly dividing cells. Toxic symptoms include anorexia, vomiting, anemia, leukopenia, thrombocytopenia, and atrophic glossitis. CNS stimulation, including convulsions, may follow an acute overdose.The side effects associated with the pyrimethamine–sulfadoxine combination include those associated with the sulfonamide and pyrimethamine alone. In addition, there is evidence of a greater incidence of allergic reactions, particularly toxic epidermal necrolysis and Stevens-Johnson syndrome, with the combination. This carries an estimated mortality of 1:11,000 to 1:25,000 when used as a chemoprophylactic.

安全性プロファイル

Poison by ingestion, subcutaneous, and intraperitoneal routes. Experimental teratogenic and reproductive effects. Questionable carcinogen. Human mutation data reported. When heated to decomposition it emits very toxic fumes of Cland NOx. Used as an antimalarial drug for humans and to treat toxoplasmosis in hogs.

ピリメサミン 上流と下流の製品情報

原材料

準備製品


ピリメサミン 生産企業

Global( 502)Suppliers
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ピリメサミン  スペクトルデータ(1HNMR)


58-14-0(ピリメサミン)キーワード:


  • 58-14-0
  • 2,4-Diamino-5-(4-chlorophenyl)-6-ethylpyrimidine
  • [2-amino-5-(4-chlorophenyl)-6-ethyl-pyrimidin-4-yl]amine
  • Pyrimethamine,5-(4-Chlorophenyl)-6-ethyl-2,4-pyrimidinediamine
  • Pyrimethamine (200 mg)
  • PyriMethaMine,darapriM
  • 5-(p-chlorophenyl)-6-ethyl-4-pyrimidinediamine
  • BW 50-63
  • bw50-63
  • Chloridin
  • Chloridyn
  • Darachlor
  • Daraclor
  • Darapram
  • 5-(4’-chlorophenyl)-2,4-diamino-6-ethylpyrimidine
  • 5-(4'-Chlorophenyl)-2,4-diamino-6-ethylpyrimidine
  • 5-(4-Chlorophenyl)-2,4-diamino-6-ethylpyrimidine
  • 5-(4-chlorophenyl)-6-ethylpyrimidine-2,4-diyldiamine
  • 5-(P-Chlorophenyl)-6-ethyl-2,4-diaminopyrimidine
  • Pyrimidine,2,4-diamino-5-(p-chlorophenyl)-6-ethyl-
  • RP 4753
  • Tindurin
  • Tinduring
  • WR 2978
  • wr2978
  • PYRIMETHAMINE
  • Daraprime
  • Diaminopyritamin
  • Erbaprelina
  • Khloridin
  • Malacid
  • チンズリン
  • ジアミノピリタミン
  • ピリメシダン
  • 5-(4-クロロフェニル)-6-エチル-2,4-ピリミジンジアミン
  • クロリジン
  • 5-(4-クロロフェニル)-6-エチルピリミジン-2,4-ジアミン
  • ピリメサミン
  • ダラプラム
  • ダラクロル
  • ピリメタミン/ダプソン,(12.5mg:100mg)
  • エルバプレリナ
  • チンデュリン
  • マラシド
  • 2,4-ジアミノ-5-(p-クロロフェニル)-6-エチルピリミジン
  • 5-(4-クロロフェニル)-2,4-ジアミノ-6-エチルピリミジン
  • 5-(p-クロロフェニル)-6-エチル-2,4-ピリミジンジアミン
  • 2,4-ジアミノ-5-(4-クロロフェニル)-6-エチルピリミジン
  • マロシド
  • ダラプリム
  • マロプリム
  • ピリメタミン
  • ピリメタミン標準品
  • ピリメタミン (JAN)
  • 抗マラリア薬
  • その他の有機分析用の標準物質
  • 生活関係標準物質
  • 食料品
  • 有機標準物質
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