DE2150234A1 - (chloro) camptothecin prepn - by oxidn of (chloro) desoxycamptothecin with oxygen - Google Patents

Abstract

Cpds. of formula (I; R=OH) : (where X is H or Cl) are prepd. by treating a soln. of (I; R=H) with O2 in the presence of an oxidn. catalyst, pref. CuCl2, at pH 7.5-4. The solvent is pref. DMF. (I; R=OH, X=H) is camptothecin, a naturally occurring tumour inhibitor. (I; R=OH) are inters. for other camptothecin derivs. (I; R=OH, X=Cl) is a new cpd.

Description

Process for the preparation of cainrtothecin and camptothecin derivatives Camptothecin, a naturally occurring substance, is used as an anti-tumor agent effective. Its synthetic production and the possibility, by devolving the Molecular structure to obtain further variants of this class of compounds, sinu for Technology, research and mechanical application are of great importance.

The invention relates to an advantageous method of manufacture of camptothecin and camptothecin derivatives.

It has been found that compounds of the formula I a) X = H b) X = C1 selective to compounds of the formula II a) X = b) X = C1 can oxidize if molecular oxygen is allowed to act on the dissolved compound I in the presence of an oxidation catalyst.

Salts of the subgroup Met are suitable as oxidation catalysts all, e.g. of copper, silver, chromium, manganese, iron, cobalt, ~ nickel, mercury, Palladium or platinum, especially copper (II) chloride. The amounts of the catalyst are conveniently about 1: 1 to 10: 1 (weight ratio substance : Catalyst).

Suitable solvents for the compound I are all customarily compounds or liquids that can be used for such oxidations, such as alcohols, e.g. methanol, tert-butanol, ether, e.g. Tetrahydrofuran, dioxane, ethylene glycol dimethyl ether, Dimethylformamide, dimethyl sulfoxide, acetonitrile.

The solution must be approximately neutral or slightly acidic for the oxidation, i.e. about pK 7.5 down to about rh 4.

Room temperature is preferred as the oxidation temperature, but it is Range of about 00 to 800C is generally suitable. The end point of the inventive Oxidation can be carried out, for example, by comparing a sample using thin-layer chromatography determine the reaction mixture with an authentic sample.

The advantages of this new synthesis over the one described in J. Am. Chem.

Soc., August 11, 1971, procedure described by Stork and Schultz are: The compound I is of greater purity and in 12 stages from the easily accessible Tryptamine available, on the other hand you need in the known procedure, starting from a more difficult to access connection, a total of 17 steps.

The yields of the process according to the invention are good and one has the option of using a wide variety of camptothecin derivatives, in which X also have other meanings and / or the benzene ring can be substituted without to create greater difficulties. Of the camptothecin derivatives is because of easier attack of the quinoline system during metabolism, lower toxicity than to be expected from the natural substance itself.

The starting compounds I are according to the method of the German patent. ... ... (patent application P 21 42 715.6 dated August 26, 1971) available. For example, the compound Ia is obtained if, for example, in the compound III according to methods known per se, the chlorine is replaced by hydrogen reductively with the aid of a partially poisoned catalyst, for which, for example, palladium / barium sulfate is suitable as the catalyst and methanol as the solvent. The twist that can be obtained in this way IV is then subjected to lactone ring closure. These precursors to the compounds I are according to the German patent.

(Patent application P 20 23 514.7 of May 14, 1970) and additional patent. ... ... (P 20 61 359.6 of 12.12.1970) accessible. Finally, the alkylation takes place to I.

Example 1 Dissolves 3 mg of deoxycamptothecin or chlorodeoxycamptothecin one freshly distilled in 3 ccm. Dimethylformamide, mixed with 1 mg CuIICl2 and conducts oxygen at room temperature. After 6 hours it is poured into 0.01 N hCl and extracted with methylene chloride. After evaporation of the solvent, one obtains 2.4 ing (80 to the oxidized compound, adorn properties 6, ci X = ti (mass spectrum, UV spectrum, NMR spectrum and thin-layer chromatographic RF value) coincide with those of natural camptothecin.

To prepare the deoxycamptothecin, the compound III in Dissolved methanol (10 ccm Ch30h for 100 mg substance) and after adding 20 mg Pd / BaS04 hydrogenated until 1 mol of hydrogen is absorbed (approx. 20 min). After filtering off the catalyst is evaporated in vacuo and 70-75% of the chlorine-free compound is obtained IV. The further processing of IV is then via reduction, for example with di-isobutyl aluminum hyaride and lactonization carried out, for example, with trifluoroacetic acid,

Claims (4)

Patent claims O Process for the preparation of camptothecin and camptothecin derivatives, characterized in that compounds of the formula a) X = b) X: C1 in dissolved form by exposure to molecular oxygen in the presence of an oxidation catalyst at pH from about 7.5 to about 4, selective to compounds of the formula a) X = hb) X = Cl oxidized. 2. The method according to claim 1, characterized in that as Oxidation catalyst copper (II) chloride used. 3. The method according to claim 1 and claim 2, characterized in that that dimethylformamide is used as the solvent. 4. The compound of formula