CYCLOPHOSPHAMIDE FILM-COATED TABLETS

Abstract

1. [sic] The invention relates to film-coated tablets with cyclophosphamide as active compound, which in the core comprise cyclophosphamide, one or more fillers, one or more dry binders but no preswollen starch, flow regulators and lubricants.

Description

[0001] The invention relates to cyclophosphamide film-coated tablets and to a process for their preparation. The invention can be used in the pharmaceutical industry

[0002] Cyclophosphamide is an agent having a broad antitumor spectrum which has been introduced [sic] in chemotherapy for decades for the treatment of solid tumors such as mastocarcinoma, bronchial carcinoma and hemoblastoses.

[0003] Until now, on [sic] known pharmaceutical forms have been tablets, coated tablets and mainly lyophilizates with various auxiliaries such as mannitol or urea.

[0004] EP 0519099 describes tablets comprising cyclophosphamide and preswollen starch, prepared by a direct tableting process.

[0005] Since cyclophosphamide is dangerous to health and for this reason direct contact with this substance represents a potential risk, the tablets prepared according to EP 0519099 are used as cores for press-coated tablets and thus coated by means of a second tableting. This process is technically complicated. Special tableting machines are furthermore needed for the preparation of press-coated tablets.

[0006] The need thus exists for a simple and economical preparation of solid pharmaceutical form [sic] comprising cyclophosphamide for oral administration.

[0007] It is necessary to take into consideration here that the pharmaceutical forms have to be coated in order that direct contact with the cytotoxic active compound is avoided.

[0008] It is moreover known that cyclophosphamide is chemically labile, thus the stability of the pharmaceutical forms must also be taken into consideration.

[0009] Surprisingly, it has been possible to prepare film-coated tablets comprising cyclophosphamide without the use of preswollen starch.

[0010] Suitable auxiliaries were selected on the basis of the compatibility investigations mentioned in Example I [sic] . It was surprising in this context that the stability of cyclophosphamide is somewhat indifferent in the presence of preswollen starch.

[0011] It was moreover surprising that the finished film-coated tablets exhibit an adequate stability although the active compound, due to the preparation, is stressed during the film-coating process by moisture and heat.

EXAMPLE 1

[0012] Investigations on the Compatibility of Cyclophosphamide with Various Tableting Auxiliaries

[0013] 53.5 mg of cyclophosphamide and 86.5 mg of (auxiliary 1-10) [sic] or 3.0 mg of (auxiliary 11-18) [sic] were in each case mixed and compressed. The pressed tablets were stored at 31° C. for 6 months. The decomposition of the active compound was carried out [sic] by means of chloride determination.

[0014] The results are summarized in the following table.

		Decomposition	Dis-
Function of the		of cyclo-	colora-
auxiliary	Auxiliary	phosphamide	tion
FILLER	1	Lactose, anhydrous	2.52	++
	2	Calcium phosphate	3.85	−
	3	Calcium phosphate	2.02	−
		anhydrous
	4	Emcompress	1.50
		(CaHPO4)
	5	D-mannitol	1.15	−
	6	Lactose	0.70	−
		monohydrate
FILLER/DRY	7	Microcrystalline	1.50-1.73*	−
BINDER/		cellulose
DISINTEGRATION	8	Cellulose (Elcema)	0.85-1.32*	−+
PROMOTER	9	Preswollen starch	1.02	−+
	10	Cornstarch	0.75	−
DISINTEGRATION	11	Crosslinked poly-	1.5	++
PROMOTER		vinyl pyrrolidone
FLOW	12	Highly disperse	0.46-1.72*	−+
REGULATOR		silica
FLOW	13	Magnesium stearate	1.51	−+
REGULATOR/	14	Stearic acid	0.94	−+
LUBRICANT	15	Glycerol	0.82	−
		palmitostearate
	16	Polyethylene	0.68	−
		glycol
	17	Talc	0.55	−
	18	Glycerol	0.30	−
		monobeherate [sic]
*Dependent on type

EXAMPLE 2

[0015] Preparation of Tablet Cores (50 mg of Cyclophosphamide)

[0016] Direct Tableting

[0017] 0.535 mg of cyclophosphamide, 0.390 mg of lactose monohydrate, 0.400 mg of microfine cellulose, 0.200 mg of cornstarch, 0.040 mg of talc and 0.020 mg of highly disperse silica are sieved and homogenized. 0.015 mg of magnesium stearate is then added and mixed. The mass prepared in this way is processed to give tablets:

Weight:         160 mg
Hardness:       >30N
Disintegration: <10 min.

EXAMPLE 3

[0018] Preparation of Film-coated Tablets (50 mg of Cyclophosphamide)

[0019] 11.83 g of polyethylene glycol and 2.37 g of polysorbate 80 are dissolved in 75.21 g of water.

[0020] 1.9 g of carboxymethylcellulose sodium are dissolved in 80.0 g of water. The solutions are brought together. 23.67 g of talc, 23.67 g of titanium dioxide and 0.24 g of simeticone [sic] are then added and the mixture is homogenized. 17.73 g of a 30% strength ethyl acrylate/methyl metharcrylate [sic] copolymer dispersion in water are then added. The tablet cores are then sprayed with the prepared suspension in a suitable apparatus:

[0021] Theoretical weight of a film-coated tablet: 166 mg

EXAMPLE 4

[0022] Investigation of the Stability of Cyclophosphamide Film-coated Tablets

Decomposition of cyclophosphamide after 3 months
	26° C./60% RH	31° C./40%
	Batch 1	0.30	4.12
	Batch 2	0.17	2.36

[0023] Stability of the film-coated tablets of up to 3 years is expected on storage at <25° C.

Claims

1. A film-coated tablet with cyclophosphamide as active compound, comprising in the core cyclophosphamide, one or more fillers, one or more dry binders but no preswollen starch, flow regulators and lubricants.

2. The film-coated tablet as claimed in claim 1, comprising in the core as a filler lactose monohydrate, D-mannitol or CaHPO4, nonpreswollen cornstarch or microfine cellulose as a dry binder, highly disperse silica as a flow regulator and magnesium stearate, stearic acid, glycerol palmitostearate, polyethylene glycol, talc or glycerol monobeherate [sic] as a lubricant.

3. The film-coated tablet as claimed in claim 2, where the cores can comprise the auxiliaries either individually or alternatively in any desired mixture.

4. The film-coated tablet as claimed in claims 1 to 3, comprising, per part of cyclophosphamide in the core, lactose monohydrate, microfine cellulose, nonpreswollen cornstarch, talc, highly disperse silica and magnesium stearate in the following ratio: lactose monohydrate 0.2-1.5, preferably 0.5-1, particularly 0.73 microfine cellulose 0.2-1.5, preferably 0.5-1, particularly 0.74 nonpreswollen cornstarch 0.1-1.5, preferably 0.2-0. 7, particularly 0.37 talc 0.01-1.5, preferably 0.05-0.08, particularly 0.07 highly disperse silica 0.01-0.1, preferably 0.01-0.5, particularly 0.04 magnesium stearate 0.01-0.1, preferably 0.01-0.05, particularly 0.03.