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HK1091146B - New use, pharmaceutical preparations as well as a process for their production - Google Patents

New use, pharmaceutical preparations as well as a process for their production Download PDF

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Publication number
HK1091146B
HK1091146B HK06113073.7A HK06113073A HK1091146B HK 1091146 B HK1091146 B HK 1091146B HK 06113073 A HK06113073 A HK 06113073A HK 1091146 B HK1091146 B HK 1091146B
Authority
HK
Hong Kong
Prior art keywords
ifosfamide
mesna
solution
vol
solubility
Prior art date
Application number
HK06113073.7A
Other languages
German (de)
French (fr)
Chinese (zh)
Other versions
HK1091146A1 (en
Inventor
Berthold Roessler
Original Assignee
Baxter International Inc.
Baxter Healthcare S.A.
Priority date (The priority date is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the date listed.)
Filing date
Publication date
Application filed by Baxter International Inc., Baxter Healthcare S.A. filed Critical Baxter International Inc.
Priority claimed from PCT/US2004/031650 external-priority patent/WO2005032515A1/en
Publication of HK1091146A1 publication Critical patent/HK1091146A1/en
Publication of HK1091146B publication Critical patent/HK1091146B/en

Links

Description

Field of the Invention
The invention concerns the use of mercaptoethane sulfonate-sodium (Mesna) to increase the solubility of Ifosfamide in storage-stable, supersaturated aqueous pharmaceutical preparations for parenteral administration.
State of the Art
Ifosfamide (2-(chlorethylamino)-3-(2-chlorethyl)-tetrahydro-2H-1,3,2-oxazaphosphorin-2-oxide) is an alkylating cytostatic agent that is administered against a variety of tumor-diseases, at times in combination with other cytostatic agents. Mesna (mercaptoethane sulfonate-sodium) is co-administered with Ifosfamide in order to reduce the side-effects of Ifosfamide (c.f. US Patent Nos. 4,770,870 and 4,220,660 ; German Patent Application DE 2806866 ).
The solubility of Ifosfamide in water is limited and at room temperature is a maximum of about 140 mg/mL (saturation concentration). The addition of auxiliary agents can sometimes lower the solubility of Ifosfamide, e.g. to under 10% (wt/vol), so that even at low concentrations, the use of a solubility-enhancing agent is necessary in order to obtain a clear, injectable solution.
A concentrated and/or high-concentrated Ifosfamide solution has critical advantages in handling in comparison to a diluted solution. The dosage of Ifosfamide depends upon the body surface or weight of the patient and lies in general between 3 g and 5 g, but can in individual cases also be over 10 g. For exacting preparation of patient-specific dosage, volumes are advantageous that are easily handled and that can be added to standard infusion solutions. For a concentrated Ifosfamide solution of e.g. 20% (wt/vol) active ingredient, 15 ml to 25 ml will have to be dosed, which allows for a sufficiently highly precise dosage as well as easy handling of single injection. In contrast to this, a currently marketed Ifosfamide solution of 4% (wt/vol) content must be dosed at 75 ml to 125 ml, and in individual cases, as much as 250 ml.
On the basis of the aforementioned limitations of solubility, solutions of Ifosfamide at concentrations > 10% (wt/vol) for parenteral use that are devoid of particles and crystals are possible only with the addition of a solubility-enhancing agent. Based on the presentation form as injectable solution, these solubility-enhancing agents must be free from any physiological concerns. In the state of the art, a urea is suggested as solubility enhancing agent (c.f. WO 99/18973 ). Urea is, however, suspected to increase the neural side-effects of Ifosfamide.
As solubility-enhancing agents, theoretically Tensides such as, e.g., Tween 80 or Poloxamer can be considered. The ability to use them, however, is limited or in some cases forbidden on account of their haemological characteristics.
US-A-4,959,215 describes Ifosfamide-Mesna compositions, in particular respective lyophilizates consisting of Ifosfamide, 0.05-1.0 parts by weight of Mesna and 0.1 to 17 parts by weight of hexitol, based on one part by weight of Ifosfamide as well as optionally other conventional pharmaceutical auxiliary substances.
Summary of the Invention
Surprisingly, it has been found that through the use of mercaptoethane sulfonate-sodium (Mesna) a supersaturated aqueous solution of Ifosfamide can be successfully prepared, whose concentration is substantially above the saturation concentration of Ifosfamide in water. The saturation concentration of about 140 mg/ml at room temperature as well as the saturation concentration of about 190 mg/ml at about 5 °C can be surpassed by a wide margin by the use of Mesna. By the use of Mesna as solubility-enhancing agent, a storage-stable concentrate of Ifosfamide can be successfully produced in respect of its physical characteristics in a concentration region from about 10% (wt/vol) to 50% (wt/vol).
The use of Mesna as solubility-enhancing agent in the production of supersaturated Ifosfamide solutions is neither described in nor suggested by the state of the art.
The use of Mesna according to the invention enables the production of aqueous concentrates of the active agent Ifosfamide in concentrations above the saturation concentration of Ifosfamide in water, i.e. greater than 10% (wt/vol), using Mesna as a solubility-enhancing agent for Ifosfamide. Preferably, preparations with Ifosfamide concentrations greater than 10% (wt/vol) up to 50% (wt/vol) are formed. At the same time, solution temperatures are selected between 0 °C and 30 °C, preferably 2 °C and 20 °C, especially preferred 5 °C and 15 °C.
The production of concentrates is brought about by dissolving the required amount of Mesna, e.g. 5 g to 50 g per 100 ml, preferably 10 g to 20 g per 100 ml and optionally a suitable buffer (phosphate, borate, carbonate buffer, preferably phosphate buffer) in Water for Injection (WFI), subsequently the corresponding quantity of Ifosfamide is added to a room temperature or preferably cooled solution of Mesna, whereby the ratio of Ifosfamid to Mesna is from 1 : 0.25 to 1 : 4, preferably 1 : 0.5 to 1 : 2, more preferably 1 : 0.8 to 1 : 1.2, most preferably 1 : 1.0 to 1 : 1.2. The ratios refer to the proportions by weight of the substances in the solution. The solutions are homogenized, sterilized by filtration and filled under aseptic conditions. Production is carried out under nitrogen. These solutions can also be lyophilized in order to obtain a longer storage life of the pharmaceutical preparation. In addition to the auxiliary agents that are set forth in the examples, the solution can contain also further substances, e.g. sodium chloride, Mannitol, lactose, polyethylenglycol, ethanol, glucose, disaccharide, cyclodextrine.
The term "cooled" solution temperatures means from about 0 °C to about below room temperature (below about 21 °C), preferably from about 2 °C to lower than or equal to about 20 °C, more preferably from about 5 °C to about 15 °C, still more preferably from about 5 °C to about 10 °C.
The invention will be more specifically demonstrated by the following examples, but should not be restricted to them.
Example 1 Ifosfamide concentrate 20% (wt/vol) with 20% (wt/vol) Mesna content Composition of the solution:
Ifosfamide 2000.0 mg
Mesna 2000.0 mg
Phosphate buffer 1000.0 mg
Water (WFI) 6540.0 mg
In the manufacture, 90% of the Water for Injection is cooled to about 5 °C to 10°C, to which is dissolved the phosphate buffer; the Mesna is subsequently added and is homogeneously dissolved. Finally, the Ifosfamide in the solution is dissolved and the pH is set at 7.4 with ortho-phosphoric acid. The solution so obtained is brought to the specified weight with the cooled Water for Injection, sterile-filtered and filled in injection vials under aseptic conditions. Sterilization and filling are not carried out under cooling.
Example 2
Ifosfamide concentrate 20% (wt/vol) with 5% (wt/vol) Mesna
Composition of the solution:
Ifosfamide 2000.0 mg
Mesna 500.0 mg
Phosphate buffer 1000.0 mg
Water (WFI) 8040.0 mg
The solution is produced identically according to the procedure of Example 1.
Example 3
Ifosfamide concentrate 20% (wt/vol) with 5% (wt/vol) Mesna, lyophilisate and reconstituion of the lyophilisate: Composition of the solution before filling and after reconstitution:
Ifosfamide 2000.0 mg
Mesna 500.0 mg
Mannitol 500.0 mg
Water (WFI) 8040.0 mg
In the manufacture, added to about 90% of the Water for Injection that is pre-cooled to about 5 °C to 10°C is, sequentially, the Mesna, the Ifosfamide and the Mannitol, whereby each is homogenized until a clear solution is obtained. Subsequently, the solution is sterile filtered and filled under aseptic conditions in injection vials to the specified weight for lyophilisation. Lyophilization ensues with a suitable freeze-dry device and lyophilization process, e.g.
Freezing 1 hour at -45 °C
3.5 hours maintained at -45 °C
Main drying 0.4 mbar, in 1.5 hours from - 45 °C to -15 °C
0.4 mbar, 120 hours at -15 °C
Post drying 0.4 mbar, increasing over 4 hours to 20 °C Max. vacuum, 6 hours at 20 °C
The injection vials are sealed shut under nitrogen.
Composition of the lyophilisate:
Ifosfamide .2000.0 mg
Mesna 500.0 mg
Mannitol 500.0 mg
Reconstitution of the lyophilisate:
For reconstitution, the lyophilisate is mixed with 8 ml Water for Injection or with a suitable infusion solution, e.g. isotonic salt solution, glucose solution for infusion, Ringer lactate soltution, etc. so that an approximately 20% (wt/vol) solution of Ifosfamide is formed. This concentrate can then be used by individual dosage as an additive for an infusion preparation. The production of a lyophilisate and its reconstitution can then ensue with the addition of an auxiliary agent, such as Mannitol, glucose, disaccharide or a similar lyophilisate filler known in the art.
Example 4:
12% (wt/vol) Ifosfamide concentrate with 5% (wt/vol) Mesna
Ifosfamide: 3 g
Mesna: 1.25 g
Water: 24.5 g
Example 5:
25% (wt/vol) Ifosfamide concentrate with 10% (wt/vol) Mesna
Ifosfamide: 6.25 g
Mesna: 2.5 g
Water: 23.75 g
Example 6:
50% (wt/vol) Ifosfamide concentrate with 20% (wt/vol) Mesna
Ifosfamide: 12.5 g
Mesna: 5.0 g
Water: 17.5 g
The making of Examples 4,5 and 6 is carried out analogously to the description of Example 1. The solubility-enhancing properties of Mesna in respect of Ifosfamide are demonstrated over a wide range of concentrations and proportions. The addition of a buffer, e.g. phosphate buffer, largely does not influence the solubility-enhancement, the buffering addition being however necessary for the chemical stabilization of the preparation in order to minimize decomposition of the active agent and in order to obtain sufficient storability of the solution. Apart from that, the Mesna provides as solubility-enhancing agent a physical stabilization that prevents crystallization.

Claims (3)

  1. Use of Mesna as solubility-enhancing agent of Ifosfamide in the production of an aqueous pharmaceutical preparation for parenteral administration with a content of Ifosfamide above the saturation concentration of Ifosfamide in water, and optionally containing one or more pharmaceutically acceptable auxiliary agents, wherein the weight ratio of Ifosfamide to Mesna is in the range of 1:0.25 to 1:4, and with the proviso that the preparation does not contain an etherified β-cyclodextrin.
  2. The use according to claim 1, wherein the auxiliary agent is selected from the group consisting of one or more buffers, sodium chloride and Mannitol.
  3. The use according to claim 1, wherein the pH is set at pH 6-8 by way of a suitable buffer.
HK06113073.7A 2003-10-01 2004-09-28 New use, pharmaceutical preparations as well as a process for their production HK1091146B (en)

Applications Claiming Priority (3)

Application Number Priority Date Filing Date Title
US50775003P 2003-10-01 2003-10-01
US60/507,750 2003-10-01
PCT/US2004/031650 WO2005032515A1 (en) 2003-10-01 2004-09-28 New use, pharmaceutical preparations as well as a process for their production

Publications (2)

Publication Number Publication Date
HK1091146A1 HK1091146A1 (en) 2007-01-12
HK1091146B true HK1091146B (en) 2011-10-07

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