NL1008582C2 - Bone material. - Google Patents

Description

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BONE MATERIAL

The invention relates to bone material for promoting bone tissue growth, provided with TGF-S which can be released into the environment over a period of time.

In the Western world, bone loss is an increasing public health problem, with millions expected to suffer from osteoporosis in the near future. For this reason alone, there is a great interest in substances to combat bone loss and to stimulate healthy new bone tissue. Not only the aforementioned condition osteoporosis is envisaged, but also missing or insufficiently present bone tissue in a bone defect, between an implant and a surrounding bone wall, etc. Bone material is now known, formed by mixing dry calcium phosphate powder with a liquid consisting of water and various additives, and applying the resulting mixture in the form of a paste on site, after which curing of the pasty bone material into bone cement takes place. . The aim is to create a temporary, absorbable bone replacement that is replaced by living bone tissue over time. This replacement is possible because cured calcium phosphate cement is soluble in surrounding, constantly refreshing body fluids, so that pores in which degraded bone cement are formed, in which living bone tissue can form. This has been described in "Journal of Materials Science: Materials in Medicine 6 (1995) 340-347, K. Kurachina et al., Journal of Materials Science: 35 Materials in Medicine 5 (1994) 164-17, FCM Driessens et al ".

Bone material to promote bone tissue growth, provided with TGF-β that can be released to the environment over a period of time, is known, in particular, from U.S. Pat. 5,422,340 (Ammann et al.). The paste material known therefrom in the form of a paste is formed by mixing tri-calcium phosphate granules with the human transforming growth factor TGF-β, whereby this factor is adsorbed on the surface of the tri-calcium phosphate granules. The granules with the TGF-β 10 factor adsorbed on their surface are then mixed with a polymer to increase the consistency of the whole, and a paste is formed for application to sites in a bone where bone growth is desired. The TGF-β factor is released to the environment over a period of time, stimulating bone growth on site.

It is noted that within the framework of the invention the term "TGF-β" has the same definition as indicated in the above-mentioned US patent.

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A drawback of the pasty bone material known from the aforementioned US patent publication is that the time period in which the TGF-β is released to the environment to stimulate bone tissue growth appears in practice to be too short to obtain an adequate amount of grown natural bone tissue. In practice, there is a long-felt need to,!? extend that period of time so that TGF-β is released by the bone material in a desired manner, especially gradually decreasing over time. Moreover, the drawback is that this known bone material, due to its pastyness, cannot take over the mechanical function of bone tissue and therefore cannot serve as a temporary replacement of bone tissue. Due to this pastyness, no adhesion of the pasty bone material to existing bone tissue takes place either. This in turn has the disadvantage that no living bone tissue can form in particular pores of degradable bone material.

The object of the invention is to provide a bone material of the type mentioned in the opening paragraph, which obviates the drawbacks of the prior art, and for this purpose such bone material according to the invention has the special feature that the bone material after curing forms bone cement and that the TGF-β is homogeneously distributed in the cured bone cement. In particular, the TGF-β is dissolved in a liquid medium, preferably water, mixed with the bone material before curing.

Preferably, a blood protein-containing solution, especially albumin, is used to keep the TGF-β in solution to ensure a homogeneous distribution of the TGF-β in the final cured bone cement.

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The bone cement according to the invention promotes bone tissue growth, which is an absorbable material which, due to its hardness, can partially take over the mechanical function of bone, as well as through its bone growth-promoting properties promotes replacement with living bone tissue. Extensive experiments have shown that the addition of the TGF-β in no way hinders its gradual release after curing of the bone cement.

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In a preferred embodiment of bone material according to the invention, the bone material contains calcium phosphate. Because of the biocompatibility, this particularly concerns a mixture of dicalcium phosphate, tri-calcium phosphate, tetra-calcium phosphate and / or hydroxyl apathite.

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In a further preferred embodiment of the present bone material, it is formed into a granulate (granules), which leads to an optimal formation of living bone tissue in spaces between the granules, before the granules themselves are replaced by living bone tissue.

The invention also refers to a method of manufacturing a bone material according to the invention, wherein the bone material is cured into bone cement and the TGF-β is distributed homogeneously in the cured bone cement. As said, it will be. TGF-β dissolved in a liquid medium, preferably water, 1 and mixed with the bone material before curing thereof. It is thus effected to provide a longer release period in which the TGF-β can be delivered to the environment after application of the bone material. The basic principle here is that 1 TGF-β always only works where it is needed.

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The invention is also related to a device for administering bone material provided with TGF-β I according to the invention, wherein at least two compartments are provided for keeping the bone material and TGF-β separate, in a mixing chamber for mixing the bone material and the TGF-β, as well as in a nozzle for spraying the mixture from the mixing chamber.

The invention will be further elucidated on the basis of a discussion of a number of tests according to a preferred variant of the invention, in which a procedure for manufacturing the present bone material with added TGF-β will first be discussed. 1. A sterile cement powder consists of a mixture of alpha tricalcium phosphate, tetracalcium phosphate monoxide and di-calcium phosphate dibasic, in a ratio of 75: 20: 5, or else if desired.

2. A sterile TGF-S solution (solution (A)) 5 consists of 4 milimolar HCl in water with 0.1% bovine serum albumin and TGF-S dissolved in a concentration ranging from 2 x 10% to 2% as desired.

3. A second sterile solution (solution (B)) consists of water with 12% sodium succinate and 5% chondroitin succinate dissolved therein.

4. Solution (A) is mixed 1 to 1 with solution 15 (B), under sterile conditions.

5. A volume part solution (A + B) is mixed with two volume parts cement powder under sterile conditions. This can happen; 20 a. In a container and mixed with a spatula, after which the cement paste is immediately applied in the patient's body on the spot and hardens there; 25 b. via a two-chamber syringe, one of which contains the cement powder and the other solution (A + B); using the syringe, powder and liquid are brought together in the body on the spot, after which the mixture hardens on the spot (claim 8).

c. in a container, mold or container, after which the mixture hardens outside the body and may or may not be ground into a powder of the desired grain size, after which it is applied into the patient's body

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6 * (claim 7).

The first test 5 Osteoblast-like cells and precursors of osteoblast-like cells were isolated from adult rat bone tissue. Then, 5x10 4 cells in 1 ml cell culture fluid with antibiotics and 10% fetal bovine serum were applied to 60 mg cement, to which may or may not have added TGF-β. The culture medium was changed after 3 to 4 days. After the tenth day, the cells were collected and the amounts of protein and alkaline phosphatase (ALP) activity determined in the cells. A significant increase in ALP activity was found in cement-containing osteoblast precursor-like cells containing 10'4% TGF-β.

The second run. The cement was formulated as described above. The release of the TGF-β in the culture medium was determined by measuring the concentration of the TGF-β in culture medium without cells. Within 24 hours, 20% of the TGF-β was found in the medium.

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The third experiment j. In the skull of adult rats, bone defects of 5 mm diameter were made up to the dura mater. The 30 defects were filled with cement (see above), with or without TGF-β added (see above). Addition of TGF-β to the cement accelerated the ingrowth of bone tissue into the cement, as histological studies have shown.

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The fourth test 10 0 6 58? 7

A so-called "critical size defect", i.e. a segment of bone that was too large to heal by spontaneous callus formation, was introduced into the left ulna of adult rabbits. The defect was filled with cement, to which TGF-β may or may not have been added. Addition of TGF-β to the cement caused accelerated replacement of the cement by living bone tissue and bridging the defect, as histological studies have shown.

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The fifth test

In the upper jaw of goats, the first two promolars were extracted both left and right. The extraction vials were filled with cement (see above) to which TGF-β was or had not been added. Addition of TGF-β to the cement accelerated the replacement of the cement with living bone tissue, as histological studies have shown.

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The sixth trial

Tooth root implants were placed in the edentulous jaw section in patients eligible for treatment with dental implants. Then the dehiscences and fenestrations were filled with calcium phosphate cement, to which TGF-β had been added. A small biopsy was taken from the permucosal portion of the implant and examined histologically. The cement had been replaced by vital bone tissue, as histological studies show.

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Claims (5)

Bone material to promote bone tissue growth, provided with TGF-β which can be released into the environment for a period of time, characterized in that the bone material forms a bone cement after curing and that the TGF-β is homogeneous in the 1 cured bone cement divided. i Bone material according to claim 1, wherein the TGF-β dissolved in a liquid medium, preferably water, is mixed with the bone material before curing thereof. Bone material according to claim 1 or 2, wherein the bone material contains calcium phosphate. Bone material according to claim 3, wherein the bone material contains a mixture of dicalcium phosphate, tri-calcium phosphate, tetra-calcium phosphate and / or hydroxyl apathite. A method of manufacturing bone material * according to any one of claims 1 to 4, wherein the bone material is cured into bone cement and the TGF-β is distributed homogeneously in the cured bone cement. 6. A method according to claim 5, wherein the TGF-β is dissolved in a liquid medium, preferably water, and mixed with the bone material before curing thereof. 7. A method according to claim 5 or 6, wherein the cured bone cement is granulated. - 1000582 The bone material delivery device according to any one of claims 1 to 4, wherein at least two compartments are provided for keeping the bone material and the TGF-β separate, in a mixing chamber for mixing the bone material and the TGF-β, as well as in a nozzle for spraying the mixture from the mixing chamber for administration of the bone material provided with the TGF-β before curing thereof. 10 5 G 0 r. ?. G 2 COOPERATION TREATY (PCT) REPORT ON NEWNESS RESEARCH OF INTERNATIONAL TYPE IDENTIFICATION OF THE NATIONAL APPLICATION Identifier of the applicant or of the fellowship j 126.77.4186 Neo-netherlands application no. Verzoex for an investigation of mtemasonaai type By oe Insanae for tntemaaonaai OncerzoeK (ISA) on net! insure for an impasto of intamaDoraai type te ge Core no. SN 31124 EN I. CLASSIFICATION OF THE SUBJECT (Pipe of various dassilicaoes. state all the dassificaoe symbols) According to the inoemaoonaie dassjftcaoe (IPC) Int.Cl.6; A 61 L 25/00, A 61 L 27/00, A 61 K 38/18 II. FIELD OF TECHNIQUE EXAMINED Minimum documentation _ Classification system _ Classification scr. __ * _ j i Int.Cl.6: A 61 L, A 61 K j! I i i __I_ Untrue anoere oocumenaae on the minimum battery menace enter as far as the right documents. j! j! i i ___________1 i; ~ '1; jlll._; NO RESEARCH SIMILAR FOR CERTAIN CONCLUSIONS (csnerxmgen eoupplementoad) 1IV, LACK OF INVENTION iccmerx.ncen cc supplement sheet] '"orm PC7, lSA,' 23lfa> C =! SS ^