IL136416A - Method for the preparation of a reagent for use in diagnosis of schizophrenia and uses thereof - Google Patents
Method for the preparation of a reagent for use in diagnosis of schizophrenia and uses thereofInfo
- Publication number
- IL136416A IL136416A IL13641698A IL13641698A IL136416A IL 136416 A IL136416 A IL 136416A IL 13641698 A IL13641698 A IL 13641698A IL 13641698 A IL13641698 A IL 13641698A IL 136416 A IL136416 A IL 136416A
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- individual
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- fractions
- schizophrenia
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Description
136416/4
ia tJ yitt ¾/m fi*iia >.)t» na>a wan miri
Method for the preparation of a reagent for use in diagnosis of schizophrenia and uses thereof
Yeda Research and Development tt"i>a mnai ipna man ντ> Company Ltd.
The Inventors:
Meir Shinitzky
/Michael Deckmann
C. 125467
- 1 - 136416/2
FIELD OF THE INVENTION
The present invention relates to diagnostic tests, and more specifically to diagnostic tests for psychiatric diseases.
LEST OF REFERENCES
The folio-wing is a list of references which is considered to be pertinent for the purpose of understanding the background of the invention:
1. Nyland, EL, Naess, A. and Limdre, H.: Lymphocyte subpopulations in peripheral blood from schizophrenic patients. Acta Psvchiat. Scand, 1980; 61; 313-318.
2. Hirata-Hibi- M., Higashi, S., Tachibana, T. and atanabe, N., Stimulated lymphocytes in schizophrenia Arch. Gen. Psvchiat. 1982; 39; 82-87.
3. CoerTey, C.E., Siillrvan, JJL. and Rice, RJL, T lymphocytes in schizophrenia. Biol. Psychiatry 1983 ; 18; 113-119.
4. olyasldna, GX Blood lymphocytes in schizophrenia - immunological andvirological aspects. Adv. Biol. Psvchiat. 1983; 12; 142-149.
. Besslex, H., Eviatar J., Meshulan. M., Tyano. S., Djaldetti, M. and SirotaP. Theophyllin-sensitive T-fymphocyte svbpopulation in schizophrenicpatients. Biol. Psvchiat-. 1987; 22; 1025-1029.
6. Mnllex, N., Ackenheil, M., Eckstein, ., Hofechiistsr, E. and Msmpsl,
W. Reduced suppressor cell function in psychiatric patients. Ann. N. T. Acad Sci. 1987; 396; 686-690.
. M-halovic, LJ. and Jankovic ΒΌ. Effects of intraventricularly injected anti-caudatus antibody on the electrical activity of the cat brain. Nature 1961 ; 192; 665.
. Rapport, MJVL, Karplak, S.E. and Mahadik, SJ?. Biological activities of antibodies injected into the brain. Fed. Proc. 1979; 38; 2391.
. Vartanian, ME. Doyskina, G.S. Lozovsky, D.V., Burbaera, G.S. and Ignaton, SA. Aspects of humoral and cellular immunity in schizophre- nia. In: Birth Defects. Original Article Series D. Bergsma and A.
Goldstein, eds. vol 14: 339-364; Alan R. Liss; New York, N.Y; 1978. 0. Rotman, A Blood platelets in psychopharmacological research Prog. Neuropsvcopharmacol. 1983; 6; 135-151.
1. Pletscher, A Biological Psychiatry, Gea Racagni, ed; Elsevier Science Publisher; 1991; 2, 354-356.
12. Shinitzky, M, Deckmann, M., Kessler, A, Sirota, P., Rabbs, A and Elizur, A, Platelet autoantibodies in dementia and schizophrenia - possible implications for mental disorders. Ann. N.Y. Acad Sci. 1991; 621: 205-217.
13. Kessler, A and Shinitzky, M, Platelets from schizophrenic patients bear autoantiboies that inhibit dopamine uptake. Psvchobiolosv 1993; 21; 229-306.
14. PCT Patent Application WO 95/23970.
. Deckmann et al, Italian Journal of Psychiatry and Behavioural Sciences, 6:29-34, 1996.
The above references will be acknowledged in the text below by indicating their number from the above list shown in brackets.
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BACKGROUND OF THE INVENTION
Schizophrenia is a syndrome which encompasses a variety of symptoms including paranoia, auditory hallucination, delusions, catatonia, bizarre behavior and emotional withdrawal. Schizophrenia affects about 1% of the total population. Its economical and social burden on society is enormous since onset occurs in youth thus requiring patients to be under medical and psychiatric supervision for most of their lives. Schizophrenia is therefore one of the most costly diseases in the mdustrialized world.
Since the biochemical basis of schizophrenia has not yet been elucidated, diagnosis today is still based solely upon psychiatric evaluation. Furthermore, no therapy is currently available for schizophrenia although the symptoms may be ameliorated by neuroleptic drugs.
Many reports have implicated the immune system in the etiology and course of several mental disorders. Serum antibodies which cross-react with brain antigens have been found in the blood of schizophrenic patients*1-65, thus mdicating that schizophrenia is also an autoimmune disease*7-95. Furthermore, platelets have been used as a model for neuronal tissue*10'115 and elevated levels of autoantibodies to platelets have been detected in schizophrenic and demented patients, but not in patients suffering from manic-depressive disorder, depression, personality disorders or schizoaffective disorders*12"145.
A cellular response against autologous platelets was also demonstrated in schizophrenia patients who showed a delayed type hypersensitivity (DTH) reaction when injected with platelets collected from their own blood 5).
It is therefore the object of the present invention to provide a test for the diagnosis of schizophrenia in a subject
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SUMMARY OF THE INVENTION
A novel finding in accordance with the invention is that schizophrenic patients exhibiting a reaction which displays characteristics of a typical delayed-type hypersensitivity reaction when injected with a specific, novel fraction of platelet proteins. This novel fraction is referred to herein as "Pool 2 protein". The Pool 2 proteins, which constitute an aspect of the invention, are characterized by having an isoelectric point (pi) which is 6.5 and preferably within the range of 6.5 to 9.5. When injected with Pool 2 proteins, schizophrenic patients show such a delayed-type hypersensitivity (DTH) reaction.
It is to be noted that although the reaction of the patients to the Pool 2 proteins is referred to above and below as a DTH reaction, there may be cases in which the time profile of the reaction of the patient to the Pool 2 proteins will be different than the time profile of a typical DTH reaction.
The present invention thus provides a protein preparation
(hereinafter "Pool 2 proteins") comprising platelet derived proteins or fractions thereof having an isoelectric point (pi) 6.5 and preferably within the range of 6.5 to 9.5. said preparation capable of eliciting a DTH reaction in a schizophrenic individual upon injection thereof to the individual.
The present invention further provides a diagnostic method for assaying schizophrenia in a subject comprising:
(a) obtaining a preparation comprising, as an active component, platelet derived proteins or fractions thereof having an isoelectric point (pi) 6.5 and preferably within the range of 6.5 to 9.5 ( "Pool 2 proteins ");
(b) injecting said protein preparation into a subject; and
(c) examining the subject for the occurrence of a delayed type hypersensitivity reaction at the site of the injection, a positive result being a
- 5 - 136416/2
reaction above that which , "is observed in non-schizophrenic subjects, indicating that the subject has a high likelihood of being schizophrenic."
In accordance with the invention it was also surprisingly found that the Pool 2 proteins may be either prepared from autologous platelets of the individual to be tested or, alternatively, from a pool of heterologous platelets which were obtained from a number of individuals other than the tested subject It was also surprisingly found that, in most cases, the DTH reaction in a scm^ophrenic patient is substantially higher when the individual is injected with such Pool 2 proteins obtained from a pool of heterologous platelets as compared to a lower DTH reaction in the same tested individual injected with Pool 2 proteins prepared from his own autologous platelets. This finding provides the advantage of preparing a Pool 2 protein preparation which may then either be used immediately or aftematively, be stored at appropriate conditions (e.g. refrigeration) and used for various periods of time to diagnose schizophrenia in a large number of individuals. This obviates the need to repeatedly obtain a blood sample comprising platelets from the tested individual immediately prior to carrying out the diagnostic assay of the invention.
Thus, by a preferred embodiment, the present invention further provides a method for the preparation of a reagent for use in diagnosis of schizophrenia, comprising:
(a) obtaining blood samples from a number of mdividuals, preparing, a pool from said samples and coUecting platelets therefrom
(b) preparing a protein fraction from said platelet preparation comprising proteins or fractions thereof having a pi of 6.5, preferably within the range of 6.5 to 9.5
- 6 - 136416/2
The Pool 2 proteins prepared from heterologous individuals may either be prepared from a number of individuals suffering from schizophrenia or, alternatively, also from a mixture of blood samples obtained from schizophrenic patients as well as healthy individuals.
The present invention further provides the use of the protein preparation which comprises platelet derived proteins or fractions thereof having an isoelectric point (pi) of about 6.5 and preferably within the range of 6.5 to 9.5 for the preparation of an injectable reagent for diagnosis of schizophrenia in an individual by determining a DTH reaction in said individual following injection of said reagent to the individual.
In one case, the platelet derived proteins or fractions thereof are prepared from heterologous platelets obtained from a number of individuals other than the individual to be tested. In another case they are prepared from autologous platelets obtained from the individual to be tested.
Although, as explained above, there is an advantage in preparing a pool of Pool 2 proteins from a number of individuals other than the individual to be tested, in accordance with the diagnostic method of the invention, it is also possible to use a Pool 2 preparation prepared from autologous platelets of the individual to be tested.
- 7 - 136416/2
Typically, the proteins of the invention will be collected by subjecting the collected platelet proteins to isoelectric focusing wherein the proteins having a pi of 6.5, preferably within the range of 6.5 to 9.5 are collected by methods known in the art.
However, in accordance with the invention it has also been found that the Pool 2 protein preparation may also be prepared by methods which do not include isoelectric focusing such as, for example, by extracting the proteins from the platelet sample using for example a detergent, such extraction resulting in Pool 2 proteins having the desired pi values and capable of eliciting a DTH reaction in a schizophrenic patient.
If desired, the Pool 2 protein preparation used for the preparation of the reagent for diagnosis of schizophrenia obtained by any one of the methods mentioned above may be subject to further fractionation steps, e.g. by thin layer chromatography, by high pressure liquid chromatography or by many other purification fractionation methods known, per se. Fractions thus obtained can each then be tested for activity, namely for its ability to cause the DTH reaction in schizophrenic patients. Such purified fractions, as well as individual proteins, polypeptides or peptides among the Pool 2 proteins which are active in eliciting the DTH reaction in schizophrenic patients, are also an aspect of the invention.
136416/2
In accordance with the invention, Pool 2 proteins used in the diagnostic assay of the invention are such which are capable of eliciting DTH activity in an injected individual, the DTH activity being tested by the test known in the art. In short, the Pool 2 proteins are intradermally injected the tested individual at the forearm or thigh and the reaction at the injection site is evaluated after 24, 48 and 72 hours by measuring the reaction diameter around the induration. As mentioned above, there may be cases in which the time profile of the reaction will differ from the typical time profile of a DTH reaction.
The present invention further provides a kit for use in diagnosis of schizophrenia, comprising protein or active protein fractions obtained therefrom, or individual active proteins or peptides having a pi of 6.5. Preferably, such proteins are provided in either injectable form or in a form suitable for preparing an injectable formulation, e.g. a lyophilysate. In one case, the kit comprises proteins or fractions thereof which have a pi within the range of 6.5 to 9.6. These proteins may be prepared from heterologous or autologous platelets. Typically, the kit will be provided with instructions for use or a chart or pictures for guidance of the manner of scoring the results.
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BRIEF DESCRIPTION OF THE FIGURES
Fig. 1 shows the reaction on the forearm of a schizophrenic patient which was injected with the following preparations:
i. Pool 2 proteins (marked as P2)
ii. Pool 1 proteins (marked as PI)
iii. Autologous platelets (marked A)
iv. PBS (marked as C = control).
The invention will now be illustrated in the following examples, which are annexed to the above drawings.
EXAMPLES
A study on the reaction of a subject to an injection of platelets collected from his or her own blood or an injection of Pool 2 proteins was carried out in Israel at The Hospital for Mental Health in Sha'ar Menashe, The Geriatric Hospital in Pardes Hana and at the Weizmaim Institute of Science.
Example 1 Injection of autologous proteins
1. Preparation of platelets
ml venous blood was collected from a subject and centrifuged for 20 mins. at 20°C and 150 g. The supernatant containing platelets was collected and centrifiiged three times for 10 min. at 20°C and 2000 g and the platelets resuspended in phosphate buffered saline (PBS) containing 5 mM EDTA. After the last washing, the platelets were resuspended in sterile PBS at a final concentration of 2x10 platelets ml.
2. Autologous skin test and measurement of delayed type hypersensitivity (DTBD reaction
0.1 ml of the platelet suspension obtained as above from a particular subject was injected intradermaUy back into the fcrssim of tis
same subject A second injection of 0.1 ml PBS spaced about 10 cm from the point of sample injection served as a control.
DTH reaction at the injection sites was measured in accordance with methods known in the art (Skornik, Y., et al, Cancer Immunol Imm nother. 11:93-96, 1981).
Results
The tests were carried out for groups subject:
a) 18 healthy subjects under the age of 65.
b) 10 healthy subjects above the age of 65.
c) 41 schizophrenic pateints.
d) 21 demented patients.
The results of mis test are shown in the following Table 1.
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Table 1
Autologous (Self-Self) Skin Reaction Against Platelets in Bmnans for the Detection of Schizophrenia
Summary of a Multi-Center Study
As can be seen, 38 out of the 41 schizophrenic patients showed a
DTH reaction, while only one healthy individual under the age of
65 out of the 18 which were tested, reacted positively. Positive
reactions were not observed in 10 healthy individuals over the age
of 65, as well as in 21 demented patients. Sensitivity of this test is
thus 92% and the specificity is 98%.
As seen in the Table, while almost all of the tested schizophrenic patients showed a DTH reaction to the Pool 2 proteins prepared from their autologous platelets, only one healthy individual had a positive DTH reaction. Thus, the diagnostic assay of the invention showed a very high sensitivity and specificity for the diagnosis of schizophrenia in a tested individuaL
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Example 2 Preparation of Pool 1 and Pool 2 proteins
Methods
Platelet suspension containing about 20 gr total protein was obtained as in Example 1, and the platelets solubilized with 40 ml of a solution containing 0.5% of the detergents NP-40 and Triton-X-100 for 5 miiis. at room temperature with gentle shaking. The solution was then centrifuged at 4000 g for 15 mins. at 20°C. The supernatant was collected, and the pellet was subjected to two further extractions with 10 ml 0.1% Triton-X-100. The three supernatants were combined and Bio-Lyte Ampholyte™ 3/10 (40%) of BioRad was added to a final concentration of 1 %. The solubilized proteins were subjected to isoelectric focusing. 60 ml of sample was applied to the Rotofor™ system of BioRad, using 0.1 M phosphoric acid as anode solution, and 0.1 M aOH as cathode solution. The isoelectric focusing was performed for about 4 hours at 10°C using 10 Watt constant power until the current remained constant for 30 mins. Proteins were divided into two separate groups in accordance with their pi: proteins having a pi in the range of 2-6.5 are referred to as Pool 1 proteins while proteins having a pi in the range of 6.5-10 are referred to as Pool 2 proteins. Pool 1 and Pool 2 proteins were harvested separately and diluted 1:50 with PBS.
Example 3 Injection of Pool 1 and Pool 2 proteins
Method
The following four preparations were injected intradermally into the forearm of a schizophrenic patient:
L Pool 2 proteins (marked as P2)
ii. Pool 1 proteins (marked as PI)
iii. Autologous platelets (marked A)
iv. PBS.
0.1 ml of each above preparation were injected and the prspsrs-
tions were injected at four different injection sites spaced about 10 cm from each other. The skin reaction at each injection site was monitored 24 h, 48 h and 72 h after injection.
Results
The results are seen in Fig. 1 where (i) is the highest injection site on the arm and (iv) is the lowest
As seen in the figure, a DTH response measured as explaiend above, was observed in the two schizophrenic patients at the site of injection of Pool 2 proteins and no DTH reaction was seen at the site of PI injection. Furthermore, the DTH reaction at the P2 site of injection was substantially enhanced as compared to the DTH reaction seen at the site of mjection of the autologous platelets. Thus, it is, in most cases, preferred to use a P2 protein preparation obtained from a pool of blood samples obtained from several heteriogous individuals in the diagnostic assay of the invention.
Claims (11)
1. Use of a protein preparation comprising platelet derived proteins or fractions thereof having an isoelectric point (pi) 6.5 and preferably within the range of 6.5 to 9.5, for the preparation of an injectable reagent, substantially as described in the specification, for diagnosis of schizophrenia in an individual by determining a Delayed Type Hypersensitivity (DTH) reaction in said individual following injection of said reagent to the individual.
2. Use in accordance with Claim 1, wherein said platelet derived proteins or fractions thereof are prepared from heterologous platelets obtained from a number of individuals other than the individual to be tested.
3. Use in accordance with Claim 1, wherein said platelet derived proteins or fractions thereof are prepared from autologous platelets obtained from the individual to be tested.
4. The use in accordance with Claims 2 or 3, wherein the proteins or fractions thereof have a pi within the range of 6.5 to 9.5.
5. A kit for use in diagnosis of schizophrenia in an individual by detection of DTH reaction in said individual, comprising: (i) a protein or a fraction thereof prepared from human platelets, said proteins or fractions thereof having a pi of 6.5; (ii) a chart and/or pictures for guidance of the manner of scoring said DTH reaction; and (iii) instructions for use.
6. A kit in accordance with Claim 4, wherein the proteins or fractions thereof are prepared from heterologous platelets obtained from a number of individuals other than the individual to be tested.
7. A kit in accordance with Claim 4, wherein the proteins or fractions thereof are prepared from autologous platelets obtained from the individual to be tested.
8. A method for the preparation of a reagent for use in diagnosis of - 15 - 136416/4 schizophrenia in an individual by detecting a DTH reaction in said individual following injection of said reagent to the individual, comprising: (a) obtaining blood samples from a number of individuals, preparing a pool from said samples and collecting platelets therefrom; (b) preparing a protein fraction from said platelet preparation comprising proteins or fractions thereof having a pi of 6.5.
9. A protein preparation comprising platelet derived proteins or fractions thereof having a pi of 6.5 and preferably within the range of 6.5 to 9.5 for use as an injectable reagent for diagnosis of schizophrenia in an individual by determining a DTH reaction in said individual following injection of said reagent to the individual, substantially as described in the specification.
10. The method in accordance with Claim 8, wherein said platelet derived proteins or fractions thereof are prepared from heterologous platelets obtained from a number of individuals other than the individual to be tested.
11. The method in accordance with Claim 8, wherein said platelet derived proteins or fractions thereof are prepared from autologous platelets obtained from the individual to be tested. For the Applicants, REINHOLD COHN AND PARTNERS By:
Priority Applications (1)
Application Number | Priority Date | Filing Date | Title |
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IL13641698A IL136416A (en) | 1997-12-07 | 1998-12-07 | Method for the preparation of a reagent for use in diagnosis of schizophrenia and uses thereof |
Applications Claiming Priority (3)
Application Number | Priority Date | Filing Date | Title |
---|---|---|---|
IL12249097A IL122490A0 (en) | 1997-12-07 | 1997-12-07 | Assay for schizophrenia based on skin reaction |
IL13641698A IL136416A (en) | 1997-12-07 | 1998-12-07 | Method for the preparation of a reagent for use in diagnosis of schizophrenia and uses thereof |
PCT/IL1998/000592 WO1999030163A1 (en) | 1997-12-07 | 1998-12-07 | Skin test for schizophrenia |
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IL136416A0 IL136416A0 (en) | 2001-06-14 |
IL136416A true IL136416A (en) | 2004-12-15 |
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IL13641698A IL136416A (en) | 1997-12-07 | 1998-12-07 | Method for the preparation of a reagent for use in diagnosis of schizophrenia and uses thereof |
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