Patent Publication Number: US-2004052922-A1

Title: Nutritional and therapeutical preparations having antioxidant activity

Description:
[0001] The present invention relates to pharmaceutical and dietary compositions, as well as to functional foodstuffs useful as coadjuvants for both preventing and treating aging processes and related conditions: atherosclerosis, hypertension, diabetes, tumors, obesity and overweight, hypertriglyceridemia, hypercholesterolemia, aging of the skin, alopecia, panniculitis (cellulite), osteoporosis, cerebral aging (Alzheimer, Parkinson, senile dementia, etc.) and loss of memory, stress, depression, menopausal syndromes, benign prostate hypertrophy, and the like.  
       [0002] Said compositions comprise:  
       [0003] a) a lipidic mixture rich in polyunsaturated fatty acids, preferably docosahexaenoic acid (DHA), eicosapentaenoic acid (EPA), conjugated linoleic acids (CLA) and γ-linolenic acid, and antioxidant vitamins, in combination with at least two of the following components:  
       [0004] b) one or more terpenes, selected from monoterpenes and/or sesquiterpenes, triterpenes, lactonic terpenes, but preferably monoterpenes or sesquiterpenes,  
       [0005] c) 1-piperoylpiperidine (in pure form and/or purified extracts or fractions containing it enriched in black pepper) and/or capsaicin and analogues thereof, preferably 1-piperoylpiperidine,  
       [0006] d) one or more polycosanols and/or polycosanolic acids.  
       [0007] The lipidic mixture can contain the polyunsaturated fatty acids in the form of tri-, di- and monoglycerids, phospholipid esters, free acids or alkali or alkaline-earth metal salts, salts with amino acids (arginine, lysine, methionine, cysteine, and the like) or salts with nitrogen bases such as ethanolamine, mono- and dimethylethanolamine, choline, and the like, or as ethyl esters. Preferred sources of these unsaturated acids are oils from sea animals (from cod, mackerel, tuna, seal, etc.) and/or oils from different types of seeds (maize, soy-bean, sunflower, colza, wheat germ, borage, “evening primrose”, red currant, linseed, perilla, etc.), olive, seaweed, pepper, mushrooms (for example  Mucor javanicus ) oils, lecithins and phospholipids of different nature, etc. with various purity degrees.  
       [0008] The antioxidant vitamins of the lipidic mixture can be selected from one or more of the following compounds:  
       [0009] vitamin E, lipoic acid, vitamin C as such and/or as acyl derivative, vitamin B6 as such and/or as acyl derivative, folic acids, vitamin B12, etc.; water-soluble vitamins (vitamin B6, folic acids, vitamin B12, etc.) are preferably added in the form of complexes with lecithins which promote their dispersion in the lipidic mixture.  
       [0010] Examples of monoterpenes include d-limonene, β-caryophyllene, sabinene, borneol, carveol, carvone, eugenol, eugenol acetate, geraniol, menthol, myrtanol, pinene, β-pinene, thymol, and the like.  
       [0011] Examples of sesquiterpenes include abscisic acid, β-ionone, rodinal, and the like.  
       [0012] Examples of lactonic terpenes include ginkgolides, bilobalides, and the like.  
       [0013] Examples of triterpenes include madecassic acid, asiatic acid, asiaticoside, etc.  
       [0014] Preferred sources of these terpenes are suitably purified fractions of:  
       [0015] A) fruit or vegetable or spices essential oils rich in limonene, thymol, menthol, etc.. and  
       [0016] B) medicinal herbs essential oils (such as  Ginkgo biloba, Centella asiatica , etc.) rich in lactonic terpenes and triterpenes.  
       [0017] 1-Piperoylpiperidine, of formula:  
                 
 
       [0018] can be present as pure compound or it can be contained in black pepper (piper nigrum) extracts.  
       [0019] Examples of vegetable extracts containing 1-piperoylpiperidine are extracts in apolar solvents of black pepper fruits which, after evaporation of the solvent, may either be used crude or be further purified by column chromatography or other conventional techniques to obtain highly pure fractions of 1-piperoylpiperidine (above 95%),  
       [0020] Capsaicin and its analogues can be present as pure compounds or contained in extracts of red pepper (capsicum annuum L.), chili, paprika, etc.  
       [0021] Examples of polycosanols (long chain aliphatic alcohols: C≧24) include octacosanol, triacosanol, tetracosanol and hexacosanol. Preferred sources of these polycosanols are suitably purified wax fractions of maize, wheat, rice, citrus fruits, sugar cane, and the like.  
       [0022] Examples of polycosanolic acids (saturated long chain fatty acids: C≧24  
                 
 
       [0023] are octacosanolic acid (montanic acid), triacosanolic, tetracosanolic, hexacosanolic acids, and the like. Preferred sources of these polycosanolic acids are suitably purified wax fractions of maize, wheat, rice, citrus fruits, sugar cane, sea animals fats, and the like. Alternatively, these fatty polycosanolic acids can easily be obtained by chemical oxidation of the alcohol group of the corresponding polycosanols according to conventional oxidation procedures.  
       [0024] The preparation of octacosanolic acid from the corresponding octacosanol (or a mixture of polycosanols containing it) is reported in the following by way of example.  
       [0025] Octacosanol was dissolved in 200 ml of acetic acid, treated with 75 g of chromic acid in acetic acid, and left for 2 hr at 0° C. and 1 hr at room temperature. Dilute hydrochloric acid and benzene were added to the mixture and the extract was evaporated under reduced pressure. The residual oil was partitioned between benzene and a solution of 5% sodium hydroxide in water-methanol 2:1. From the benzene layer, 30 g of neutral material was recovered. An oil that separated from the aqueous layer was acidified with hydrochloric acid and treated with benzene, which was evaporated to give 40 g of octacosanolic acid. The methyl ester of the latter was pure by GLC analysis. The product was distilled at 170° C./0.01 mm. This method is a partial modification of the procedure by Steinberg for the preparation phytanic acid from the corresponding phytol (Daniel Steinberg et al., (1966), J. Lipid Res., vol. 7, pp 684-690; Effects of dietary phytol and phytanic acid in animals).  
       [0026] Polyunsaturated fatty acids [that are preferably rumenic acid and conjugated linoleic acids (CLA): the positional isomers of CLA include Δ-7, Δ-9; Δ-8, Δ-10; Δ-9, Δ-11; Δ-10, Δ-12; Δ-11, Δ-13, and Δ-12, Δ-14 conjugated octadecadienoic acids. Each of the aforementioned positional conjugated diene isomers can occur in the following geometric configurations: cis-, trans-; trans-, cis-; cis-, cis- and trans-, trans-. Rumenic acid is the proposed common name of the predominant CLA isomer: cis-9, trans-11); γ-linolenic acid; eicosapentaenoic acid and docosahexaenoic acid] are present in the compositions of the invention in amounts ranging from 0.01 to 500 mg, preferably from 5 to 50 mg per kg body weight of the treated subject.  
       [0027] Vitamins are present in the compositions of the invention in amounts corresponding to their daily dosage ranges used in humans. Particularly preferred ranges are the following:  
       [0028] 1) vitamin E: 0.01 to 20 mg, preferably 0.2 to 0.8 mg per kg body weight;  
       [0029] 2) lipoic acid: 0.01 to 10 mg, preferably 0.2 to 0.8 mg per kg body weight;  
       [0030] 3) vitamin C: 0.1 to 50 mg, preferably 0.5 to 3.0 mg per kg body weight;  
       [0031] 4) vitamin B6: 1 to 300 μg, preferably 5 to 50 μg per kg body weight;  
       [0032] 5) folates: 0.1 to 30 μg, preferably 2 to 6 μg per kg body weight; and  
       [0033] 6) vitamin B12: 0.001 to 0.3 μg, preferably 0.02 to 0.06 μg per kg body weight.  
       [0034] Terpenes are present in amounts ranging from 0.01 to 100 mg, preferably from 0.5 and 10 mg per kg body weight.  
       [0035] 1-Piperoylpiperidine is present in amounts ranging from 0.001 to 5 mg, preferably from 0.02 and 0.2 mg per kg body weight.  
       [0036] Capsaicin is present in amounts ranging from 0.01 to 100 mg, preferably from 0.1 and 7.5 m g per kg body weight.  
       [0037] Polycosanols and/or polycosanolic acids are present in amounts ranging from 0.01 to 50 mg, preferably from 0.1 to 2 mg per kg body weight.  
       [0038] The compositions of the invention can further contain other conventional components, such as oligoelements, mineral salts, bioflavones, extracts of medicinal herbs, phytosterols, amino acids, peptides, etc.  
       [0039] The present invention also relates to the procedures for the preparation of the mixtures of one or more active principles either in the form of oily solutions (see examples 1-3), water-dispersible lipoprotein powders (see examples 4 and 5) or of powders water-dispersible liposaccharide powders (see example 6), as well as to the various oral formulations and functional foodstuffs containing the above mentioned active principles. Oily solutions may be used both for the preparation of suitable functional foodstuffs (dressing oils and oily food derivatives such as margarine, butter, mayonnaise, sauces, creams, chocolate, etc.) and for the galenic formulations consisting of hard- or soft- gelatin capsules containing them.  
       [0040] The water-dispersible lipoprotein powders are prepared by complexing lipophilic active principles with suitable water-soluble protein excipients such as albumins, delipidized albumins, soy-bean proteins, wheat proteins, caseins, milk serum proteins, gelatins, and the like. The water-dispersible liposaccharidic powders are prepared by complexing the lipophilic active principles with suitable saccharide excipients such as lactose, starches, cellulose, honey or fractions thereof, chitins and chitosans, pectins, inulins, natural fibers, cyclodextrins, and the like.  
       [0041] Both powders can be used for the preparation of a variety of functional foodstuffs, for example by:  
       [0042] a) mixing with flours for the preparation of bread, pasta, cracker, biscuits or other bakery products;  
       [0043] b) addition to fruit juices, soft drinks or other beverages;  
       [0044] c) addition to milk and derivatives thereof (yogurt, puddings, ricotta, cheese, etc.).  
       [0045] Furthermore, said powders can be used for galenic formulations, such as tablets, sugar-coated pills, sachets, effervescent tablets, chewing gums, etc.  
       [0046] Some examples of procedures for the preparation of both the oily mixtures and the powders of the active principles, as well as of the different possible formulations of the invention, are reported in the following: 
     
    
    
     EXAMPLE 1  
     Oily Solution of  
     [0047]                                              a)   18.3 g of a mixture consisting of 60% of fish oil   g   19           (containing 28% of EPA and 18% of DHA),           20% of borage oil (containing 18% of γ-linolenic acid)           and 20% of CLA-enriched maize oil (40%) added with           vitamin E (200 mg), vitamin C palmitate (400 mg),           lipoic acid (100 mg) +       b)   terpene fractions of essential oils of lemon (70%),   g   0.475           thyme (25%), clove (2.5%), and nutmeg (2.5%),           preferably containing d-limonene, sabinene,           α-pinene, β-pinene, eugenol, thymol, β-caryophyllene +       c)   1-piperoylpiperidine +   mg   100       d)   policosanols (80%) and polycosanolic acids (20%)   g   0.425           from wax rice                    
     [0048] Mixture a) is heated at 45°-50° C. under mild stirring, then slowly added with components b), c) and d) which homogeneously dissolve in a few minutes. The resulting homogeneous oily solution is then cooled at room temperature and stored for further galenic or alimentary uses.  
     EXAMPLE 2  
     Oily Solution of  
     [0049]                                              a)   18.3 g of cod oil containing 18% of EPA   g   19           and 12% of DHA added with vitamin E           (200 mg), vitamin C palmitate (400 mg),           lipoic acid (100 mg) +       b)   terpene fractions of essential oils of lemon (70%),   g   0.475           nutmeg (10%), thyme (20%) containing           d-limonene, sabinene, α-pinene, β-pinene, eugenol,           thymol and β-caryophyllene +       c)   1-piperoylpiperidine +   mg   25       d)   polycosanols and/or polycosanolic acids from rice wax   g   0.5                    
     [0050] The oily mixture of the various active principles is prepared as described in Example 1.  
     EXAMPLE 3  
     Oily Solution of  
     [0051]                                              a)   95.9 g of EPA ethyl ester (50%) + DHA ethyl   g   98           ester (30%) + γ-linolenic           acid ethyl ester (20%) added with           vitamin E (600 mg) vitamin C palmitate (1.2 g) and           lipoic acid (300 mg) +       b)   terpene fractions of essential oils as in Example 1 +   g   1       c)   1-piperoylpiperidine as in Example 1 +   mg   50       d)   polycosanols and/or polycosanolic acids from sugar cane   g   0.9           wax                    
     [0052] The oily mixture of the various active principles is prepared as described in Example 1.  
     EXAMPLE 4  
     Water-Dispersible Lipoprotein Powders of  
     [0053]                                              a)   delipidized egg albumin or milk caseins or   g   500           soy proteins or a mixture thereof) +       b)   terpene fractions of essential oils as   g   5           in Example 1 +       c)   1-piperoylpiperidine +   g   0.05       d)   polycosanols and/or polycosanolic acids from citrus   g   5           wax +       e)   vitaminized mixture of fish oil, oil of borage and CLA   g   30           as in Example 1                    
     [0054] All the components are dissolved under stirring in 2.5 liters of water and mixed for 2/4 minutes in a mechanical blade homogenizer at 20°-25° C.; the solution is subsequently spray-dried to a powder, which is the stabilized water-dispersible lipoprotein complex of the lipophilic and vitaminic active principles and can be used as such for the preparation of both pharmaceutical or dietary formulations and various functional foodstuffs.  
     EXAMPLE 5  
     [0055] Water-Dispersible Lipoprotein Powders of  
                                              a)   soy proteins +   g   250       b)   246.95 g of soy lecithin (rich in linoleic and linolenic   g   250           acids) added with vitamin E (1 g), vitamin C           (2 g), vitamin B6 (50 mg), folic acid (100 μg)           and vitamin B12 (100) +       c)   polycosanols and/or polycosanolic acids from rice wax +   g   2.5       d)   terpene fractions of essential oils as   g   5           in Example 1 +       e)   1-piperoylpiperidine   g   0.05                  
 
     [0056] The powders are prepared as described in Example 5.  
     EXAMPLE 6  
     [0057] Water-Dispersible Liposaccharidic Powders  
                                              a)   wheat strach or β-cyclodextrins or pectins or   g   200           cellulose and vegetable fibers of other species) +       b)   polycosanols and polycosanolic acids from wheat   g   1.0           waxes +       c)   terpene fractions of essential oils as in Example 1 +   g   1.0       d)   1-piperoylpiperidine +   mg   10       e)   49.150 g of a mixture of linseed oil (50%) and   g   20           borage oil (50%) added with vitamin E           (100 mg) vitamin C palmitate (200 mg), lipoic acid           (50 mg) and vitamin B6 (5 mg)                  
 
     [0058] The mixture of the different active principles is obtained as described in Example 4.  
     [0059] Pharmacological and/or Dietetic Tests  
     [0060] The pharmacological and/or dietetic characteristics of the compositions of the present invention were experimentally tested on rat and clinically tested on man.  
     [0061] Rats received hypercaloric, hypertriglyceridemizing and hypercholesterolemizing diet. After twenty days of treatment, the effect of the compositions on the following parameters was evaluated:  
     [0062] 1) lipoperoxides levels in plasma, liver, brain and heart;  
     [0063] 2) body weight;  
     [0064] 3) fluidity of the membranes of erythrocyte ghosts and plasma platelets;  
     [0065] 4) total cholesterol and HDL cholesterol plasma levels;  
     [0066] 5) total triglycerids plasma levels.  
     [0067] 80 Male rats, each weighing 150-200 g, were used. The animals were subdivided into 8 groups of 10 animals each:  
     [0068] 1 st  group: control (C); 10 animals (control at time 0) received no treatment, 10 animals received for 20 days standard hypercaloric, hyperlipidemizing and hypercholesterolemizing diet consisting of:  
     [0069] 20% casein; 3.5% mixture of oligoelements and mineral salts; 0.1% mixture of vitamins; 0.2% choline ditartrate; 2% cellulose; cholesterol 0.5%; 0.25% sodium cholate; 58.44% saccharose; 10.0% lard and 4.9% olive oil.  
     [0070] 2 nd  group: treated with vitaminized fish oil (OP); animals received for 20 days the same diet as the controls, except that 1.9 g of vitaminized fish oil as reported in Example 2 replaced in part a similar amount olive oil (olive oil used: 3.0%).  
     [0071] 3 rd  group A: animals were treated with a polycosanols mixture (octacosanol=50%) of rice wax (PLC), animals received for 20 days the same diet as the controls, except that 0.5 g of rice wax polycosanols replaced in part a similar amount of olive oil (olive oil used: 4.4%).  
     [0072] 3 rd  group B: animals were treated with a mixture of polycosanolic acids (PLC ac.) (montanic≅50%) obtained by oxidation of the mixture of rice wax polycosanols of 3 rd  group A; animals received for 20 days the same diet as the controls, except that 0.5 g of rice wax polycosanolic acids replaced in part a similar amount of olive oil (olive oil used: 4.4%).  
     [0073] 4 th  group: animals were treated with a terpene mixture (TRP); animals received for 20 days the same diet as the controls, except that 0.475 g of a terpene mixture as reported in Example 1 replaced in part a similar amount of olive oil (olive oil used: 4.425%).  
     [0074] 5 th  group: treated with 1-piperoylpiperidine (P); animals received for 20 days the same diet as the controls, except that 0.025 g of 1-piperoylpiperidine replaced a similar amount of olive oil (olive oil used: 4.875%).  
     [0075] 6 th  group: treated with a terpene mixture+1-piperoylpiperidine+vitaminized fish oil (TRP+P+OP); animals received for 20 days the same diet as the controls, except that 1.9 g of vitaminized fish oil+0.475 g of a terpene mixture+0.025 g of 1-piperoylpiperidine replaced a similar amount of olive oil (olive oil used: 2.5%).  
     [0076] 7 th  group: treated with vitaminized fish oil+a mixture of terpenes+1-piperoylpiperidine+a mixture of polycosanols (50%) and polycosanolic acids (50%) (OP+TRP+P+PCL); animals received for 20 days the same diet as the controls, except that 1.9 g of vitaminized fish oil, 0.475 g of a terpene mixture, 0.025 g of 1-piperoylpiperidine and 0.5 g of polycosanols and polycosanolic acids replaced 2.9 g of olive oil (olive oil used: 2.0 g).  
     [0077] Results are reported in the following tables I, II and III.  
               TABLE I                          Percent changes of the fluidity of the membrane of       erythrocyte ghosts and plasma platelets (expressed       as % compared with controls values at time 0) of the       rats before and after 20 days of dietary treatment.                                 membrane           membrane fluidity   fluidity           (erythrocyte ghosts))   (plasma platelets)                                     1 st  A control rats at time 0   100%   100%       1 st  B control rats after 20 day    72%    69%       diet       2 nd  treated rats (OP)    76%    74%       3 rd  A treated rats (PLC)    74%    71%       3 rd  B treated rats (Ac. PLC)    82%    81%       4 th  treated rats (TRP)    76%    71%       5 th  treated rats (P)    73%    70%       6 th  treated rats (OP + TRP + P)    90%    91%       7 th  treated rats    96%    96%       (OP + TRP + P + PLC)                  
 
     [0078]               TABLE II                          Lipoperoxides levels [expressed as n mols of malonyldialdehyde (MDA)       per gram of tissue or per ml of plasma] in plasma, liver, brain and heart       of rats before and after 20 day dietary treatment.                                                                                 Percent               Percent       Percent       Percent       change           MDA   change vs.   MDA   change vs.   MDA   change vs.   MDA   compared           PLASMA   controls   LIVER   controls   BRAIN   controls   HEART   with controls                                                             1 st  A control   2.5 ± 0.5   //   25.5 ± 5.9   //    55 ± 4   //   24 ± 5   //       rats at time 0       1 st  B control   5.1 ± 0.6     100%   44.2 ± 8.2     100%   108 ± 6     100%   45 ± 6     100%       rats after 20       days of diet       2 nd  treated   5.0 ± 0.6    −1.9%   45.1 ± 8.2      2%   106 ± 7    −1.8%   44 ± 9    −2.2%       rats (OP)       3 rd  A treated   4.8 ± 0.5    −5.8%   43.1 ± 6.5    −2.4%   105 ± 9    −2.8%   42 ± 7    −6.6%       rats (PLC)       3 rd  B treated   3.9 ± 0.5   −22.0%   36.2 ± 6.1   −22.1%    95 ± 7   −12.0%   39 ± 7   −13.3%       rats (Ac. PLC)       4 th  treated   4.7 ± 0.4    −7.8%   41.8 ± 8.2    −5.4%   108 ± 7    −0.0%   44 ± 9    −2.2%       rats (TRP)       5 th  treated   5.0 ± 0.3    −1.9%   43.5 ± 7.8    −1.5%   107 ± 5    −0.9%   44 ± 7    −2.2%       rats (P)       6 th  treated   3.6 ± 0.4   −29.4%   34.7 ± 6.8   −21.4%    81 ± 8   −25.0%   36 ± 8     −20%       rats (OP +       TRP + P)       7 th  treated   2.9 ± 0.4   −43.1%   29.9 ± 7.1   −32.3%    76 ± 10   −29.6%   32 ± 8   −28.8%       rats OP +       TRP + P + PLC)                    
     [0079]               TABLE III                          Change of the body weight and of total cholesterol,       HDL cholesterol and triglycerids plasma levels in rats       before and after 20 days of diet treatments.                                     Total cholesterol   HDL cholesterol   total triglycerids   body weight           (mg dl −1 )   (mg dl −1 )   (mg dl −1 )   (g)               1 st  A) control rats    35.6 ± 1.8   26.2 ± 1.4   50.2 ± 7.7   180 ± 12       at time 0       1 st  B) control rats   126.2 ± 13.5 (100%)   29.4 ± 1.6   82.5 ± 9.5 (100%)   224 ± 19 (100%)       after 20 day diet       2 nd  treated rats   120.4 ± 12.7 (−4.5%)   28.9 ± 2.8   80.5 ± 6.8 (−2.4%)   221 ± 16 (−1.3%)       (OP)       3 rd  A) treated rats   114.3 ± 10.1 (−12.5%)   31.6 ± 3.9   81.4 ± 8.7 (−1.3%)   219 ± 18 (−2.2%)       (PLC)       3 rd  B) treated rats    89.2 ± 8.1 (−29.3%)   32.0 ± 4.1   75.2 ± 8.5 (−8.8%)   208 ± 16 (−7.1%)       (Ac. PLC)       4 th ) treated rats   113.9 ± 12.4 (−9.7%)   29.9 ± 2.0   80.4 ± 10.5 (−2.5%)   219 ± 14 (−2.2%)       (TRP)       5 th ) treated rats   125.2 ± 12.5 (−0.7%)   29.3 ± 1.5   81.9 ± 8.7 (−0.7%)   223 ± 16 (−0.4%)       (P)       6 th ) treated rats    71.7 ± 8.9 (−43.1%)   32.1 ± 3.8   72.5 ± 7.9 (−12.1%)   200 ± 20 (−10.7%)       (OP + TRP + P)       7 th ) treated rats    54.8 ± 3.9 (−56.5%)   32.4 ± 4.1   68.7 ± 5.4 (−16.7%)   186 ± 15 (−16.9%)       (OP + TRP + P + PLC)                    
     [0080] Membrane fluidity of erythrocyte ghosts and plasma platelets was measured using TMA-DPH as fluorescent probe, according to the method by Caimi F. et al., 1999, Thromb. Hoemost., 82 pp. 149.  
     [0081] Malonyldialdehyde was evaluated according to the procedure by K. Yagi et al., 1982, in “Lipid Peroxides in Biology and Medicine”, Academic Press, New York, pp. 324-340.  
     [0082] The data reported in tables I, II and III evidence that the compositions of yhe invention are able of promoting, in rats receiving for 20 days a hypercaloric diet and enriched in saturated animal fats and cholesterol, a surprising synergistic effect in:  
     [0083] restoring membrane fluidity of ghosts and platelets;  
     [0084] improving antioxidant defenses of plasma, liver, brain and heart;  
     [0085] reducing excessive increase in body weight;  
     [0086] limiting excessive increase in plasma cholesterol and triglycerid levels.  
     [0087] Said beneficial and therapeutical effects are always significantly higher than the sum of the beneficial effects obtainable by administering separately the single components of the mixture.  
     [0088] The data reported in Tables I, II and III show that mixtures of polycosanolic acids administered alone always promote, in rats receiving for 20 days a hypercaloric diet enriched in saturated animal fats and cholesterol, a surprisingly higher effect than that obtained with the corresponding mixtures of polycosanols in:  
     [0089] restoring membrane fluidity of ghosts and platelets;  
     [0090] improving antioxidant defenses of plasma, liver, brain and heart;  
     [0091] a reducing excessive increase in body weight;  
     [0092] limiting excessive increase in plasma cholesterol and triglycerid levels.  
     [0093] Clinical trials were carried out on different groups of patients both healthy and suffering from one or more of the many aging-related dysmetabolic disorders (atherosclerosis; obesity and overweight; hypercholesterolemia and/or hypertriglyceridemia; hypertension; diabetes; cerebral-degenerative diseases such as Alzheimer, Parkinson, senile dementia, loss of memory and the like; stress and/or depression; menopausal syndromes; prostate hypertrophy; osteoporosis; aging of the skin; panniculopathies (cellulite); alopecia). Patients were subjected to dietotherapic treatment with the mixtures reported in Example 1 or in Example 2. Doses and times varied depending on the treated groups.  
     [0094] In all clinical trials, the beneficial, therapeutical effects obtainable with the administration of the mixtures reported in Example 1 or in Example 2 were always significantly high, in the prevention of aging biological symptoms (better membrane fluidity, improvement of antioxidant defenses, limitation of weight excesses) and in the improvement of some of the tested clinical parameters; therefore said compositions may be usefully employed both is aging prevention and as coadjuvants and synergetic agents to improve the therapeutical action of drugs already normally in use in the treatment of the above cited diseases.  
     [0095] Furthermore, said beneficial aspects were always by far higher than the sum of the effects obtainable by the administrations of the single active principles of the different mixtures.  
     [0096] Finally, these clinical trials in humans showed that the administration of a mixture of polycosanolic acids alone was surprisingly more effective in preventing aging biochemical symptoms (better membrane fluidity, improvement of antioxidant defenses, limitation of weight excesses, reduction of plasma cholesterol and triglycerides, etc.) than the administration of the mixture of the corresponding polycosanols alone.