CA2109958C

CA2109958C - Calcium, trace mineral, vitamin d and drug therapy combinations

Info

Publication number: CA2109958C
Application number: CA002109958A
Authority: CA
Inventors: Mark Benson Andon
Original assignee: Procter and Gamble Co
Current assignee: Procter and Gamble Co
Priority date: 1991-05-28
Filing date: 1992-05-15
Publication date: 1997-06-10
Anticipated expiration: 2012-05-15
Also published as: SK132693A3; CZ281823B6; HU9303364D0; NO934282D0; AU1996892A; HUT66379A; NO934282L; WO1992021355A1; AU666654B2; BR9206072A; KR100244603B1; JPH07502012A; IE921701A1; NZ242920A; CZ255393A3; EP0586521A1

Abstract

Nutritional mineral supplements comprising calcium citrate malate, salts of manganese, copper and zinc and a member or members selected from the group of vitamin D or its metabolites or precursors and drug therapies consisting of calcitonin, editro-nate, diphosphonated and amino-diphosphonates are disclosed. Estrogen can also be used with these supplements. These supple-ments, which provide at least 25 % RDA of the calcium, trace minerals and vitamins, are used in addition to the normal diet.
These supplements are useful for increasing bone growth and for treating age-related bone loss in humans and animals. The sup-plements may be in the form of solid tablets, liquid unit dosage forms, or in a beverage.

Description

~ 21~99~8 CALCIUM, TRACE MINERAL, YITAMIN D AND
DRUG THERAPY COMBINATIONS
.. , TECHNICAL FIELD
The present invention relates to nutritional and therapeutic i~,:u~c ts in calcium supplements containing trace minerals, in particular copper, manganese and zinc and vitamin D, estrogen, calcitonin or Didronel or diph~s~ 7te drug therapies. These supplements are useful 0 for increasing bone growth and treating age-related bone loss. They can be used in co~junction with foods and beverages or taken as an oral solid or liquid supplement.
The invention also relates to a method of building bone or treating bone loss in osteoporosis patients, post-menopaus-al women and/or elderly men.
BACK~ROUND OF THE INVENTION
Vitamin and mineral supplements for human and veteri-nary use are commonplace. Some diets, heavy physical exercise and disease conditions may require the intake of 2û considerable quantities of minerals and vitamins apart from those generally obtained through what otherwise would be considered a normal diet. Vitamin and mineral supplementa-tion is important primarily for those who have inadequate diets, including growing children. Older adults have an additional need for calcium to help prevent the bone loss which occurs as a normal c~. e~ of the aging process.
In particular, pG~ eal women need additional calcium due to hormon21 changes which can accelerate the bone loss rate leading to a further diminishment in bone mass.
The trace minerals which affect bone growth are cop-per, zinc and manganese. Supplementation of the diet with these minerals along with a highly bioavailable source of calcium is highly desirable. Commercially available miner-al supplements are useful in many circumstances where increased mineral intake is desirable. Most of th~se multi-vitamin and multi-mineral tablets are low in calcium, requiring separate supplementation with calcium sources.
In addition, not all calcium sources are equal in terms of bioavailability and absorption. The addition of the vita-min D, calcitonin, estrogen and/or other therapy (editronate or diphosphonates) makes the supplementation more complex since three pills or more could be involved.
It would be more convenient if all of the minerals and drugs and/or vitamins could be administered conjo~ntly in a convenient and/or pleasant tasting form which would not re-quire extra attention, planning and implementation by the user. This could be done in the form of foods and beverag-es as well as in the form of tablets.
There are well-recognized problems associated with adding both minerals and vitamins to foods and beverages.
Some of these are taste; calcium tends to be chalky in flavor. In addition, the solubility of many calcium sourc-es prevents them from being added to many beverages.
Others are interactions of the minerals or vitam~ns with the food or beverage which affects the stability and/or the bioavailabilty of the product. This invention provides a ~eans for making such product.
This invention also relates to methods of building bone in humans and other animals, i.e., for the treatment of age-related bone loss and related disorders. In partic-ular, this invention relates to such methods of trea~tment by administration of certain calcium salts and the miner-als, copper, zlnc and manganese along with vitamin D and/or drug therapy.
Calcium is the fifth most abundant element in the human body. It plays an important role in many physiologi-cal processes, including nerve and muscle functions. Not surprisingly, nutritional and metabolic deficiencies of calcium can have broad-ranging adverse effects. Since about 987~ to 99% of the body's calcium is found in bone tissues, many of these adYerse effects are manifested _ _ _ _ _ WO92/21355 ?1n~ gUS92/0399 through deficiencies in the structure, function and integ-rity of the skeletal system.
The most common metabolic bone disorder is osteoporosis. Osteoporosis can be generally defined as the reduction in the quantity of bone, either from the reduc-tion in bone formation or the acceleration of bone resorption, in either eYent the result is a decrease in the amount of skeletal tissue. In general, there are two types of osteoporosis: primary and secondary. "Secondary osteoporosis" is the result of an identifiable disease process or agent. HoweYer, approximately 90% of all osteoporosis cases are idiopathic "primary osteoporosis~.
Such primary osteoporosis includes po~L ~ ~al osteoporosis, age-associated osteoporosis (affecting a majority of individuals over the age of 70 to 80), and idiopathic osteoporosis affecting middle-aged and younger men and women.
For some osteoporotic individuals the loss of bone tissue is sufficiently great so as to cause mechanical failure of the bone structure. Bone fractures often occur for example, in the wrist, hip and spine of women suffering from po,i r7~lC~l osteoporosis. Kyphosis (abnormally increased curvature of the thoracic spine) may also result.
The mechanism of bone loss in osteoporotics ~s be-lieved to involve an imbalance in the process of ~bone remodelingn. Bone remodeling occurs throughout life7 renewing the skeleton and maintaining the strength of bone.
Two reactions are involved, bone loss or resorption and bone growth or accretion. This remodeling occurs in a series of discrete pockets of activity in the bone, called nosteoclasts" and "osteoblastsn. Osteoclasts (bone dis-solving or resorbing cells) are responsible for the resorption of a portion of bone within the bone matrix, during the resorption process. After resorption, the osteoclasts are followed by the appearance of osteoblasts 2~9~8 (bone forming cells), which then refill the resorbed por-tion with new bone.
In young healthy adults, the rate at which the osteoclasts and osteoblasts are formed maintains a balance of bone resorption and bone formation. However, as normal S ~ , ~y of aging an imbalance in this remodeling pro-cess develops, resulting in loss of bone at a rate faster than the accretion of bone. As imbalance continues over time the reduction in bone mass and thus bone strength leads to fractures.
Many compositions and methods are described in the medical literature for the "treatment" of osteoporosis.
See, for example, R. C. Haynes, Jr. et al., ~Agents affect-ing Calcification", The Pharmacolo~ical Rasis of TheraDeutics. 7th Edition (A. 6. Gilman, L. S. Goodman et al., Editors, 1985); and G. D. Whedon et al., ~An Analysis of Current Concepts and Research Interest in Osteoporosis~, Current Advances in Skeletoaenesis (A. Ornoy et al., Ed~-tors, 1985). Estrogen is often used to affect the metabo-lism of calcium by influencing the osteoblast cells.
Z Treatments using fluoride have also been described. Howev-er, the utility of such agents may be limited, because of possible adverse side effects. See W. A. Peck, et al., Phvsician's Resource Manual on OSteODOroSis (1987), pub-lished by the National Osteoporosis Foundation.
Nutritional therapies for osteoporosis have ~lso~been proposed. Many calcium-containing compounds and composi-tions have been described for use as nutritional supple-ments. Many commercial preparations are also available, typically containing calcium carbonate or calcium phos-phate. Other calcium salts have also been described for use in calcium supplements, including calcium lactate, calcium citrate and calcium gluconate.
US 3,949,098 issued Bangert (assigned Nabisco, 1976~
describes a nutr~tious orange dr~nk c ~ ~rate that con-tains whey protein. The patent suggests the addition of WO 92/21355 . PCr/US92/03995 5 ;2~1~99$8 minor amounts of vitamins and other nutrients which include various cupric salts, manganese salts, zinc salts, as well as calcium salts.
German OLS 2,845,570 issued to E.R.E. (Europe Repre-sentation Establishment, 1980) describes a honey containing composition. Honey contains low levels of calcium, manga-nese, copper as well as trace amounts of magnesium, iron, r~ p~ .., silicon and nickel. The value of honey as a medicant is undisputed according to this patent applica-tion. This application claims a honey containing composi-tion with levarotatory ascorbic acid and citric acid. This patent has issued as US 4,243,794 ~1981).
US 4,497,800 issued to Larsen et al (assigned Mead Johnson & Company, 1985) describes a nutritionally complete ready-to-use liquid diet for providing total patient nour-ishment. The diet contains free amino acids and small peptides, a .a,L~hy~l~te source, and nutritionally signifi-cant amounts of all essential vitamins and minerals, and stabilizers. The minerals include calcium, copper, zinc and manganese, among others. Most of these minerals are given as the gluconate salt.
"Effects of calcium carbonate and hydroxyapatite on zinc and iron retention in po, p-- al womenn, Dawson-Hughes, Seligson and Hughes, American Journal Q C~inical Nutrition. 44, 83-88 (1986) describes the effect of calcium carbonate on whole-body retention of zinc and iron in thirteen healthy post r -al women. The test meal, including both dry food and a formulated beverage, included calcium, copper and zinc at a level of one-third the usual daily requirement. These are levels normally found in human diets.
US 3,992,555 issued to Kovacs (assigned Vitamins, Inc., 1976) describes food supplements prepared by mixing assimilable iron - : 'c, vitamins and minerals with a heated edible fat carrier. The minerals include calcium zinc, copper, and -e among others.

US 3,950,547 issued to Lamar et al (assigned Syntex Inc, 1976) describes a dietary composition containing peptides and/or amino acids, lipids and ca~Lo~,~d.aLes in an aqueous emulsion. Suitable minerals for adding at low levels include among others calcium, copper and zinc.
US 4,107,346 issued to Kravitz (1978) describes a dietary salt composition for use as a replacement for salt 1n foods. The role of copper is described as a component of several enzymes essential for nutrition. The patent further discloses that ~spontaneous fractures are common in animals feeding off copper deficient soils or who are given artificially depleted copper diets~. (column 4, lines 20-30) Zinc is described as helping in growth, wound healing and improving taste and smell. Clinical symptoms of manganese deficiency have not been observed in man.
However, there is no question that manganese is essential for human nutrition. Main manifestations of its deficiency are impaired growth and skeletal abnormalities. Calcium is described as bei~g necessary for blood coagulation, for calcium retention, and for relieving the sy0ptoms of osteoporosis. Examples of salts that contain these four trace minerals are disclosed.
US 4,070,488 issued to Davis (unassigned, 1978) dis-closes a highly stabilized balanced nutrit~ve composition useful in supplementing the diet of humans and/or animals.
This compositlon contains gelatin. The patent discloses that the sulfhydryl groups of the gelatin can render copper inactive toward ascorbic acid.
US 4,214,996 issued to B~ r et al (R.G.B. Labo-ratories, 1980) discloses mineral compositions wh~ch are very soluble. These compositions contain calcium, phospho-rus, zinc, as well as manganese. Not all of the composi-tions that are described contain all four elements.
US 4,351,735 to E '' ,~. et al (R.G.B. Laboratories, 1982) is related to the `996 patent.

W092/213S5 ~n395~/US92/0399 "Nutrients and Nutrition of Citrus Fruits," Citrus Nutrition and Qualitv. Ting, (American Chemical Society, 1980) disc~oses the presence of certain trace minerals in orange juice. These include copper, zinc, iron and manga-nese. Calcium and magnesium are the two major divalent cations in orange juice. The leYels of al~ the minerals are low.
I, ,e ru,d et al, "Interactiûn ûf pH and ascorbate in intestinal iron absorption," (1983) describes the iron absorption from various food materials. The diet which was 1û low in iron also contained calcium carbonate, Illa.l~a,.~Se sulfate and copper sulfate among others.
US 4,419,369 issued to Nichols et al (assigned Baylor College of Medicine, 1983) describes an improved dietary protein mineral module for infants. An a~ ,.iD~àte analy-sis of the material shows the presence of iron, zinc, copper and calcium.
The utility of these known supplements varies. Unlike agents (such as estrogen) which affect the metabolism of bone, nutritional supplements such as calcium, have been thought to merely provide a source of the nutrient (which may or may not be properly absorbed and metabolized). See, for example, B. Riis et a~., "Does Calcium Supplementation Prevent P~, rallcal Bone Loss?," New Enqland J. of Medi-cine, 316, 173-177 (1987); L. Nilas et al., "Calcium Supplementation and PosL ,~ ~al Bone Loss,~ British Medical Journal. ~, 1103-1106 (1984); and H. Spencer et al., "NIH cDr- - l~t c~ r~ Osteoporosis," Journal of NutritiQn. ~, 316 -319 (1986).
It has now been discovered, however, that the adminis-tration of mixtures of certain calcium salts and trace minerals are effective for delaying age-related loss of bone (see co-pending application of Smith et al., Serial Number 07/562,773). Furthermore, it has been separately found that the administration of mixtures of certain calci-um salts with vitamin D is also effective for attenuating (i see 1 ~ ltr9t1~. number on page 32) S~ 8 age-associated bone loss (see co-pending application of Andon et al, Serial Number (P&G Case 4394). It would be desirable, therefore to have mixed calcium, trace mineral and vitamin D therapies which are compatible and nutr~tion-ally available since this method would provide greater S efficacy as compared to nutritional regimens known in the art. In addition, this nutritional regimen would be ex-tremely useful as an additional or adjunct therapy for known drug treatments of bone disease and age-related bone loss, i.e. calcitonin, estrogen and didronel, including salts of amino functional compounds. Moreover, it would be quite useful to have such nutritional supplements which could be added to food and beverage compositions without undesirably affecting organoleptic and aesthetic proper-ties .
It is an object of the present invention to provide calcium and trace mineral supplements which, when combined with v~tamin D, and/or calcitonin, Didronel or estrogen, provide bone growth and can be used to treat age-related bone loss or to correct the imbalance that occurs between bone formation and bone resorption.
It is a further object of this invention to provide foodstuffs, beverages and beverage concentrates which are supplemented with calcium, trace minerals, vitamin D, and/or related drug therapies.
These and other objects are readily apparent from the description herein.
SUMMARY OF THE INVENTION
The supplements employ specific calcium salts of mixtures of cttric and malic acids. The drug and/or vitamin therapies which they are combined with include vitamin D, Didronel (diphosphonates) and calcitonin. The mineral supplements comprise zinc, copper and a.., -e.
Estrogen can be used in conjunction with any of these therapi es .
.

WO 92/21355 PCI`/US92/03995 9: 21~9958 The present invention provides methods for building bone in a human or other animal subject, comprising admin-istering to said subject a safe and effective amount of vitamin D, didronel, estrogen and/or calcitonin, along with calcium citrate malate and copper, zinc and ~ ~e salts. The calcium citrate malate comprises a complex or a mixture of calcium salts having a ratio of moles citrate to moles malate of from about 1:0.16 to about 1:13.5. The combination of these minerals and drugs is preferably administered in an oral dosage form, containing pharmaceu-tically-acceptable carriers and e%cipients.
All ratios, proportions and percentages herein are by weight, unless otherwise specified. All weights of the minerals are on an elemental basis unless otherwise speci-fied .
DETAII Fn DESCRIPTION OF THE INVENTION
The present invention relates to stable miner-al/vitami~ and/or drug supplements and supplemented foods and beverages including dry beverage mixes and to a method of building bone.
As used herein, the term "comprising" means various components can be conjointly employed in the mineral sup-plements, foods and beverages of the present invention.
Accordingly, the terms "consisting essentially of" and "consisting of" are embodied in the term comprising.
By ~nutritional~ or ~nutritionally-supplemental amount" herein is meant that the mineral and vitamin sourc-es used in the practice of this invention provide a nour-ishing amount of the trace minerals, calcium and vitamin D.
This is supplemental or in addition to the amount found ~n the diet. This supplemental amount will comprise at least 25X of the r~ d Dietary Allowance (RM) of the daily intake of calcium, copper, manganese, zinc and vitamin D.
Preferably, at least 50% of the ~ ' i Dietary Allow-ance (RDA) will be provided. The RDA for minerals and vitamins is as defined in The United States of America (see 3~ ~'CIIUS92/03995 2t~9S8 ~er ~cd Daily Dietary Allowance-Food and Nutrition Board, National Academy of Sciences-National Research Council ) .
Speciflc compounds and compositions to be used in these processes must, accordingly, be pharmaceutically acceptable. As used herein, a '`pharmaceutically accept-ablea component is one that is suitable for use with humans and/or animals without undue adverse side effects (such as toxicity, irritation, and allergic response) commensurate with a reasonable benefit/risk ratio. Further, as used herein, the term "safe and effective amount" refers to the quantity of a component which is sufficient to yield a desired therapeutic response without undue adverse side effects (such as toxicity, irritation, or allergic re-sponse) commensurate with a reasonable benefit/risk ratio when used in the manner of this invention. The specific ~safe and effective amount" will, obviously, vary with such factors as the particular condition being treated, the physical condition of the patient, the duration of the treatment, the nature of .~r,t therapy (if any), and the specific formulations employed.
As used herein, the term "flavors~ includes both fruit and botanical flavors.
As used herein the term "sweeteners" includes sugars, for example, glucose, sucrose, and fructose. Sugars also include high fructose corn syrup solids, invert sugar, sugar alcohols, including sorbitol, and mixtures thereof.
Artificial sweeteners are also included in the term sweet-ener.
As used herein, the term "trace minerals~ means cop-per, manganese and zinc. These minerals play an important role in nutrition, but are required in only small or trace amounts in the diet. All three of these minerals are important enzymatic cofactors which are essential in devel-opment of bone in animals and humans. The trace minerals WO 92/21355 PClr/US92/03995 Il 21099~8 herein are administered in the form of pharmaceutically acceptabl e sal ts .
The "carboxylate counterion~ used in the preparation of the p~efe"èd mineral salts herein can be any ingestible carboxylate species. However, some judgement must be made with regard to flavor contribution. For example, citrate, malate and ascorbate yield ingestible complexes whose flaYors are judged to be quite acceptable, particularly in fruit juice beverages. Tartaric acid is acceptable, par-ticularly in grape juice beverages, as is lactic acid.
Longer-chain fatty acids may be used in solid mineral supplements, but can affect flavor and water solubility.
For essentially all purposes, the malate (pYé~
gluconate, citrate and ascorbate moieties suffice, although others can be selected, according to the desires of the formul ator .
The counterion for the trace minerals can also be phosphate, chloride, sulfate, nitrate or the like. Howev-er, these inorganic counterions can undesirably interact with calcium ions, especially in beverages. In high con-centrations, these counterions, particularly chloride and sulfate, may contribute an undesirable flavor note to the supplement, food, or beverage containing them. Accordingly, the carboxylate counterions noted above are ~,er~.,.d herein .
Cal ci tonin Calcitonin is a 32 amino acid protein produced by the thyroid C cells in higher mammals. It is known to block the stimulatory effects of PTH and other humoral agents on bone resorption. Calcitonin therapy decreases the rate of bone loss in osteoportoic patients. It is also used to treat Paget's disease of the skeleton and is used in combi-nation with ethane dihydroxy diphosphonate. As used here-in, the term calcitonin includes thyrocalcitonin, whether natural or synthetic.
Vitamin D

WO 92/21355 PCr/US92/03995 21~99~8 12 ~
Vitamin D includes vitamin D, cholecalciferol (D3), ergocalciferol (D2) and its biolofically active metabolites and p~Ul~U~S such as, 1c~, 25-(ûH)2 vitamin D; 25 OH
vitamin D, its biologic precursor; and 1~ hydroxy vitamin D, and analogues of the dihydroxy compound. These materi-als promote intestinal absorption of calcium, contribute to plasma calcium regulation by acting on bone density and stimulate reabsûrption of calcium by the kidney.
Didronel It is the disodium salt of l-hydroxyethylidene diphosphonic acid (EHDP or editronate). It and other related diphosphonates and amino diphosphonates are collec-tively referred to herein as "diphosphonates".
Didronel and the diphosphonates act primarily on the bone. They inhibit the formation, growth and dissolution of l,~d,u~d~atite crystals and their amorphous p~ ur5ùlS
by chemisorption to calcium phosphate surfaces. Generally, they do not adversely effect the levels of parathyroid hormones or cal ci um.
80ne-active drugs which are pharmaceutically-accept-able salts of amine-functional compounds include pharmaceu-tically-acceptable salts of amine-functional diphosphonate drug ds and phG ,~ alkylphosphinate drug com-pounds, including the prodrug esters thereof. Such com-pounds are disclosed, for example, in U.S. Patent Nos.
3,683,û80 issued to Francis on August 8, 1972; 4,304,734 issued to Jary, Rihakova ~ Zobacova on December 8, 1981;

4,687,768 issued to Benedict ~ Johnson on August 18, 1987;
4,711,880 issued to Stahl 5 Schmitz on December 8, 1987;
and 4,719,203 issued to Bosies ~ Gall on January 12, 1988;
copending U.S. patent application Serial Nos. 808,584,* of Benedict ~ Perkins filed December 13, 1985; 945,069 of Ebetino, Buckingham ~ McOsker filed December 19, 1986;
945,068 of Ebetino ~ Benedict filed December 19, 1986; and 069,666 of Ebetlno filed July 6, 1987; and European Patent Application Nos. 0,û01,584 of Blum, Hempel ~ Worms, }(~ee page 32 ~or I lira~ nwnbcræ) ~ 13 g 5 8 ';
publ i shed May 2 1979; 0, 039, 033 publ i shed Apri l 11.
1981; 0,186,405 of Benedict & Perkins, published July 2.
1986: and 0 243,173 of Oku, Todo, Kasahara, ~akamura Kayakiri & Hashimoto, published October 28, 1987.
Bone-active drugs more preferred in compositions of the present invention include pharmaceutically-acceptable salts of the following compounds or esters thereof: 6-amino-l-hydroxy-hexane-l,l-diphosphonic acid, 4-amino-1-hydroxy-butane-l,l-diphosphonic acid, N,N-dimethyl-4-amino-l-hydroxy-butane-l,l-diphosphonic acid, N,N-diethyl-4-amino-l-hydroxy-butane-l,l-diphosphonic acid, 3-amino-1-hydroxy-propane-1,1-diphosphonic acid, N,N-dimethyl -3-amino-l-hydroxy-propane-l,l-diphosphonic acid; N,N-diethyl-3-amino-l-hydroxy-propane-l,l-diphos-phonic acid, 6-aminohexane-l,l-diphosphonic acid, phenyla-minomethane diphosphonic acid, N,N-dimethylaminoethane diphosphonic acid, N-(2-hydroxyethyl)-aminomethane diphos-phonic acid, N-acetylaminomethane diphosphonic acid, 3-(2-acetylaminocyclohexyl)-l-~,~,d,u~p) ouane-l,l-diphosphonic acid, 2 -(2-aminomethylcyclohexyl)-1-hydroxyethane-1,1-di-phosphonic acid, cis-3-(2-aminocyclohexyl ) -l-l,~d, u~y~l o-pane-l,l-diphosphonic acid, 3-(l-aminocyclohexyl)-l-hydroxypropane-l,l-diphosphonic acid, 3 -~2-am~nocyclohexyl )-l-h~, u~u. upane-l,l-diphosphonic acid, 3-(2-aminocyclopentyl)-l-h~.l-o~uru-pane-l,l-diphosphonic acid, l-aminoindan-2,2-diphosphonic acid, 4 -(aminomethyl)-indan-2,2-diphosphonic acid, l-~aminomethyl)-dihydro-2-pyrindine-6,6-diphosphonic acid, 4-aminohexahydroindan-2,2-diphosphonic acid, 4 -(aminomethyl)-hexahydroindan-2,2-diphosphonic acid, octahydro-l-pyridine-5,5-diphosphonic acid; octahydro-2-pyridine-5,5-diphosphonic acid; octahydro-l-pyridine-6,6-diphosphonic acid; octahydro-2-pyridine-6,6-diphosphonic acid; octahydro-l-pyridine-7,7-diphosphonic acid; octahy-dro-2-pyridine-1,7-diphosphonic acid; 2-methyl-octahydro-l-E

= 2~ ~9S8 pyridine-5,5-diphosphonic 2cid; 1,3-diethyl-octahydro-2-py-ridine-5,5-diphosphonic acid; 7-hydroxy-octahydro-l-pyri-dine-6,6-diphosphonic acid; 4-methoxy-octahydro-2-pyridine-6,6-diphosphonic acld; 5-vinyl-octahydro-1-pyridine-7,7-di-phosphonic acid; I -(dimethylamino)-octahydro-2-pyri-5 dine-7,7-diphosphonic acid; N-acetyl-octahydro-2-pyri-dine-6,6-diphosphonic acid; N-benzyl-octahydro-l-pyri-dine-5,5-diphosphonic acid; N-(p-meti ~,1 yl)-octa-hydro-2-pyridine-7,7-diphosphonic acid; 2-(3,4-dichloro-phenyl)-octahydro-l-pyridine-7,7-diphosphonic acid; 2-(p-dimethylaminophenyl)-octahydro-l-pyridine-7,7-diphosphonic acid; 4-chloro-octahydro-l-pyridine-6,6-diphosphonic acid;
4-amino-octahydro-1-pyridine-6,6-diphosphonic acid;

7-carboxy-octahydro-l-pyridine-6,6-diphosphonic acid;
5-carboxy(methyl ester)-octahydro-l-pyridine-6,6-diphos-5 phonic acid; 4-hydroxy-octahydro-2-pyridine-6,6-diphos-phonic acid, propanoate ester; 4-(N,N-dimethylamino)-octa-hydro-l-pyridine-6,6-diphosphonic acid; 5 -(N-acetamido)-octahydro-l-pyridine-7,7-diphosphonic acid; 7-(ethylke-tone)-octahydro-2-pyridine-5,5-diphosphonic acid; and 4-nitro-octahydro-1-pyridine-6,6-diphosphonic acid; (2'-pi-peridinyl)-methane diphosphonic acid;
(3'-piperidinyl)-methane diphosphonic acid; (4'-piperidinyl)-methane diphosphonic acid; 2-(2'-piperidinyl)-ethane-l,l-diphosphonic acid; 2-(3'-piperidinyl)-ethane-l,l-diphosphonic acid; 2 -(4'piperidinyl)ethane-l,l-diphosphonic acid; 2-(2'piperi-dinyl)-l-hydroxy-ethane-l,l-diphosphonic acid; 2-(3'-piperidinyl)-l-hydroxy-ethane-l,l-diphosphonic acid; 2-(4'-piperidinyl)-l-hydroxy-ethane-l,l-diphosphonic acid; 2-(2'-(3~methyl)-piperidinyl)-ethane-l,1-diphosphonic acid;
2-(2' -(5'-methyl)-piperidinyl )-ethane-l,l-diphosphonic acid; 2-(2'-(3'-methyl)-piperidinyl)-l-hydroxy-ethane-l,l-diphosphonic acid; 3 -(2'-piperidinyl)-propane-1,1-diphosphonic acid; 3 -(3'-piperidinyl)-propane-1,1-diphosphonic acid; 3 -(4'-piperidinyl)-propane-1,1-diphosphonic acid; 3 ~, ~.~

WO 92/21355 r PCr/US92/03995 1 . 2 1 0 9~ 9 S 8 -(2'-piperidinyl)-1-hydroxy-propane-1,1-diphosphonic acid;
3-(3'-piperidinyl)-1-hydroxy-propane-1,1-diphosphonic acid;
3 -(4'-piperidinyl )-1-hydroxy-propane-1,1-diphosphonic acid; 3 -(2'-piperidinyl)-propane-2,2-diphosphonic acid; 3 -(3'-piperidinyl)-propane-2,2-diphosphonic acid; 3 -(4'-piperidinyl)-propane-2,2-diphosphonic acid; 2 -(2'-(N-methyl)-piperidinyl)-l-hydroxy-ethane-l,l-diphosphonic acid; 2-(2'-piperi-dinyl)-l-amino-ethane-l,l-diphosphonic acid; 2 -(3'-piperidinyl)-1-amino-ethane-1,1-diphosphonic acid;
0 2-(4'-piperidinyl)-1-amino-ethane-1,1-diphosphonic acid;
2-(2'-(3'-methyl)-piperidinyl)-1-amino-ethane-l,l-diphosphonic acid; 2-(2'-piperidinyl)-1-hydroxy-propane-l,l-diphosphonic acid; 3-(2'-piperidinyl)-propionic acid-2,2-diphosphonic acid; 2 -(2'-piperidinyl)-1-(N-methyl)amino-ethane-l,l-diphosphonic acid; 4-(2'-piperidinyl)-1-hydroxy-butane-1,1-diphosphonic acid; 2 -(2'-(5'-amino)-piperidinyl)-1-hydroxy-ethane-l,l-diphosphonic acid; 2-(2'-(3'-ethyl)-piperi-dinyl)-l-hydroxy-ethane-l,l-diphosphonic acid; 2-(2'-(3'-carboxy)-piperidinyl)-l-hydroxy-ethane-l,l-diphosphonic acid; (2-(2'-(5'-carboxy) -piperidinyl ) -l-hydroxy-ethane-l, l-diphosphonic acid; 2-(2'-(1',4'-diazinyl))-ethane-1,1-diphosphonic acid;
2-(2'-(1',4'-diazinyl))-1-hydroxy-ethane-1,1-d~phosphonic acid; 2-(2'-(1',3'-diazinyl))-ethane-1,1-diphosphonic acid;
2-(3'-(1',2'-diazinyl))-ethane-1,1-diphosphonic acid;
N-(2'-piperidinylidene)-amino-methane diphosphonic acid;
N-(3'-piperidinyl)-amirc . ! - diphosphonic acid;
N-(4'-piperidinyl)-ami : i'- -- diphosphonic acid;
N-(2'-(3'-methyl)-piperidinylidene)-amino-methane diphosphonic acid; N-(2'-(5'-methyl)-piperidinylidene)-amino-methane diphosphonic acid; 2 -(N-(2'-piperidinylidene)-amino)-ethane-1,1-diphosphonic aci d; 1- (N- (2 ' -pi peridi nyl i dene) -amino)-ethane-l,l-diphosphonic acid; N-(2'-(1',3'-diazinyl-idene))-aminomethane d~ :~osphonic acid;

~1099~8~ 16 ~ .
.
N-(2'(1',4'-diazinylidene))-aminomethane diphosphonic acid;
N-(2'-(1',3',5'-triazinylidene))-aminomethane d~phosphonic acid; N-(4'-(1',2'-diazinyl))-aminomethane diphosphonic acid; 0-(3'piperidinyl)-oxamethane diphosphonic acid;
0-(4'-piperidinyl)-oxamethane diphosphonic acid; 2 -(0-(3'-piperidinyl)-oxa)-ethane-1,1-diphosphonic acid; 1 -(0-(3'-piperidinyl)-oxa)-ethane-1,1-diphosphonic acid;
0-(4'-(1',2'-diazinyl))-oxamethane diphosphonic acid;
S-(3'-piperidinyl)-thiomethane diphosphonic acid;
S-(4'-piperidinyl)-thiomethane diphosphonic acid; 2 -(S-(3'-piperidinyl)-thio)-ethane-1,1-diphosphonic acid;
1-(S-(3'-piperidinyl)-thio)-ethane-1,1-diphosphonic acid;
S-(4'-(1',2'-diazinyl))-thiomethane diphosphonic acid;
N-(2-pyridyl)-aminomethane diphosphonic acid; N-(2-(5-amino)-pyridyl)-aminomethane diphosphonic acid; N-(2-(5-chloro)-pyridy~)-aminomethane diphosphonic acid; N-(2-(5-nitro)-pyridyl)-aminomethane diphosphonic acid; N-(2-(3,5-dichloro)-pyridyl)-aminomethane diphosphonic acid; N-(4-pyridyl)-N-ethyl-aminomethane diphosphonic acid; N-(2-(3-picolyl))-aminomethane diphosphonic acid; N-(Z-(4-picolyl))-aminomethane diphosphonic acid; N-(2-(5-picolyl))-aminomethane diphosphonic acid; N-(2-(6-picolyl))-aminomethane diphosphonic acid; N-(2-(3,4-lutidlne))-aminomethane diphosphonic acid; N-(2-(4,6-lutidine))-aminomethane diphosphonic acid; N-(2-pyrimidyl)-aminomethane diphosphonic acid; N-(4-(2;6-dimethyl )-pyrimidyl ) -aminomethane diphosphonic acid;
N-(2(4,6-dihydroxy)-pyrimidyl)-aminomethane diphosphonic acid; N-(2-(5-methoxy)-pyridyl)-aminomethane diphosphonic acid; N-(2-pyridyl)-2-aminoethane-1,1-diphosphonic acid;
N-(2-(3-picolyl))-2-aminoethane-1,1-diPhosPhoniC acid;
N-(3-pyridyl)-2-amino-1-chloroethane-1,1-diphosphonic acid;
N-(3-pyridyl)-2-amino-1-chloroethane-1,1-diphosphonic acid;
N-(2-(4-picolyl))-2-amino-1-hydroxy-ethane-1,1-diphosphonic acid; (3-pyridyl)-aminomethane d~phosphonic acid; 2 -(2-pyridyl)-1-amino-ethane-1,1-diPhosphonic acid;

wo 92/213ss Pcr/usg2/o3sgs 0-(4-pyrldyl)-1-am~no-2-oxa-ethane-1,1-diphosphonic acid;
N-(phenyl)thiocarbamoylmethane diphosphonic acid; N-(4-chlorophenyl)carbamoylmethane diphosphonic acid; N-(4-chlorophenyl)thiocarbamoylmethane diphosphonic acid; N-(2-benzoyltb]thienyl)thiocarbamoylmethane diphosphonic acid);
N-(4-trifluoromethylphenyl)thiocarbamoylmethane diphos-phonic acid); N-(3-trifluoromethylphenyl)thiocarba-moylmethane diphosphonic acid);
N-(4-chloro-3-trifluoromethylphenyl)thiocarbamoylmethane diphosphonic acid); (4-chlorophenyl)sulfonylaminomethane 0 diphosphonic acid); and N-(3-mesylaminophenyl)thio-carbamoylmethane diphosphonic acid). Bone-actiYe drug C ,-' Js which are more preferred still in compositions of the present invention include pharmaceutically-acceptable salts of the following compounds or esters thereof:
6-amino-1-hydroxy-hexane-1,1-diphosphonic acid, 3-amino-1-hydroxy-propane-1,1-diphosphonic acid, octahydro-l-pyridine-6,6-diphosphonic acid, 2-(2'-piperi-dinyl)-ethane-l,l-diphosphonic acid; 2 -(3'-piperidinyl )-ethane-l,l-diphosphonic acid; 2 -(2'-piperidinyl)-1-hydroxy-ethane-1,1-diphosphonic acid;
2-(3'-piperidinyl)-1-hydroxy-ethane-1,1-diphosphonic acid;
N-(2'-(3'-methyl)-piperidinylidene)-amino-methane diphos-phonic acid; N-(2'-(1',3'-diazinylidene))-aminomethane diphosphonic acid; and N-(2-(3-methylpiperidinylidene))-aminomethane-1,1-diphosphonic acid. Other IJf~r.. ~e~i bone actiYe drug compounds for use in the compositions of the present inYention include the Fl:c~ hyl phosphinic acid compounds which are analo-gous to the above diphosphonic acid compounds.
As used herein, a "pharmaceutically-acceptable salt of an amine-functional compound~ means a salt of addition of the compound having similar pharmacological activity (effi-cacy and safety) to the base form of the compound. Prefer-ably a salt of addition of a compound has substantially the same pharmacological activity as the base form of the , Wo 92/2135S PCr/USs2/03995 - 2~0~95~ 18 compound. A salt of addition of a compound can be formed by the association of an amine-functional drug compound in 1ts base form with an appropriate acid. Acids known to form pharmaceutically-acceptable salts of addition with base forms of certain amine-functional drug compounds include, but are not limited to, the following: hydrochlo-ric, hydl ~LI ~ ic, hydriodic, maleic, succinic, tartaric, fumaric, lactic, citric, ascorbic, oxal ic, gluconic, phos-phoric, nitric, sulfuric, methane sulfonic, ethane sulfonic and 2-naphthalene sulfonic~
stroqen Estrogen therapy can be used along with any of these regimens. The method herein also comprises coadministering from about 0.3 mg to about 6 mg of estrogen along with the calcium and trace minerals and vitamin D, calcitonin or editronate (or diphosphonates). Preferably from 0.625 mg to about 1.25 mg of estrogen is taken daily. Any viable estrogen hormone replacement can be used.
Calcium Trace Mineral ComDonent In supplements of the type disclosed herein, the nutritionally supplemental amount for the minerals will generally comprise more than 50% of the RDA and preferably 80X-100% RDA, most preferably 100% of the RDA, per unit portion of the finished supplement. Of course, it is recognized that the preferred daily intake of any mineral may vary with the user.
In general, the RDA (calcium) will range from 360 mg per 6 Kg for infants to 800 mg/54-58 Kg female, depending somewhat on age. Moreover, it can be difficult to supple-ment beverages w~th more than 20-30X RDA of calcium (based per serving) without encountering precipitation and/or organoleptic problems. However, this level of supplementa-tion is equivalent to cow's milk in calcium value, and is therefore acceptable.
The r~- ~2~' dietary allowance for zinc is 15 milligrams (mg) per day for males and 12 mg per day for -21099~8 females. There is no specific RDA for -~e and cop-per. A safe and adequate range has been established as 2 to 5 mg for manganese and for copper, the range is 1.5 mg to 3 mg per day.
Any soluble salt of the trace minerals can be used, for example, zinc chloride, zinc sulfate, _r., so sulfate, manganese gluconate, copper sulfate and copper gluconate are useful. A nutritionally supplemental amount of these minerals is used. However, the particular salt used and the level will depend upon their interaction with other supplement ingredients.
Inorganic anions which are useful for making the trace mineral salts are sulfate, nitrate, phosphate, hydrogen phosphate and carbonate. Organic anions include carboxylate anions, e.g. citrate, malate tartrate, acetate and glyconate.
It is essential to this supplementation that the calcium salts be soluble in the stomach. This solubilization aids in making the calcium more readily bioavailable. It is equally important that the trace minerals be solubilized and absorbed by the stomach and or intestine. Therefore the choice of calcium and mineral salts depends upon the interaction of the salts in acid (stomach pH) solutions or basic (intestinal pH) solutions.
Solubility also plays an important role in the prepa-ration of foods and beverages containing these supplements.
Calcium Citrate Malate ComDositions:
The methods of this inven~ion involve administration of a mixture of calcium salts, herein "calcium citrate malate,~ comprising calcium salts of citric acid and malic acid. The calcium citrate malate may consist of a mi%ture of calcium citrate and calcium malate, a complex of calcium containing citrate and malate ligands, a mixture of a calcium salt with citric acid and malic acid, or combina-tions thereof. Mixtures of a calcium salts and citric and malic acids may be used to form calcium citrate malate in WO 92/21355 PCr/US92/03995 ~o~ss 20 situ, the beverage. Preferred are cal~ium citrate malate mixtures made by adding calcium carbonate, calcium hydroxide or other suitable source to a mixture of citric and malic acids.
The molar ratio of citrate:malate is from about 1:0.16 to about 1:13.5, preferably from about 1:0.5 to about 1:4.5, more preferably from about 1:0.75 to about 1:3. The ratlo of moles calcium:total moles citrate:total moles of malate is from about 2:1:1 to about 8:2:1, preferably from about 4:2:3 to about 6:3:4. The calcium citrate malate may contain other acid anions in addition to citrate and malate. Such anions may include, for example, carbonate, hydroxide, phosphate and mixtures thereof depending on the cal ci um source .
Preferably, the calcium citrate malate is neutral, comprised entirely of cltrate and malate anions. Thus, preferably, the equivalents of calcium (2 X moles calcium) is about equal to the total number of equivalents of citrate (3 X moles citrate) plus malate (2 X moles malate).
A preferred calcium citrate malate has a calci-um:citrate:malate molar composition of about 6:2:3 and 4:2:3.
The calcium cltrate malate used in the methods of this ~nvention may be provided in solid or liquid forms. Calcium citrate malate for use in solid forms may be made, for e%ample, by first dissolving citric acid and malic~ acid, in the desired molar ratio, in water. Calcium carbonate may then be added to the solution, ~n such amount that the ratio of moles calcium to moles citrate and moles malate is as desired. Carbon dioxide will be evolved. The solution may then be dried (as by freeze drying or oven drying at temperatures below 100C) to obtain the calcium citrate malate. Methods for making calcium citrate malate are described in the following documents: Japanese Patent Specification SH0 56-97248, Kawai, published August 5, 1981; and in U. S. 4,722,847 issued to Heckert (1988).
Co-pending application of Fox et al, Serial Number 07/537313 (i ~ee page 32 for I ' l~r~t~ nulliber) W092/2135s filed June 14, 1990; Japanese Patent Specification SHO 56 -97248, Kawai, published August 5, 1981; and in U.S.
4,722,847 issued to Heckert (1988).
Calcium carbonate can be used as the calcium source.
Other sources include calcium oxide and calcium hydroxide.
Calcium chloride, calcium phosphate and calcium sulphate are suitable for use herein, but they can form an acid solution which could adversely affect the flaYor of bever-ages and water solutions of the calcium citrate malate.
A solid forms during the mixing of the calcium oxide 0 or calcium hydroxide with the citric and malic acid. When these materials are used, it is necessary to mix the solu-tion until all of the calcium appears to have dissolved.
The calcium citrate malate ligand will precipitate when its solubility is exceeded.
The preferred method of preparation is to prepare a highly ~ ted solution of the calcium citrate malate which quickly and efficiently forces metastable calcium citrate malate out of solution. C~ tions of from 20X
to 75% are preferred. Preferably the concentration is from 40X to 65%.
The reaction t~ can be ambient (20C) or higher. Preferably the t -:~L~ of the reaction is in the range of 30C to 80C. Most preferably it is from 40C
to 60C.
Flavor ComDonent The flavor component of the present invention contains flavors selected from natural flavors, botanical flavors and mixtures thereof. The term ~fruit flavors" refers to those flavors derived from the edible reproductive part of a seed plant, especially one having a sweet pulp associated with the seed. Also included within the term ~fruit fla-vor" are synthetically prepared flavors made to simulate fruit flavors derived from natural sources.
The term rbotanical flavor" refers to flavors derived from parts of a plant other than the fruit; i.e. derived 9~8 22 from bean, nuts, bark, roots and leaves. Also included within the term "botan1cal flavor" are synthet~cally pre-pared flavors made to simulate botanical flavors derived from natural sources. Examples of such flavors include cocoa, chocolate, vanilla, coffee, kola, tea, and the 1ike.
Botanical flavors can be derived from natural sources such as essential oils and extracts, or can be synthetically prepared .
The part~cular amount of the flavor component effec-tive for imparting flavor characteristics to the supple-0 ments and food or beverage mixes of the present invention (nflavor enhancing") can depend upon the flavor(s) select-ed, the flavor impression desired, and the form of the flavor component. The flavor component can comprise at least 0.05% by weight of the beverage composition and preferably from 0.05% to about 10%. The amount of flavor added to the food, beverage or supplement ~s within the skill of one in the art and depends on the flavor intensity desi red .
For chocolate or cocoa, the amount of flavor added is from about 0.05% to about 20SL. Lower levels of artificial or synthetic chocolate flavors are used than for cocoa i tsel f .
Beverages can be flavored with fruit or other botani-cal flavors, e.g., vanilla, s~r ' .~', cherry, pineapple, banana, and mixtures thereof.
The calcium, c~tric and malic acids can be added wlth the trace minerals and vitamin D to a lOOX fruit juice or a dlluted fruit juice. The sugars present in the juice are useful sweeteners, and the juice can be the flavor compo-nent. Such beverages can contain from 5X to lOOX juice.
Preferably dilute juice beverages will have from 10% to 40X
~uice. Preferred juices for 100~'. juice products or diluted products are orange, cranberry, apple, pear, grape, rasp-berry, lemon, grapefruit, pineapple, banana, blackberry, blueberry and passion fruit juices and mixtures thereof.
_ _ _ Wo 92~2135~ P~ S92/03995 23 ~ ~ 2~1~99~
Sweetener COmDOnent The sweetener composition is usually a --rr~rjde or a disaccharide. These include sucrose, fructose, dex-trose, maltose and lactose. Other ca~uù~ aLes can be used if less sweetness is desired. Mixtures of these 5sugars can be used.
In addition to sugar of the present invention can contain other natural or artificial sweeteners. Other suitable sweeteners include saccharin, cyclamates, acetosulfam, L-aspartyl-L-phenylalanine lower alkyl ester sweeteners (e.g. aspartame), L-aspartyl-D-alanine amides disclosed in U.S. Patent 4,411,925 to Brennan et al., issued October 23, 1983, L-aspartyl-D-serine amides dis-closed in U.S. Patent 4,399,163 at Brennan et al., issued August 16, 1983, L-aspartyl-L-1-1,~d,u~. Ll~l- alkaneamide sweeteners d i scl osed i n U . S . Patent 4, 338, 346 to Brand, issued December 21, 1982, L-aspartyl-1 hyd1uxJ_Lhyl-alkaneamide sweeteners disclosed in U.S. Patent 4,423,û29 to Rizzi, issued December 27, 1983, L-aspartyl-D-phenylglycine ester and amide sweeteners disclosed in European Patent Application 168,112 to J. M. ~anusz, pub-lished January 15, 1986, and the like. A particularly ~, erc., cd sweetener is aspartame.
The amount of the sweetener effective in the fûod, beverage, mixes or supplements of the invention depends upon the particular sweetener used and the sweetness inten-sity desired. For noncaloric sweeteners, this amount varies depending upon the sweetness intensity of the par-ticular sweetener. For sugar (i.e., sucrose), this amount can be from 10% to 85X (typically from 55% to 70XJ by 3C weight. In determining the amount of sugar, any sugar or other sweetener present in the flavor componen~ is also included. Low-calorie sweetener combinations containing a noncaloric sweetener such as aspartame and a sugar, such as corn syrup solids, or sugar alcohols can also be used in :

24 ~ 5 8 beverage mixes. In general, the amount of sweetener will be from about 0.5% to about 85%.
Other Inqredients Other minor ingredients are frequently included in supplements, foods and beverages. Such ingredients include preservatives such as ben~oic acid and salts thereof, sulfur dioxide, butylated hydroxyanisole, butylated hydroxytoluene, etc. Also, typically included are colors derived either from natural sources or synthetically pre-pared .
Salt, e.g. sodium chloride, and other flavor enhancers can be used to improve the flavor of the food, beverage or suppl ement .
Emulsifiers can also be included. Any food grade emulsifier can be used. Lecithin is a preferred emulsifi-er. Other edfble emulsifiers include mono- and diglycerides ~f long chain fatty acids, preferably saturat-ed fatty acids, and most preferably, stearic and palmitic acid mono- and diglycerides. Propylene glycol esters are also useful in beverage mixes.
Fats or oils can also be added to supplements or foods to make them more palatable.
~H and Other BeYeraqe In~redients The pH of the beverages and beverage ccncentrates of the present invention is dep~nd~,t upon the weight ratios of the acids, the total amount of acids and the sourness impression desired. Typically, the pH can range from 2.5 to 6.5. Preferred carbonated beverages have a pH of from 3.0 to 4.5.
Other minor beverage ingredients are frequently in-cluded in beverages and concentrates. Also, typically included are colors derived either from natural sources or synthetically prepared. See L. F. Green, Develo~ments in Soft Drinks Technoloqy, Vol. 1 (Applied Science Publishers Ltd. 1978), pp. 185-186 for preservatives and colors used in beverages , 25 2 ~ 5 8 Beveraqe Pre~aration The beYerages and concentrates of the present inven-tion can be prepared by standard beverage formulation techniques. It should be understood, however, that carbon-ated beverage making techniques, when appropriately modi-fied, are also applicable to noncarbonated beverages.
Also, while the following description is with referen~e to sugar containing beverages, diet beverages containing noncaloric sweeteners can also be prepared by appropriate modification. 8everages can include dry beverage mixes which are made by mixing flavors, sweeteners, and other optional ingredients as well as fruit juices and dilute fruit juices.
In making a sugar sweetened carbonated beverage, a beverage concentrate is usually formed containing from 30 to 70% by weight water. This beverage concentrate typical-ly contains the emulsified or water-soluble flavors, emul-sion stabilizing agents, and weighting agents if needed, any color desired and suitable preserYatives. After the concentrate is formed, sugar and water are then added to make a beverage syrup. This beverage syrup is then mixed with an appropriate quantity of water to form the finished beverage. The weight ratio of water:syrup is from about 3:1 (3x syrup) to about 5:1 (5x syrup). To make a carbon-ated beverage carbon dioxide can be introduced either into the water mixed with the beverage syrup or into the drink-able diluted beverage to achieve carbonation. The beverage can be sealed in a container such as a bottle or can. See L.F. Green, DeveloDments in Soft Drinks Technoloqv, Vol. 1, (Applied Science Publishers Ltd. 1978), pp. 10Z-107 for a further description of beverage making. in particular the process for carbonation.
The amount of carbon dioxide in the beverage depends upon the particular flavor system used and the amount of carbonation desired. Usually, carbonated beverages of the present invention contain from 1.0 to 4.5 volumes of carbon WO 92/21355 . PCI/US92103995 ~9~8 26 dioxide. Preferred carbonated beverages contain from 2 to 3.5 volumes of carbon dioxide.
The calcium source and the acids (citric, malic, phosphoric) can be added at various points in these pro-cesses. The calcium source and acids are preferably added at the same point in this process, but can also be added at different points. Usually, the calcium source and acids are included during preparation of the beverage ~ Lrdte or beverage syrup. Preferably the trace minerals are added after the calcium and acid source have been mixed in.
Vitamin D can be added with the oil flavors or weighting oil .
When making a dry beverage, it is preferred to mi% a powdered calcium citrate malate powder and trace mineral salts with the sugar or artificial sweeteners, vitamin D
and flavors. Colors and colored coated sugars can be added. Dry chocolate milk beverages are preferred dry beverage mixes. These can be diluted either with water or milk. Milk provides additional vitamin D and calcium citrate. A typical formula for chocolate mixes is:
a) from OX to 25% milk solids, preferably from 5X to 20X non-fat milk solids;
b) from 0.05% to 20X flavor, preferably cocoa;
c) from about 0.5 to about 85X sweetener, preferably sucrose; and d) from aDout 0.6% to about 0.15X calcium citrate malate and from about 0.60 to about 30 micrograms vitamin D.
SUDD1 ement Form~
Solid forms include tablets, capsules, granules and bulk powders. Tablets may contain suitable binders, lubri-cants, diluents, disintegrating agents, coloring agents, flavoring agents, flow-inducing agents and melting agents.
Liquid oral dosage forms include aqueous solutions, emul-sions, suspensions, solut~ons and/or suspensions reconsti-~u e~ 'om non-err~,~es....t gr~nules ~nd ~rr.,l~s~...L

WO 92/2135!i PCI/US92/03995 27 2~1099~j8 preparations reconstituted from err~ csc...t granules.
Such liquid oral dosage forms may contain, for example, suitable solvents, preservatives, emulsifying agents, suspending agents, diluents, sweeteners, melting agents, and coloring and flavoring agents. A preferred liquid dosage form contains calcium citrate malate and the trace minerals in a juice-containing beverage or other beverage.
The trace minerals, calcium citrate malate, vitamin D
and/or and drug therapy can be coadministered in one tab-let, liquid, food or beverage or they can be administered 0 separately. A capsule containing the trace mineral salts, a second tablet with the calcium citrate malate and a third containing vitamin D and/or drug therapy are easy to formu-late and to swallow. A mineral and vitamin D supplement could also be coadministered with a calcium beverage.
1s Specific examples of i,i,a""~.c~lically acceptable carriers and excipients that may be used to formulate oral dosage forms of the present invention are described in U.
S. Patent 3,903,297, Robert, issued September 2, 1975 Techniques and compositions for making dosage forms useful in the methods of this invention are described in the following ~cr~.e -; 7 Modern Pharmaceutics, Chapters 9 and 10 (Banker ~ Rhodes, Editors, 1979); Lieberman et al., Ph~""dce..lical Dosaqe Forms: Tablets (1981); and Anse~, Introduction to Pharmaceutical Dosaqe Forms 2nd Edition.
(1976).
Method of Buildinq Bone Various oral dosage forms of calcium citrate malate, trace minerals, v~tamin D and/or drug therapies may be used in the present invention. Such dosage forms comprise a safe and effective amount of calcium citrate malate, trace minerals, vitamin D and/or drug therapies and a pharmaceu-tically acceptable carrier. Preferably the pharmaceutical-ly acceptable carrier is present at a level of from about 0.1% to about 99Z, preferably from about O.lX to about 75X, by weight of the composition. Unit dosage forms (i.e., Wo 92/21355 Pcr/uS92/03995 ~ 8 dosage forms containing an amount of calcium citrate malate suitable for administration in one single dose, according to sound medical practice) preferably contain from about 100 mg to about 1000 mgr preferably from about 100 mg to about 500 mg, more preferably from about 200 mg to about 300 mg of calcium (on an elemental basis). Unit dosage forms of copper (on an elemental basis) contain 0.5 to 5 mg, preferably 0.5 to 4.0 mg, of manganese (on an elemental basis) contain I to 8 mg and preferably from 2 mg to 7 mg, and of zinc (on an elemental basis) contain 1.5 to 30 mg and preferably 7.5 to 20 mg zinc.
Preferably, from about 175 milligrams to about 2000 milligrams of calcium (as elemental calcium) are adminis-tered to said subject, per day. More preferably, from about 250 milligrams to about 1500 milligrams, most prefer-lS ably from about 350 milligrams to about 1000 milligrams, of calcium are administered, per day. The specific amount of calcium citrate malate to be administered depends upon the relative percentage weight of calcium in the particular calcium citrate malate employed.
The rur '-~i daily allowance for vitamin D is 200-400 IU ~iepending on age of the subject. The supple-ments used herein have a unit dosage amount of from about 2S IU to about 1000 IU or from about 0.6 to 25 micrograms.
The effective amount of calcitonin is about 100 IU per day. From about 25 IU to 120 IU can be administered with the calcium citrate malate, trace minerals and vitamin D.
The effective amount of diphosponate is from about 200 mg to about 1000 mg. The usual safe and effective amount of 3idronel and the di,~ tes is from I mg/kg/day to 20 mg/kg/day. Preferably from 5 to 10 mg/kg/day are used.
This dose can be administered in 2 dosage units, one in the morning and 1 in the evening. Didronel and the bi ~p~c ~h ~tes for treatment of age-related bone loss are typlcally administered in an intermittent cyclical fashion.

WO 92/21355 ~CI/US92/03995 29 21~9~8 , Specifically, the present inYention provides a method for building bone in a human or other animal subject, comprising administering to said subject a safe and effec-tive amount of calcium citrate malate, and copper, zinc and - and vitamin D and/or either calcitonin, editronate or estrogen for a period of time sufficient to achieve an increase in the net skeletal mass of said sub-ject. As used herein, rbuilding bone" refers to a decrease in the net skeletal loss of bone of the subject treated and therefore a net skeletal increase in mass. The slowing of the rate of bone loss and the increase in growth rate occur simultaneously so the net bone density may stay the same.
The increase in mass may be at any skeletal site, including spine, hip, long bones of arms or legs or in the whole skeleton. Preferably, the net skeletal mass is increased by at least about 0.1%, more preferably at least about 1%.
The loss of bone is cumulative over a long period of time. Typically, lifetime loss in bone mass is about 35%
in males and 50X in females. Thus, even though a net skeletal increase of as little as 0.5X in one year is not particularly critical, over 10 years this results in 5X
more bone mass than would be present if bone loss continued at lts usual rate.
"Administering~ refers to any method which, in sound medical practice, delivers the vitamin D and/or drug, calcium citrate malate and trace minerals used in this invention to the subject ~o be treated in such a manner so as to be effective in the building of bone.
The specific period of time sufficient to achieve an increase in the net skeletal mass of the subject may depend on a variety of factors. Such factors include, for exam-ple, the specific mineral formulation employed, the amount of minerals administered, the age and sex of the subject, the specific disorder to be treated, concomitant therapies employed (if any), the general physical health of the subject (including the presence of other disorders), the wo 92r2l3ss PCI/US92/03995 21~99~8 extent of bone loss in the individual, and the nutritional habits of the individual. Although the administration of even small quant~ties of calcium citrate malate, trace m1nerals, vitamin D and/or drug therapy may build bone, the net increase in bone mass may not be detectable for short S peri ods of admi ni strati on .
For the treatment of age-related bone loss, the calci-um citrate malate, trace minerals and vitamin D, and~or calcitonin or bi~l ' ~rh~ ~tes or estrogen are administered according to sound medical practice for at least about six months, preferably for at least about twelYe months. Of course, such administration may be continued indefinitely, according to sound medical practice.
The ~ethods of this invention may be employed in the treatment of any of a variety of disorders in which the building of bone is desired. Thus, preferably, the human or other animal ~subject" of the methods of this invention is ~in need" of a method for building bone, i.e., the subject has a disorder for which building of bone or de-crease in rate of bone resorption would be advantageous according to sound medical practice. Such disorders ln-clude, for example, bone fractures, reduced bone mass and disorders typified by bone loss, such as age-related bone loss and osteoporosis (both primary and secondary for~s).
A preferred method of this invention is for the treat-ment of age-related bone loss.
The following example illustrates compositions of the type provided by the practice of this invention, but is not intended to be limiting thereof.
ExamDl e I
Several post . ~7~al women are treated by adminis-tering a composition containing calcium citrate malate having a molar calcium:citrate:malate composition of about 6:2:3. The calcium citrate malate is made by first dis-solving approximately 384.2 grams of c~tric acid and ap-proximately 402.3 grams of malic acid in cu~\u~ tely 2 . . _ _ , . _ , . , =

WO 92/213SS Pcr/US92/0399S
31 21~9958 liters of water. This citrate/malate solution is then heated to approximately 55C (131F), with stirring.
Separately, approximately 600.6 grams of calcium carbonate is added to approximately 1.2 liters of water, forming a slurry, with stirring.
The citrate/malate solution is then removed from its heat source, and the calcium carbonate slurry is added slowly, with stirring. The rate of addition is controlled, to contain the reaction as carbon dioxide is released. An additional quantity of water, app~uAi,,,a~ely 0.4 liters, is finally added. The reaction mixture is then stirred for a,u~,.ùAil,,d~ely I to 1.5 hours. The reaction is essentially complete as the pH of the solution equilibrates to approxi-mately 4.3.
A precipitate of calcium citrate malate is thus formed. The excess reaction liquid is filtered off. Th~
calcium citrate malate is dried, for a~.uAil,,ltely 12 ho~rs at au",~Ai",<l~ely 105C (221F), reducing the moisture level to less than about IX. The dried product is then milled to ~lj.UAilll4tely 1û-20 mesh size, for a swallowable tablet formulation. Each tablet contains 25û mg.
The swallowable tablet dosage form is then made, comprising:
ComDonent % (Bv Weiqht) Calcium citrate malate* 99.73 Magnesium stearate 0.27 ~Having a molar calcium:citrate:malate composition of au~luAilllcltely 6:2:3, made as described aboYe in this exam-ple.
The tablet formulation is made by thoroughly admixing 3û the powders, and tabletting using a standard tablet press, to form tablets weighing a,u~"ùximdtely 1104 milligrams.
The tablets are then coated, using a pan coater. The coating solution contains approximately 11%
I,JJ,uA.~u..rylmethyl cellulûse, app~uAin~ately 2X

WO 92/21355 ~ PCI/US92/03995 polyethylene glycol, approximately 3.5X colorant, and the balance of water.
A capsule containing 15 mg zinc (from zinc sulfate), 5 mg manganese (from, - -se gluconate) and 2.5 mg copper (from copper gluconate) and 10 micrograms of vitami~ D is also administered to each patient.
ExamDle Ir A powdered mineral supplement comprising 2000 gm of calcium citrate malate, 6.3 mg of copper sulfate (2.5 mg copper), 31.3 mg of zinc chloride (15 mg zinc) and 5 mg of 10 manganese (15.4 mg of ,._.. , e~c sulfate I '~d~ale) is prepared by tabletting the mixture of powders. This tablet is taken in a daily regimin with 2 mg/kg of Didronel for 6 months .
ExamDle III
A tablet containing 200 mg calcium (from calcium citrate malate), 1 mg copper (from copper gluconate), 1.5 mg manganese (from manganese gluconate), 3 mg zinc (from zinc gluconate), and 3 micrograms vitamin D (from cholecalciferol) is taken 4 times daily along with a single tabletted dose of 0.625 mg conjugated estrogen taking once da~ly for 2 years.
(* r. 11rs~ Dumbers:) 07/562,773 publiE~hed 20 February 1992 as ~092-02235 25 808,584 published 29 July 1987 as EP 0,230,068 945,069 published 06 July 1988 as 1~ 0,273,514 945,068 published 13 ~uly 1988 as EP 0,274,158 069,666 published 11 Jaluary 1989 as ~P 0,298,553 07/573,313 published 26 December 1991 as ~091-19692

Claims

CLAIMS:

1. A mineral and vitamin supplement for building bones comprising a unit dosage mixture of:
a) from 100 to 1000 mg of calcium (on an elemental basis) in the form of a carboxylate selected from the group consisting of citrate, malate, lactate and mixtures thereof;
b) from 0.5 to 5 mg of copper (on an elemental basis);
c) from 1.5 to 30 mg of zinc (on an elemental basis);
d) from 1 to 8 mg of manganese (on an elemental basis); and e) from 0.6 to 25 micrograms of vitamin D.

2. A supplement according to Claim 1 wherein vitamin D is present at 0.15 to 5 micrograms per supplement and is in the form of vitamin D metabolites and precursors such as 1A25-(OH)2 vitamin D, 25 OH vitamin, 1AOH vitamin D2 or D3 and/or analogues of the dihydroxy compound.

3. A supplement according to Claim 2 wherein the molar ratio of calcium:citrate:malate is from 2:1:1 to 8:2:1.

4. A supplement according to Claim 3 wherein the molar ratio of calcium:citrate:malate is from 4:2:3 to 6:3:4.

5. A supplement according to Claim 2 wherein said copper, zinc and manganese are salts of anions selected from the group consisting of chloride, sulfate, gluconate, citrate, malate, lactate, tartrate, nitrate, and mixtures thereof.

6. A supplement according to Claim 5 wherein said anions are selected from the group consisting of chloride, gluconate, malate and citrate.

7. A supplement for building bones comprising a unit dosage mixture of:
a) from 100 to 1000 mg of calcium (on an elemental basis) in the form of a carboxylate selected from the group consisting of citrate, malate, lactate and mixtures thereof;
b) from 0.5 to 5 mg of copper (on an elemental basis);
c) from 1.5 to 30 mg of zinc (on an elemental basis);
d) from 1 to 8 mg of manganese (on an elemental basis); and e) from 200 mg to 1000 mg of diphosphonate.

8. A supplement according to Claim 7 wherein said diphosphonate is Didronel.

9. A supplement according to Claim 7 wherein said diphosphonate is an aminodiphosphonate.