Drug – bio-affecting and body treating compositions – Designated organic active ingredient containing – Peptide containing doai
Reexamination Certificate
1997-12-31
2003-04-01
Low, Christopher S. F. (Department: 1653)
Drug, bio-affecting and body treating compositions
Designated organic active ingredient containing
Peptide containing doai
C514S007600, C514S102000, C514S108000, C514S018700, C530S331000
Reexamination Certificate
active
06541454
ABSTRACT:
BACKGROUND OF THE INVENTION
Calcium-related disorders in general and osteoporosis in particular are a major public health problem in developed countries. Several important pathological conditions are calcium-related and involve irregularities in calcium metabolism: Paget's disease, osteoporosis, hypercalcemia of malignancy, and osteolysis front bone metastases, etc. Bisphosphonates are a relatively new family of drugs used clinically in various calcium-related disorders including tumor osteolysis, and are undergoing clinical trials for osteoporosis. They are poorly absorbed following oral administration probably due to their high polarity and charge. IV and IM administration is a serious obstacle to their wide-spread use.
In the patent of Bosies et al. (U.S. Pat. No. 4,666,895 May 19, 1987) peptidyl diphosphonic acid derivatives are described. Bosies et al. Patent hypothesize that some peptidyl compounds will have better activity on bone: “In particular, they can be used in cases where the formation and breakdown of bone is disturbed, for example in cases of osteoporosis”. Nothing is claimed, regarding the absorption of such compounds from the gastrointestinal tract following oral administration. The dosage recommended is much higher than that needed when effective oral absorption takes place. The dosage range recommended (see column 6) is from . . . “1 mg to 1000 mg, and preferably from 10 to 200 mg.” Such doses are typical for non-absorbable bisphosphonates such as etidronate and pamidronate. The daily oral recommended dose of a recently approved bisphosphonate in the US, alendronate (Fosamax) is 10 mg and 40 mg, in the treatment of osteoporosis and Paget's disease, respectively (American Hospital Formulary Service AHFS Drug Information, section 92:00, 1995). As is known widely, this drug is 100 to 1000 times more effective than etidronate, the drug chosen by Bosies et al, for comparison. Typical absorption of such bisphosphonates in humans is in the range of 1%. Effective hydrolysis of the prodrug to the parent drug, for e.g., pamidronate or alendronate, is achieved following oral administration in the cytosol (intestinal cells). It is clear that if a peptidyl derivative of such a drug is administered to humans the dose should be reduced by 50 to 100 times, in order not to be lethal, due to the enhanced absorption of about 50 to 100 times of the prodrug. Bosies relates only to subcutaneous injections, in comparison to a first generation bisphosphonate, etidronate. Furthermore, selection of the peptidyl derivatives is not based on recognition by the transporter system nor on the possibility for hydrolysis to the parent drug. In their patent they seed a new compound, the administered drug being the active drug at the site of action (bone). The present invention relates specifically to the activity of the parent drug yielded form the prodrug following oral absorption.
The results are described ambiguously (+ and −system), and the activity of the compounds is compared to first generation bisphosphonate, etidronate (a non-nitrogen containing compound) rather than a more appropriate comparison to nitrogen-containing drugs such as pamidronate, known to be more effective (pamidronate and alendronate, nitrogen containing bisphosphonates, in clinical use are 10 to 1000 times more effective than etidronate. To the best of our knowledge no further development (since 1987) nor a scientific report is available for such compounds claimed by Bosies et al.
Bisphosphonates
Bisphosphonates have been approved for clinical use in Paget's disease, tumor osteolysis, and hypercalcemia of malignancy and approved in some countries for osteoporosis therapy. Most bisphosphonates are disodium salts of tie tetraacids (M.W. approximately 250), and are poorly absorbed from the GI tract (approximately 1% of the oral dose is absorbed). Chronic IM or SC administration of bisphosphonates causes irritation and necrosis, and the oral route has been associated with GI disturbances, resulting in poor patient compliance and side effects. For example, the treatment protocol of pamidronate in tumor osteolyis is 1-day slow and diluted IV infusion to avoid thrombophlebitis, but treatment is repeated if normocalcemia is not attained. Another example is the chronic therapy (years) required in osteoporosis.
Absorption Barriers
Clinically, the oral route is the most common and accepted one for delivering drugs of a low molecular weight, of up to 400-600. However, the low permeability of the intestinal epithelia towards highly polar and charged molecules impedes the effective absorption of many low molecular weight drugs. Many such drugs must be delivered parenterally by frequent injections. This is highly risky without close medical supervision. The problem is particularly acute in cases of drugs used for treatment of various chronic diseases such as cancer and age-related diseases, such as osteoporosis, which require prolonged drug treatment.
New Drugs for Calcium-related Disorders
Drugs require a degree of lipophilicity to pass through the GI barrier. In order to increase oral absorption of drugs with low membrane permeability, nonpolar prodrugs are often utilized. Due to the wide variety of esterases present in the target tissue for oral prodrug-regeneration, esters are the most common prodrugs when GI absorption is considered. Acyloxymethyl esters of bisphosphonic acids were proposed however this did not lead to a useful drug (European Patent EP 0 416 689 A2, date of filing Aug. 29, 1990). Similarly, Fels et al. proposed pharmaceutical compositions comprising bisphosphonates and sodium lauryl sulfate for increased oral absorption (U.S. Pat. No. 4,980,171, Dec. 25, 1990).
One way to increase membrane permeability of drugs is by utilization of the peptide carrier system (G. L. Amidon et al.,
Absorption of difficult drug molecules: Carrier-mediated transport of peptides and peptide analogues,
Novel drug delivery and its therapeutic application, L. F. Prescott and W. S. Nimmo, Eds., John Wiley & Sons (1989) pp. 45-56).
SUMMARY OF INVENTION
The hypothesis of the present patent is completely different from the working hypothesis of Bosies et al. By carefully selecting specific di and/or tripeptide derivatives of bisphosphonates, enhanced oral bioavailability can be achieved due to the recognition by the active carrier transporter of the intestinal mucosae and the hydrolysis to the parent drug following oral administration.
Thus, the prodrug in our invention is a delivery system rather than a new compound for bone diseases. Therefore, the present selection of new compounds is based on enhanced absorption for the GI tract and hydrolysis to the parent compound resulting in improved oral, clinical treatment by a low dose. The selection of the di/tri-peptidyl moiety is based on transporter recognition and hydrolysis and not, as in Bosies et al patent, on resorbing activity on the bone.
Thus, the present invention relates to novel compounds of the general formula
wherein Z is
wherein Z
1
and Z
2
are independently a side chain of an amino acid or hydrogen,
wherein Z
4
is hydrogen or Z
4
and Z
1
together with —N—CH—CO represent a proline residue.
where Q is
where Z
3
is a bond or a spacer group selected from NH, CO, NHCO, NHCO(CH
2
)
q
—CO, (CH
2
)
r
CO where r is zero or an integer,
and where q is an integer or zero,
m is 2, 3 or 4,
n is greater than or equal to 0
X is —H or —OH,
Y is —H or —NR
2
R
3
,
where A designates a 5- or 6-membered heterocyclic ring which contains 1, 2 or 3 nitrogen atoms, zero, 1 or 2 oxygen atoms and which may contain a sulfur atom, which contains up to and including 3 double bonds, where R
2
and R
3
are independently hydrogen, lower alkyl, lower alkenyl, lower alkoxy, (di)alkylaminoalkyl, alkoxyalkyl and where the ring A may be substituted by one or more conventional substituents, and to pharmaceutical compositions of improved absorption from the gastro-intestinal tract which contain as active ingredient an efficient quantity of a compound defined above.
Preferred
Alferiev Ivan Sergeievitch
Amidon Gordon L.
Breuer Eli
Friedman-Ezra Aviva
Golomb Gershon
Eitan Pearl Latzer & Cohen-Zedek
Yissum Research Development Company of the Hebrew University Jer
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