Drug – bio-affecting and body treating compositions – Designated organic active ingredient containing – Having -c- – wherein x is chalcogen – bonded directly to...
Reexamination Certificate
1997-04-16
2003-09-30
Huang, Evelyn Mei (Department: 1625)
Drug, bio-affecting and body treating compositions
Designated organic active ingredient containing
Having -c-, wherein x is chalcogen, bonded directly to...
C514S308000, C514S309000, C546S140000, C546S141000, C546S146000, C546S147000, C546S149000
Reexamination Certificate
active
06627641
ABSTRACT:
TECHNICAL FIELD OF THE INVENTION
The present invention relates to naphthylisoquinoline alkaloids and derivatives thereof which exhibit in vitro and in vivo antimalarial activity, methods of obtaining useful antimalarial naphthylisoquinoline derivatives, pharmaceutical compositions containing such antimalarial compounds, and methods for using the compounds for the treatment or prevention of malaria. The compounds of the present invention exhibit advantageous pharmacological, toxicological, or antimalarial properties, such as for example, inhibiting in vitro and in vivo the viability, growth, reproduction, and pathological effects of Plasmodia parasites, including drug-resistant strains thereof, which are known to cause malaria.
BACKGROUND OF THE INVENTION
It is estimated that more than 2-3 million people die of malaria each year, and many more suffer from debilitating infection. Approximately a third of the world's population lives in malaria-endemic areas, including Central and South America, Asia, and Africa. Transient visitors or workers in these areas also are at ever-increasing risk of contracting malaria. Mosquitoes that carry malaria parasites have become resistant to insecticides, and the deadliest parasites have become resistant to previously effective antimalarial drugs such as chloroquine and other clinically used agents. New effective antimalarial chemotherapy agents are urgently needed. The present invention provides useful new antimalarial compounds and pharmaceutical compositions, as well as methods of using such antimalarial compounds and pharmaceutical compositions to prevent or treat malaria. These and other objects and advantages of the present invention, as well as additional inventive features, will be apparent from the description of the invention provided herein.
BRIEF SUMMARY OF THE INVENTION
The present invention is directed to useful antimalarial pharmaceutical compositions comprised of a suitable, pharmaceutically acceptable carrier and an antimalarial effective amount of at least one naphthylisoquinoline alkaloid selected from the group consisting of dioncophylline B, dioncopeltine A, dioncophylline A, dioncophylline C, dioncolactone A, N-methyl-dioncophylline A, ancistrobrevine D, ancistrocladine, michellamine A, michellamine B, N-methyl-dioncophylline A and atropisomer thereof, 5′-O-demethyl-8-O-methyl-7-epi-dioncophylline A, 4′-O-demethyl-dioncophylline A, dioncophylleine A, (±)-dioncophyllacine A, hamatine, ancistrobrevine B, ancistrobrevine A, 6-O-demethyl-ancistrobrevine A, ancistrobarterine A, 7-epi-dioncophylline A, N-formyl-ancistrocladine, N-methyl-ancistrocladine, 6-deoxy-N-methyl-ancistrocladine, N-formyl-O,O-dimethyl-dioncophylline C, N-formyl-dioncophylline C, N-formyl-8-O-benzyl-dioncophylline C, N-formyl-8-O-methyl-dioncophylline C, N-formyl-8-O-pivaloyl-dioncophylline C, N-formyl-8-O-acetyl-dioncophylline C, N-formyl-8-O-benzoyl-dioncophylline C, and 8-O-methyl-dioncophylline C, and derivatives thereof wherein one or more phenolic hydroxyl group(s) may instead be an ester, sulfonate ester, or ether group; one or more methyl ether group(s) may instead be a phenolic hydroxyl group; one or more phenolic hydroxyl group(s) may instead be an aromatic hydrogen substituent; one or more secondary amine site(s) may instead be an amide, sulfonamide, tertiary amine, or alkyl quaternary ammonium salt; one or more tertiary amine site(s) may instead be a secondary amine; and one or more aromatic hydrogen substituent(s) may instead be a halogen, nitro, amino, hydroxyl, thiol, or cyano substituent, or a pharmacologically acceptable salt thereof.
The present invention additionally includes a method of obtaining useful antimalarial compounds by applying one or more well-known chemical reactions to a naphthylisoquinoline alkaloid selected from the group consisting of dioncophylline B, dioncopeltine A, dioncophylline A, dioncophylline C, dioncolactone A, N-methyl-dioncophylline A, ancistrobrevine D, ancistrocladine, michellamine A, michellamine B, N-methyl-dioncophylline A and atropisomer thereof, 5′-O-demethyl-8-O-methyl-7-epi-dioncophylline A, 4′-O-demethyl-dioncophylline A, dioncophylleine A, (±)-dioncophyllacine A, hamatine, ancistrobrevine B, ancistrobrevine A, 6-O-demethyl-ancistrobrevine A, ancistrobarterine A, 7-epi-dioncophylline A, N-formyl-ancistrocladine, N-methyl-ancistrocladine, 6-deoxy-N-methyl-ancistrocladine, N-formyl-O,O-dimethyl-dioncophylline C, N-formyl-dioncophylline C, N-formyl-8-O-benzyl-dioncophylline C, N-formyl-8-O-methyl-dioncophylline C, N-formyl-8-O-pivaloyl-dioncophylline C, N-formyl-8-O-acetyl-dioncophylline C, N-formyl-8-O-benzoyl-dioncophylline C, and 8-O-methyl-dioncophylline C, to provide a naphthylisoquinoline derivative wherein one or more phenolic hydroxyl group(s) may instead be replaced by an ester, sulfonate ester, or ether group; one or more methyl ether group(s) may instead be replaced by a phenolic hydroxyl group; one or more phenolic hydroxyl group(s) may instead be replaced by an aromatic hydrogen substituent; one or more secondary amine site(s) may instead be replaced by an amide, sulfonamide, tertiary amine, or alkyl quaternary ammonium salt; one or more tertiary amine site(s) may instead be replaced by a secondary amine; and one or more aromatic hydrogen substituent(s) may instead be replaced by a halogen, nitro, amino, hydroxyl, thiol, or cyano substituent.
The present invention also encompasses a method of treating or preventing a malaria infection which comprises administering to a mammal in need thereof an antimalarial effective amount of at least one compound selected from the group, consisting of dioncophylline B, dioncopeltine A, dioncophylline A, dioncophylline C, dioncolactone A, N-methyl-dioncophylline A, ancistrobrevine D, ancistrocladine, michellamine A, michellamine B, N-methyl-dioncophylline A and atropisomer thereof, 5′-O-demethyl-8-O-methyl-7-epi-dioncophylline A, 4′-O-demethyl-dioncophylline A, dioncophylleine A, (±)-dioncophyllacine A, hamatine, ancistrobrevine B, ancistrobrevine A, 6-O-demethyl-ancistrobrevine A, ancistrobarterine A, 7-epi-dioncophylline A, N-formyl-ancistrocladine, N-methyl-ancistrocladine, 6-deoxy-N-methyl-ancistrocladine, N-formyl-O,O-dimethyl-dioncophylline C, N-formyl-dioncophylline C, N-formyl-8-O-benzyl-dioncophylline C, N-formyl-8-O-methyl-dioncophylline C, N-formyl-8-O-pivaloyl-dioncophylline C, N-formyl-8-O-acetyl-dioncophylline C, N-formyl-8-O-benzoyl-dioncophylline C, and 8-O-methyl-dioncophylline C, and derivatives thereof wherein one or more phenolic hydroxyl group(s) may instead be an ester, sulfonate ester, or ether group; one or more methyl ether group(s) may instead be a phenolic hydroxyl group; one or more phenolic hydroxyl group(s) may instead be an aromatic hydrogen substituent; one or more secondary amine site(s) may instead be an amide, sulfonamide, tertiary amine, or alkyl quaternary ammonium salt; one or more tertiary amine site(s) may instead be a secondary amine; and one or more aromatic hydrogen substituent(s) may instead be a halogen, nitro, amino, hydroxyl, thiol, or cyano substituent, or a pharmacologically acceptable salt thereof.
The treatment method of the present invention may also involve co-administering an antimalarial effective amount of chloroquine or other antimalarial agent(s), such as mefloquine, halofantrine, artemisinin, artemether, or quinine, with at least one compound, or pharmacologically acceptable salt thereof, selected from the aforementioned antimalarial naphthylisoquinoline alkaloids or derivatives.
DESCRIPTION OF THE PREFERRED EMBODIMENTS
The present invention is predicated on the discovery that certain naphthylisoquinoline alkaloids and derivatives thereof, preferably in substantially pure form, have in vitro and in vivo antimalarial activity, and therefore are useful for antimalarial treatments. Many of these naphthylisoquinoline compounds have chemical formulae, or are derivatives thereof, which have been previously reported in the chemical literature
Assi Laurent Ake
Boyd Michael R.
Bringmann Gerhard
François Guido
Phillipson J. David
Huang Evelyn Mei
Leydig , Voit & Mayer, Ltd.
The United States of America as represented by the Department of
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