Drug – bio-affecting and body treating compositions – Designated organic active ingredient containing – Peptide containing doai
Reexamination Certificate
2000-05-26
2004-07-27
Bugaisky, Gabriele (Department: 1653)
Drug, bio-affecting and body treating compositions
Designated organic active ingredient containing
Peptide containing doai
C514S002600, C514S014800, C514S015800, C530S324000, C530S327000, C530S300000
Reexamination Certificate
active
06767896
ABSTRACT:
BACKGROUND OF THE INVENTION
The invention relates to relatively short conotoxin peptides, about 10-20 residues in length, which are naturally available in minute amounts in the venom of the cone snails or analogous to the naturally available peptides, and which preferably include two disulfide bonds. These conotoxin peptides have analgesic activity and are thus useful for treating or preventing pain.
The publications and other materials used herein to illuminate the background of the invention, and in particular, cases to provide additional details respecting the practice, are incorporated by reference, and for convenience are referenced in the following text by author and date and are listed alphabetically by author in the appended bibliography.
Conus is a genus of predatory marine gastropods (snails) which envenomate their prey. Venomous cone snails use a highly developed projectile apparatus to deliver their cocktail of toxic conotoxins into their prey. In fish-eating species such as
Conus magus
the cone detects the presence of the fish using chemosensors in its siphon and when close enough extends its proboscis and fires a hollow harpoon-like tooth containing venom into the fish. This immobilizes the fish and enables the cone snail to wind it into its mouth via an attached filament. For general information on Conus and their venom see the website “grimwade.biochem” at “unimelb.edu.au” Prey capture is accomplished through a sophisticated arsenal of peptides which target specific ion channel and receptor subtypes. Each Conus species venom appears to contain a unique set of 50-200 peptides. The composition of the venom differs greatly between species and between individual snails within each species, each optimally evolved to paralyze its prey. The active components of the venom are small peptides toxins, typically 12-30 amino acid residues in length and are typically highly constrained peptides due to their high density of disulphide bonds.
The venoms consist of a large number of different peptide components that when separated exhibit a range of biological activities: when injected into mice they elicit a range of physiological responses from shaking to depression. The paralytic components of the venom that have been the focus of recent investigation are the &agr;-, &ohgr;- and &mgr;-conotoxins. All of these conotoxins act by preventing neuronal communication, but each targets a different aspect of the process to achieve this. The &agr;-conotoxins target nicotinic ligand gated channels, the &mgr;-conotoxins target the voltage-gated sodium channels and the &ohgr;-conotoxins target the voltage-gated calcium channels (Olivera et al., 1985). For example a linkage has been established between &agr;-, &agr;A-& &phgr;-conotoxins and the nicotinic ligand-gated ion channel; &ohgr;-conotoxins and the voltage-gated calcium channel; &mgr;-conotoxins and the voltage-gated sodium channel; &dgr;-conotoxins and the voltage-gated sodium channel; &kgr;-conotoxins and the voltage-gated potassium channel; conantokins and the ligand-gated glutamate (NMDA) channel. For a partial list of Conus peptides and their amino acid sequences see the website “pir” at “georgetown.edu”.
However, the structure and function of only a small minority of these peptides have been determined to date. For peptides where function has been determined, three classes of targets have been elucidated: voltage-gated ion channels; ligand-gated ion channels, and G-protein-linked receptors.
Conus peptides which target voltage-gated ion channels include those that delay the inactivation of sodium channels, as well as blockers specific for sodium channels, calcium channels and potassium channels. Peptides that target ligand-gated ion channels include antagonists of NMDA and serotonin receptors, as well as competitive and noncompetitive nicotinic receptor antagonists. Peptides which act on G-protein receptors include neurotensin and vasopressin receptor agonists. The unprecedented pharmaceutical selectivity of conotoxins is at least in part defined by a specific disulfide bond frameworks combined with hypervariable amino acids within disulfide loops (for a review see McIntosh et al., 1998).
There are drugs used in the treatment of pain, which are known in the literature and to the skilled artisan. See, for example, Merck Manual, 16th Ed. (1992). However, there is a demand for more active analgesic agents with diminished side effects and toxicity and which are non-addictive. The ideal analgesic would reduce the awareness of pain, produce analgesia over a wide range of pain types, act satisfactorily whether given orally or parenterally, produce minimal or no side effects, be free from tendency to produce tolerance and drug dependence.
Due to the high potency and exquisite selectivity of the conopeptides, several are in various stages of clinical development for treatment of human disorders. For example, two Conus peptides are being developed for the treatment of pain. The most advanced is &ohgr;-conotoxin MVIIA (ziconotide), an N-type calcium channel blocker (see Heading, C., 1999; U.S. Pat. No. 5,859,186). &ohgr;-Conotoxin MVIIA, isolated from
Conus magus
, is approximately 1000 times more potent than morphine, yet does not produce the tolerance or addictive properties of opiates. &ohgr;-Conotoxin MVIIA has completed Phase III (final stages) of human clinical trials and is now awaiting U.S. Food and Drug Administration approval as a therapeutic agent. &ohgr;-Conotoxin MVIIA is introduced into human patients by means of an implantable, programmable pump with a catheter threaded into the intrathecal space. Preclinical testing for use in post-surgical pain is being carried out on another Conus peptide, contulakin-G, isolated from
Conus geographus
(Craig et al. 1999). Contulakin-G is a 16 amino acid O-linked glycopeptide whose C-terminus resembles neurotensin. It is an agonist of neurotensin receptors, but appears significantly more potent than neurotensin in inhibiting pain in in vivo assays.
In view of a large number of biologically active substances in Conus species it is desirable to further characterize them and to identify peptides having many of the characteristics of an ideal analgesic for the treatment of pain. Surprisingly, and in accordance with this invention, Applicants have discovered novel conotoxins that can be useful for the treatment of pain and could address a long felt need for a safe and effective treatment.
SUMMARY OF THE INVENTION
The invention relates to relatively short conotoxin peptides, about 10-20 residues in length, which are naturally available in minute amounts in the venom of the cone snails or analogous to the naturally available peptides, and which preferably include two disulfide bonds. These conotoxin peptides have analgesic activity and are thus useful for treating or preventing pain.
In one embodiment, the present invention reports the isolation and characterization of a peptide from venom of Conus species such as marble cone,
Conus marmoreus
, that represents a new class of peptides and that possesses analgesic properties. In a second embodiment, related conotoxin peptides are isolated by DNA cloning. This invention provides isolation and characterization of a new class of peptides from the venom of the cone snails. The specific example of an isolated peptide is a representative member of a new family of Conus peptides.
More specifically, the present invention is directed to conotoxin peptides having the general formula I:
Xaa-Xaa
0
-Xaa
1
-Cys-Cys-Gly-Xaa
2
-Xaa
3
-Xaa
4
-Cys-Xaa
5
-Xaa
6
-Cys-Xaa
7
(SEQ ID NO:1)
wherein Xaa is des-Xaa, Asn, Gln or pyro-Glu; Xaa
0
is des-Xaa
0
, Gly, Ala, Glu, &ggr;-carboxy-Glu (Gla), Asp, Asn, Ser, Thr, g-Asn (where g is glycosylation), g-Ser or g-Thr; Xaa
1
is Val, Ala, Gly, Leu, Ile, Ser, Thr, g-Asn, g-Ser or g-Thr; Xaa
2
is Phe, Tyr, meta-Tyr, ortho-Tyr, nor-Tyr, mono-halo-Tyr, di-halo-Tyr, O-sulpho-Tyr, O-phospho-Tyr, nitro-Tyr, Trp (D or L), neo-Trp, halo-Trp (D or L), any synthetic aromatic amino acid, an aliphatic amino acid bearing linear o
Corpuz Gloria P.
Cruz Lourdes J.
Garrett James E.
Jones Robert M.
McIntosh J. Michael
Bugaisky Gabriele
Cognetix, Inc.
Rothwell Figg Ernst & Manbeck
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