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Neurobiology Cannabinoids act backwards (2001)

Vaughan, Christopher W. ; Christie, MacDonald J.

[s.l.] : Nature Publishing Group

Nature 410 (2001), S. 527-530

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ISSN: 1476-4687

Source: Nature Archives 1869 - 2009

Topics: Biology , Chemistry and Pharmacology , Medicine , Natural Sciences in General , Physics

Notes: [Auszug] Preparations from the plant Cannabis sativa have been used since antiquity, not only for their intoxicating effects, but also to treat a number of ailments. The main active component of these preparations, Δ9-tetrahydrocannabinol, produces most of its effects on the central ...

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1038/35069167

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2

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OPIOID RECEPTOR SIGNALLING MECHANISMS (1999)

Connor, Mark ; Christie, MacDonald J

Melbourne, Australia : Blackwell Science Asia Pty. Ltd.

Clinical and experimental pharmacology and physiology 26 (1999), S. 0

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ISSN: 1440-1681

Source: Blackwell Publishing Journal Backfiles 1879-2005

Topics: Medicine

Notes: 1. Three pharmacological types of opioid receptors, μ, δ and κ, and their corresponding genes have been identified. Although other types of opioid receptors have been suggested, their existence has not been established unequivocally. A fourth opioid receptor, ORL1, which is genetically closely related to the others, has also been isolated. ORL1 responds to the endogenous agonist nociceptin (orphanin FQ) and displays a pharmacological profile that differs greatly from μ, δ and κ receptors.2. All opioid receptors mediate many of their cellular effects via activation of heterotrimeric G-proteins. The μ, δ and κ receptors are all capable of interacting with the pertussis toxin-sensitive G-protein α-subunits Gi1, Gi2, Gi3, Go1, Go2 and the pertussis toxin-insensitive Gz and G16. None of the opioid receptors interacts substantially with Gs and μ receptors do not activate Gq, G11, G12, G13 or G14.3. Differential coupling of different opioid receptors to most types of G-proteins is marginal. The μ, δ and κ receptors appear to preferentially activate Go and Gi2 over other pertussis toxin-sensitive G-proteins, although there is evidence that μ receptors show some preference for Gi3. δ Receptors couple more efficiently to G16 than do μ or κ receptors.4. There is some evidence that opioid receptors, particularly μ and ORL1 receptors, can also couple to cellular effectors in a G-protein-independent manner.5. In general, the consequences of activation of any of the opioid receptors in a given cell type depend more on the profile (stoichiometry) of the G-proteins and effectors expressed than on the type of opioid receptor present in the cell. Notions that different types of opioid receptors intrinsically couple preferentially to one type of effector rather than another should, therefore, be discarded.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1046/j.1440-1681.1999.03049.x

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3

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Cellular Actions Of Opioids And Other Analgesics: Implications For Synergism In Pain Relief (2000)

Christie, MacDonald J ; Connor, Mark ; Vaughan, Christopher W ; [et al.]

Melbourne, Australia : Blackwell Science Pty

Clinical and experimental pharmacology and physiology 27 (2000), S. 0

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ISSN: 1440-1681

Source: Blackwell Publishing Journal Backfiles 1879-2005

Topics: Medicine

Notes: 1. μ-Opioid receptor agonists mediate their central analgesic effects by actions on neurons within brain regions such as the mid-brain periaqueductal grey (PAG). Within the PAG, μ-opioid receptor-mediated analgesia results from inhibition of GABAergic influences on output projection neurons. We have established that μ-opioid receptor activation in the PAG causes a presynaptic inhibition of GABA release that is mediated by activation of a voltage-dependent K+ channel via 12-lipoxygenase (LOX) metabolites of arachidonic acid.2. At a cellular level, μ-opioid agonists have also been shown to open inwardly rectifying K+ channels, close voltage-gated Ca2+ channels and presynaptically inhibit glutamatergic synaptic transmission in the PAG.3. The μ-opioid receptor-mediated presynaptic inhibition of GABAergic transmission was abolished by phospholipase A2 inhibitors and non-specific LOX and specific 12-LOX inhibitors. Cyclo-oxygenase (COX) and specific 5-LOX inhibitors did not reduce the inhibitory effects of μ-opioid agonists.4. The opioid actions on GABAergic transmission were mimicked by arachidonic acid and 12-LOX metabolites, but not 5-LOX metabolites. The efficacy of μ-opioids was enhanced synergistically by treatment of PAG neurons with inhibitors of the other major enzymes responsible for arachidonic acid metabolism, COX and 5-LOX.5. These results explain a previously described analgesic action of COX inhibitors in the central nervous system that was both independent of prostanoid release and inhibited by opioid receptor antagonists and they also explain the synergistic interaction of opioids with COX inhibitors. These findings also suggest new avenues for the development of centrally active analgesic agents involving combinations of lowered doses of opioids and specific 5-LOX inhibitors.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1046/j.1440-1681.2000.03291.x

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4

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MOLECULAR AND FUNCTIONAL DIVERSITY OF K+ CHANNELS (1995)

Christie, MacDonald J.

Oxford, UK : Blackwell Publishing Ltd

Clinical and experimental pharmacology and physiology 22 (1995), S. 0

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ISSN: 1440-1681

Source: Blackwell Publishing Journal Backfiles 1879-2005

Topics: Medicine

Notes: 1. Amino acid sequences encoding K+ channels belong to several subfamilies of the voltage-gated ion channel superfamily which includes Na2+-, Ca2+-, and cyclic nucleotide gated channels. The Kv family is the largest group, and encodes delayed rectifier, A-type, and large conductance Ca2+ activated K+ channels.2. The α-subunits of Kv channels form as tetramers of four independent subunits. Each subunit has six membrane spanning regions and a pore forming ‘P’ region. Subunits belong to subfamilies (Kv1–4, BK, Eag) comprising multiple members, each of which has distinct properties resembling each of the major types of native Kv channel when expressed as homomultimers in heterologous systems.3. Enormous diversity of Kv channel function arises from the multiplicity of subunits, the formation of heteromultimers within subfamilies and from association with intracellular β-subunit proteins.4. In the absence of direct structural information, mutational analyses have provided considerable insights into the structure of the voltage-sensor, pore-forming region and the sites of action of drugs, toxins and associated proteins.5. Another subfamily, the inwardly rectifying, or KIR, family, appears to have arisen from a deletion of the first four membrane spanning regions of ancient Kv channels, changing gating properties from outward to inward rectification. These include the G-protein gated inward rectifiers and Katp channels.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1111/j.1440-1681.1995.tb02331.x

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5

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Cloning and expression of a rat D 2 dopamine receptor cDNA (1988)

Bunzow, James R. ; Tol, Hubert H. M. Van ; Grandy, David K. ; [et al.]

[s.l.] : Nature Publishing Group

Nature 336 (1988), S. 783-787

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ISSN: 1476-4687

Source: Nature Archives 1869 - 2009

Topics: Biology , Chemistry and Pharmacology , Medicine , Natural Sciences in General , Physics

Notes: [Auszug] Table 1 K{ values (nM) for L-RGB2Zem-l and rat striatum RGB-2 transformed Ltk~ cells Rat striatum (+)Butaclamol 0.83 1.0 (-)Butaclamol 〉 1,000 〉 1,000 Haloperidol 3.0 5.3 Dopamine + GTP 17,000 6,300 Sulpiride high affinity 80 67(87%) low ...

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1038/336783a0

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6

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The structure of a novel insecticidal neurotoxin, ω-atracotoxin-HV1, from the venom of an Australian funnel web spider (1997)

Fletcher, Jamie I. ; Smith, Ross ; O'Donoghue, Séan I. ; [et al.]

[s.l.] : Nature Publishing Group

Nature structural biology 4 (1997), S. 559-566

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ISSN: 1072-8368

Source: Nature Archives 1869 - 2009

Topics: Biology , Medicine

Notes: [Auszug] A family of potent insecticidal toxins has recently been isolated from the venom of Australian funnel web spiders. Among these is the 37-residue peptide ω-atracotoxin-HV1 (ω-ACTX-HV1) from Hadronyche versuta. We have chemically synthesized and folded ω-ACTX-HV1, shown that it is ...

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1038/nsb0797-559

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7

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Discovery and characterization of a family of insecticidal neurotoxins with a rare vicinal disulfide bridge (2000)

Wang, Xiu-hong ; Connor, Mark ; Smith, Ross ; [et al.]

[s.l.] : Nature America Inc.

Nature structural biology 7 (2000), S. 505-513

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ISSN: 1072-8368

Source: Nature Archives 1869 - 2009

Topics: Biology , Medicine

Notes: [Auszug] We have isolated a family of insect-selective neurotoxins from the venom of the Australian funnel-web spider that appear to be good candidates for biopesticide engineering. These peptides, which we have named the Janus-faced atracotoxins (J-ACTXs), each contain 36 or 37 residues, with four ...

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1038/nsb0600_505

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8

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Lack of correlations between plasma concentration of medroxyprogesterone acetate, hypothalamic-pituitary function, and tumour response in patients with advanced breast cancer (1985)

Hedley, David W. ; Christie, Macdonald ; Weatherby, Robert P. ; [et al.]

Springer

Cancer chemotherapy and pharmacology 14 (1985), S. 112-115

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ISSN: 1432-0843

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary Plasma medroxyprogesterone acetate (MPA) concentrations were measured in 61 patients with advanced breast cancer, after 3 weeks' treatment using 200 mg PO 8-hourly, to determine whether the previously reported wide interpatient variations correlated with tumour response or toxicity. Seventeen patients (28%) responded to the drug, and their mean plasma MPA concentration was 97 ng/ml ±68 SD, compared with 115 ng/ml ±87 SD for the patients whose disease progressed. Side-effects attributed to MPA were seen in 18 patients, who had a mean drug concentration of 113 ng/ml±104 SD. This was not significantly higher than that of the patients who did not experience drug toxicity. Because of a suggestion that some of the antitumour activity of the drug could be mediated via an effect on the hypothalamic-pituitary axis, we also measured plasma FSG, LH, and prolactin concentrations after the 3-week treatment with MPA, but found no correlations with either drug concentration or tumour response. These results indicate that with the present treatment schedule the monitoring of plasma MPA concentrations has no role in routine practice and suggest that the inherent sensitivity of the tumour to progesterone is probably the major determinant of response.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00434347

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9

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Spider toxins: A new group of potassium channel modulators (1999)

Fletcher, Jamie I. ; Wang, Xiuhong ; Connor, Mark ; [et al.]

Springer

Perspectives in drug discovery and design 15-16 (1999), S. 61-69

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ISSN: 1573-9023

Keywords: hanatoxins ; heteropodatoxins ; funnel-web spider toxins ; spider toxins ; voltage-gated K+ channels

Source: Springer Online Journal Archives 1860-2000

Topics: Chemistry and Pharmacology

Notes: Abstract Spider toxins that target potassium channels constitute a new class of pharmacological tools that can be used to probe the structure and function of these channels at the molecular level. The limited studies performed to date indicate that these peptide toxins may facilitate the analysis of K+ channels that have proved insensitive to peptide inhibitors isolated from other animal sources. Thus far, two classes of K+ channel-selective spider toxins have been isolated, sequenced, and pharmacologically characterised – the hanatoxins (HaTx) from Grammastola spatulata and heteropodatoxins (HpTx) from Heteropoda venatoria. The hanatoxins block Kv2.1 and Kv4.2 voltage-gated K+ channels. In Kv2.1 K+ channels this occurs as a consequence of a depolarising shift in the voltage dependence of activation and not by occlusion of the channel pore. These toxins show minimal sequence homology with other peptide inhibitors of K+ channels, but they do share some homology with other ion channel toxins from spiders, particularly with regard to the spacing between cysteine residues. We have recently isolated three K+ channel antagonists from the venom of the Australian funnel-web spider Hadronyche versuta; at least two of these toxins are likely to constitute a new class of spider toxins active on K+ channels as they are approximately twice as large as HaTx and HpTx.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1023/A:1017039418046

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Sensitivity of morphine-tolerant rats to muscarinic and dopaminergic agonists: Relation to tolerance or withdrawal (1979)

Christie, Macdonald J. ; Overstreet, David H.

Springer

Psychopharmacology 65 (1979), S. 27-34

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ISSN: 1432-2072

Keywords: Morphine tolerance and withdrawal ; Super- and Sub-sensitivity ; Dopaminergic and cholinergic receptors

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract Male hooded Wistar rats were treated chronically once daily with morphine sulfate (20 mg/kg SC) after completing a session in an operant chamber. Periodical challenges with morphine (8 mg/kg) prior to the operant session established that tolerance development was virtually complete within 10 days. The morphine-treated rats were more sensitive to the behavioral suppressing effects of apomorphine, a dopamine agonist, and pilocarpine, an acetylcholine agonist, when administered in the tolerant state (morphine given 30 min prior to operant session), regardless of whether they were administered peripherally or directly into the striatum. Conversely, the morphine-treated rats were less sensitive to both agonists when administered in the withdrawal state (morphine given 24 h prior to the operant session). In animals undergoing a similar regimen of chronic morphine treatment, receptor binding studies revealed a lowered affinity (Higher K D apparent) for the dopamine receptor in the striatum of morphine-withdrawn rats, using 3H-spiroperidol as the ligand. The morphine-withdrawn rats also appeared to have fewer muscarinic cholinergic receptors (lower B max), using 3H-QNB as the ligand. The also had a lower concentration of membrane-bound phosphodiesterase modulator protein. In general, no significant differences were observed for the above parameters in the morphine-tolerant rats. These behavioral and neurochemical studies are consistent with the view that morphine-tolerant rats are supersensitive to dopamine and acetylcholine agonists and morphine-withdrawn rats are subsensitive.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00491974

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