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Morphine Biotransformation By Microbial Phenol OxidasesKorkmaz Erdural, Beril 01 December 2005 (has links) (PDF)
ABSTRACT
MORPHINE BIOTRANSFORMATIONS BY
MICROBIAL PHENOL OXIDASES
Erdural Korkmaz, Beril
M.S., Department of Chemical Engineering
Supervisor: Prof. Dr. Ufuk Bakir
Co-Supervisor: Prof. Dr. Ayhan S. Demir
January 2006, 96 pages
The objective of this study is to perform morphine biotransformation by using phenol oxidases. Syctalidium thermophilum, Thermomyces lanuginosus and Phanerochaete chrysosporium cells and culture fluid were used as microbial intracellular and extracellular phenol oxidases. Besides the phenol oxidases produced in laboratory, commercial pure phenol oxidases, A. bisporus tyrosinase and laccase, T. versicolor laccase and horseradish peroxidase, were also used in the morphine biotransformation reactions. Morphine biotransformation to pseudo-morphine was achieved by using pure T. versicolor laccase, A.bisporous tyrosinase and laccase. Before utilization of phenol oxidases in morphine biotransformations, the time course of microbial phenol oxidase productions were followed. Maximum phenol oxidase activity of S. thermophilum were detected on the 5th day of cultivation as
0.17 U/ml and the 4th day of cultivation as 0.072 U/ml, respectively. On the other hand, maximum laccase activity of P. chrysosporium was detected on the 8th day of cultivation as 78.5 U/ml. Although phenol oxidases which were obtained from S. thermophilum or T. lanuginosus could not catalyze morphine biotransformation, phenol oxidases including a peroxidase of P. chrysosporium transformed morphine to pseudo-morphine and an unknown product.
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A study on the acute and chronic effects of morphine on rat stomachs何美美, Ho, Mai-mai. January 1986 (has links)
published_or_final_version / Pharmacology / Doctoral / Doctor of Philosophy
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Some effects of morphine and hydrocortisone on glucose utilization in rat diaphragm彭李瓊華, Peng Lee, Chung-hua. January 1964 (has links)
published_or_final_version / Biochemistry / Doctoral / Doctor of Philosophy
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Investigations in series of ring C-bridged morphinansMartinez Bermejo, Fernando January 2000 (has links)
No description available.
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Cholecystokinin in the Rostral Ventromedial Medulla in Models of Neuropathic Pain and Morphine AdministrationHerman, David S January 2006 (has links)
States of abnormal pain induced by injuries to peripheral nerves share common features with opioid antinociceptive tolerance including mechanical and thermal hypersensitivity. Sustained administration of morphine in humans and in animals induces a state of abnormal pain (i.e., hyperalgesia) and may be associated with the development opioid antinociceptive tolerance. Persistent neuropathic pain states and opioid induced abnormal pain require descending facilitation arising from the rostral ventromedial medulla (RVM). Cholecystokinin (CCK), a pronociceptive peptide, may be up-regulated following opioid treatment and nerve injury in the brain and spinal cord. Therefore, it is hypothesized that CCK in the RVM may be up-regulated by sustained opioid administration and my consequently drive descending pain facilitatory mechanisms to produce hypersensitivity and antinociceptive tolerance.Acute systemic morphine administration produced a potentiation of CCK release in the RVM as measured using microdialysis techniques. Sustained systemic morphine administration sufficient to produce thermal and tactile hypersensitivity resulted in a significant increase in basal CCK release in the RVM. Spinal nerve ligation (SNL) produces similar behavioral hypersensitivity. CCK levels in the RVM also increased following SNL. These findings suggest that endogenous CCK released in the RVM drives descending facilitatory pathways to produce hypersensitivity following sustained morphine administration and neuropathic pain.Disease states such as neuropathic pain offer special challenges in drug design due to system changes that accompany these diseases. Here, novel peptides with agonist binding affinity and bioactivity at δ and μ opioid receptors and simultaneous antagonist activity at CCK receptors have been developed. Using in vivo behavioral measures, it was shown that intrathecal (i.th.) administration of these compounds suppresses the thermal and tactile hypersensitivity caused by spinal nerve ligation (SNL).These studies support the hypothesis that endogenous CCK drives descending pain facilitatory pathways and that bi-functional compounds that act as opioid agonists and CCK antagonists are effective for the treatment of neuropathic pain.
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Examination of the cerebral metabolic effects of morphine in rats exposed to acute and chronic footshock and conditioned stressGescuk, Bryan D. January 1994 (has links)
Thesis (Ph.D.)--Boston University / PLEASE NOTE: Boston University Libraries did not receive an Authorization To Manage form for this thesis or dissertation. It is therefore not openly accessible, though it may be available by request. If you are the author or principal advisor of this work and would like to request open access for it, please contact us at open-help@bu.edu. Thank you. / The purpose of this research was to determine, using the 2[14C]deoxyglucose autoradiographic method, the local cerebral metabolic rates for glucose (LCMRglu) after the administration of morphine or saline in rats escaping from acute or chronic footshock or exposed to conditioned stress. All animals were given morphine (4mg/kg, sc) or saline 7 days, 3 days and 10 minutes prior to the tracer injection. The effects of stimulation in the acute and chronic footshock studies revealed that an identical noxious stimulus may not have similar effects on functional cerebral activity if there are differences in experience with the str1xsor. The results of the conditioned stress experiment demonstrate that simply placing an animal in an environment previously associated with footshock is sufficient to elicit changes in LCMRglu.
The effects of morphine in the control and acute footshock experiments were similar in that nearly all of the 73 analyzed brain regions (99% and 93%, respectively) showed decreases in LCMRg1u. Morphine, however, caused fewer decreases (56%) in the chronic footshock study. Interestingly, the percentage of structures showing decreases in the conditioned stress study (79%) was approximately halfway between the effects seen in the two footshock studies. Morphine in the presence of acute footshock, compared to acute footshock alone, caused significant decreases in elements of the limbic telencephalon, basal forebrain and thalamic midline (paraventricular and paratenial nuclei).
On the other hand, morphine did not cause any significant decreases in these structures (or others) in the chronic footshock study. Rather, the combination of morphine and chronic footshock, compared to morphine alone, caused significant increases in several brainstem structures previously implicated in opioid analgesia: the locus coeruleus, gigantocellular reticular nucleus and raphe magnus. Additionally, significant effects were seen in basal ganglia structures which are normally associated with the motor system. The effects seen in these structures, along with the significant effect demonstrated in the parafasicular thalamic nucleus, suggest that morphine works to attenuate pain in animals exposed to chronic footshock via neural networks responsible for sensorimotor reactions to pain. Alternatively, animals exposed to chronic footshock may have developed tolerance to the effects of morphine. The effects of morphine, however, in the chronic footshock experiment are much different from those seen in the acute footshock study where morphine acts primarily in limbic structures and midline thalamus to attenuate the affective reaction to pain. / 2031-01-01
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The production of polyclonal and monoclonal antibodies against morphine.January 1988 (has links)
by Julia Luen-wah Woo. / Thesis (M.Ph.) -- Chinese University of Hong Kong, 1988. / Bibliography: leaves 90-94.
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A study of the acute and chronic effects of morphine on autonomic activities in rats /Leung, Man-kit, Christopher. January 1986 (has links)
Thesis (Ph. D.)--University of Hong Kong, 1987.
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Morphine treatment and acute myocardial ischaemia in rats /Ko, Weng-wah, Wendy. January 1988 (has links)
Thesis (Ph. D.)--University of Hong Kong, 1988.
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Changing in potassium sensitivity in muscle of chronically morphinized rats.Wong, Siu-chun, Susanna. January 1970 (has links)
Thesis (Ph. D.)--University of Hong Kong, 1970. / Typewritten.
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