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1

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The neuropeptide bradykinin stimulates phosphoinositide turnover in HSDM1C1 cells: B2-antagonist-sensitive responses and receptor binding studies (1993)

Sharif, N. A. ; Whiting, R. L.

Springer

Neurochemical research 18 (1993), S. 1313-1320

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ISSN: 1573-6903

Keywords: Bradykinin ; receptors ; phosphoinositides ; PI turnover ; receptor binding ; HSDM1C1 cells ; fibrosarcoma

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract Bradykinin (BK) and its analogs (1 nM-100 μM) stimulated phosphoinositide (PI) turnover in murine fibrosarcoma (HSDM1C1) cells in a concentration-dependent manner. The relative potencies (EC50) were: BK=48±4 nM; Lys-BK=39±3 nM; Met-Lys-BK=158±33 nM; Des-Arg9-BK=2617±598 nM (means±SEM, n=3–14). All these analogs were full agonists and they produced up to 5.4±0.4-fold stimulation of PI turnover at the highest concentration (10–100 μM) of the peptides. In contrast, the analogs [D-Arg0-HYP3-Thienyl5,8-D-Phe7]-BK (HYP3-antagonist), [D-Arg0-HYP3-Thienyl,5,8-D-Phe7]-BK (Thienyl antagonist) and Des-Arg9-Leu8-BK were inactive, as agonists, at 0.1 nM-1 μM in this system. These data suggested that BK-induced PI turnover in these cells was mediated via B2-type of BK receptors. This was confirmed further by the fact that both the B2-selective Hyp3- and Thienyl-antagonists inhibited BK-induced PI turnover with KBS of 369±51 nM and 368±118 nM respectively while the B1-selective antagonist, Des-Arg9-Leu8-BK, was inactive at 1 μM. [3H]BK receptor binding studies revealed two binding sites, one with high affinity (Kd=0.24±0.06 nM; Bmax=1.4±0.4 pmol/g tissue) and the other with low affinity (Kd=18.5±0.95 nM; Bmax=25.1±0.52 pmol/g tissue), on HSDM1C1 cell homogenates. The rank order of affinity of BK analogs at inhibiting specific [3H]BK binding was similar to that found for PI turnover. Taken together, these data have provided evidence for the presence of two B2-type BK binding sites on the HSDM1C1 cells. Based on the affinity parameters, the low-affinity component of [3H]BK binding in HSDM1C1 cells appears to be coupled to the phospholipase C-induced PI turnover mechanism. The high-affinity component has been previously shown to mediate the production of prostaglandins by activation of phospholipase A2.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00975053

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2

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M3 muscarinic receptors on murine HSDM1C1 cells: Further functional, regulatory, and receptor binding studies (1995)

Sharif, N. A. ; To, Z. P. ; Wong, K. H. ; [et al.]

Springer

Neurochemical research 20 (1995), S. 61-68

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ISSN: 1573-6903

Keywords: Muscarinic ; M3 receptors ; HSDM1C1 cells ; PI turnover ; [3H]4-DAMP binding ; Receptor binding

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract In the present studies, the pharmacology and regulation of the functional muscarinic receptors on HSDM1C1 cells were probed using phosphoinositide (PI) turnover assays. In addition, the receptor binding of the putative M3-selective radioligand, [3H]4-DAMP, to cell homogenates was characterized. Carbachol (EC50=9 μM), (+)muscarine (EC50=4.5 μM) and cis-dioxolane (EC5=0.72 μM) were full agonists which stimulated PI turnover by 13.3±1.0 fold above basal values. The potencies of numerous agonists in this assay system were relatively similar to their affinities in receptor binding assays. Exposure of HSDM1C1 cells to 10 nM–10 μM muscarine during the last 24h of [3H]myo-inositol-labeling resulted in a concentration-dependent reduction in the cisdioxolane affinity and maximal PI response induced by subsequent treatment with cis-dioxolane. pertussis toxin (5–2000 ng/ml) caused a partial reduction in the cis-dioxolane-induced PI turnover. Likewise, exposure of the HSDM1C1 cells to an active phorbol ester (TPA) resulted in a partial inhibition of the cis-dioxolane-induced (100 μM) PI turnover. The half-maximal effect of TPA was produced at 1.8±0.3 nM. [3H]4-DAMP binding to cell homogenates was of high affinity (Kd=0.19±0.04 nM) and moderate capacity (Bmax=201±22 fmol/mg protein). The pharmacological specificity (4-DAMP〉p-FHHSiD〉dicyclomine〉pirenzepine〉methoctramine〉AFDX-116 〉gallamine) resembled that for [3H]NMS binding and correlated well with that observed for inhibition of PI turnover. These studies further support the identification of M3 receptors on HSDM1C1 cells. These receptors have been shown to be influenced by pertussis toxin, an active phorbol ester and to exhibit desensitization.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00995154

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3

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Quantitative autoradiography demonstrates selective modulation of rat brain regional dopamine (D1 and D2) receptor subtypes after chronic manipulation of dietary salt (1995)

Sharif, N. A. ; Nunes, J. L. ; Rosenkranz, R. P. ; [et al.]

Springer

Neurochemical research 20 (1995), S. 121-128

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ISSN: 1573-6903

Keywords: Dopamine receptors ; autoradiography ; hypertension ; schizophrenia ; Parkinson's disease

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract The effects of chronic dietary sodium chloride (NaCl) consumption on renal function and brain dopamine receptors were studied in adult, male normotensive rats. Compared to rats maintained on the normal NaCl (0.33%) diet, animals maintained on the low NaCl (0%) diet for 4 weeks exhibited significant increases in plasma aldosterone, chloride and changes in urinary electrolyte excretion. In contrast, rats maintained on the high NaCl (8%) diet for 4 weeks demonstrated significant increases in urine volume and urinary sodium, chloride and dopamine excretions and water intake. Rats fed the high NaCl diet displayed a 42–59% decrease (p〈0.001–0.05) in D1 binding in the nucleus accumbens (NA), olfactory tubercle (OT) and the striatum (STM), without any effects on D2 binding in these brain regions. Rats maintained on the low NaCl diet also demonstrated decreased D1 binding in the ventral (24%, p〈0.02) and lateral (29%, p〈0.01) STM, but not in the OT, NA, entopeduncular nucleus and substantia nigra. Rats fed low or high NaCl diets exhibited a 35–180% increase (p〈0.01–0.05) in D2 binding in several mid-brain areas (e.g. hypothalamus, thalamus and hippocampus) and hindbrain regions (e.g. superior colliculus and nucleus tractus solitarius) without affecting the D1 binding. These data indicate that chronic modification of dietary salt intake profoundly affects the renal handling of sodium/water excretion and leads to selective up- and/or down-regulation of DA receptor subtypes in different areas of the brain. These findings may have relevance to centrally-mediated hypertension, Parkinson's disease, schizophrenia and other brain disorders involving dopamine and dopamine receptors.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00970535

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4

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5-Methoxytryptamine and 2-methyl-5-hydroxytryptamine-induced desensitization as a discriminative tool for the 5-HT3 and putative 5-HT4 receptors in guinea pig ileum (1990)

Craig, D. A. ; Eglen, R. M. ; Walsh, L. K. M. ; [et al.]

Springer

Naunyn-Schmiedeberg's archives of pharmacology 342 (1990), S. 9-16

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ISSN: 1432-1912

Keywords: 5-HT4 ; 5-HT3 ; Desensitization ; 5-Methoxytryptamine ; 2-Methyl-5-HT

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary Agonist-induced desensitization has been utilized to discriminate and independently “isolate” the neuronal excitatory receptors to 5-hydroxytryptamine (5-HT) in the guinea pig ileum (5-HT3 and putative 5-HT4 receptors). Electrically stimulated longitudinal muscle myenteric plexus preparations, and non-stimulated segments of whole ileum were used. Exposure to 5-methoxytryptamine (10 μmol/l) inhibited completely responses to 5-HT at the putative 5-HT4 receptor without affecting 5-HT3-mediated responses. Conversely, exposure to 2-methyl-5-HT (10 μmol/l) inhibited completely responses to 5-HT at the 5-HT3 receptor without affecting putative 5-HT4-mediated responses. The inhibition with 5-methoxytryptamine and 2-methyl-5-HT, either alone or in combination, appeared selective as responses to KCI, DMPP, carbachol, histamine, and substance P were unaffected or only very slightly modified. Furthermore, the pA2 values for ICS 205–930 at the putative 5-HT4 (pA2 = 6.2 to 6.5) and 5-HT3 (pA2 = 7.6 to 8.1) receptors (estimated in the presence of 2-methyl-5HT and 5-methoxytryptamine, respectively) were consistent with those estimated in the absence of desensitization. 5-Methoxytryptamine, but not 2-methyl-5-HT, suppressed completely but reversibly the concentration-effect curve to renzapride, suggesting that responses to this agent are mediated exclusively via agonism at the putative 5-HT4 receptor. It is concluded that 5-methoxytryptamine and 2-methyl-5-HT can be utilized as selective probes to discriminate the putative 5-HT4 receptor from the 5-HT3 receptor in guinea pig ileum. This finding is of importance as no selective antagonist exists for the putative 5-HT4 receptor. Furthermore, the presently described method of agonist-induced desensitization and 5-HT receptor discrimination may be useful for the identification and characterization of the putative 5-HT4 receptor in other tissues and species.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00178965

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5

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The action of (±)L-660,863 [(±)3-(3-amino-1,2,4-oxadiazole-5-yl)-quinuclidine] at muscarinic receptor subtypes in vitro (1992)

Eglen, R. M. ; Harris, G. C. ; Ford, A. P. D. W. ; [et al.]

Springer

Naunyn-Schmiedeberg's archives of pharmacology 345 (1992), S. 375-381

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ISSN: 1432-1912

Keywords: (±)L-660,863 ; Carbachol ; (+)cis dioxolane ; Muscarinic receptor subtypes

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary 1. The muscarinic pharmacology of a novel oxadiazole muscarinic agonist, (±) L-660,863, [±3-(3-amino- 1,2,4-oxadiazole-5-yl)-quinuclidine] has been studied using pharmacological, radioligand binding and biochemical techniques, in vitro. 2. In isolated tissue experiments, (±)L-660,863 was a more potent agonist than carbachol in all preparations studied, being most potent at muscarinic receptors mediating negative chronotropy in guinea-pig right, spontaneously beating atria and least potent at receptors mediating contractions in canine saphenous vein and endothelial denuded rabbit aorta (-log EC50) values were 8.8, 6.6 and 6.3, respectively. The apparent affinities (-log KA) of (±)L-660,863, estimated by receptor inactivation, showed some selectivity toward the atrial M2 muscarinic receptor (-log KA = 7.6) in comparison to the M1 or M3 muscarinic receptors (-log KA = 5.4 and 6.2), respectively. This degree of selectivity was also observed in competition radioligand binding studies. 3. At M3 muscarinic receptors mediating inositol phosphates (IPs) accumulation in longitudinal muscle of guinea-pig ileum, the potency of (00B1;)L-660,863 (-log EC50 value = 6.2) was similar to the apparent affinity calculated at M3 muscarinic receptors in the functional studies (see above). In contrast, at muscarinic receptors mediating IPs accumulation in guinea-pig atria and ventricles, the potency for (±)L-660,863 (-log EC50 = 6.2 and 6.4, respectively) was lower than the apparent affinity calculated at M2 muscarinic receptors from inotropic and binding studies in cardiac tissue (see above). These data suggest that the concentration-occupancy curve for (±)L-660,863 at cardiac muscarinic receptors mediating IPs accumulation lies to the right of the concentration-response curve. Similar conclusions may be made with regard to contraction by (±)L-660,863 of endothelial denuded rabbit aorta mediated by M2 receptors (Jaiswal et al. 1991). These findings may imply differences between muscarinic receptors mediating negative inotropy and IPs accumulation in guinea-pig myocardium or contraction of endothelial denuded rabbit aorta. 4. (±)L-660,863, in conclusion, acted as a potent muscarinic agonist, with some degree of M2 muscarinic receptor selectivity M2 VS M1 - 160 fold; M2 vs M3 - 25 fold \3- the first muscarinic agonist with, such a profile of activity. This compound may provide a useful tool with which to characterize muscarinic receptor function, as evidenced by the biochemical studies in cardiac tissue.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00176613

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6

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Interaction of p-F-HHSiD (p-Fluoro-hexahydrosila-difenidol) at muscarinic receptors in guinea-pig trachea (1990)

Eglen, R. M. ; Cornett, C. M. ; Whiting, R. L.

Springer

Naunyn-Schmiedeberg's archives of pharmacology 342 (1990), S. 394-399

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ISSN: 1432-1912

Keywords: Muscarinic receptor subtypes ; Guinea-pig trachea ; para-Fluoro-hexahydrosila-difenidol

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary 1. para-Fluoro-hexahydrosila-difenidol (p-FHHSiD) has been proposed as an M3 selective antagonist. However, the M3 selectivity is variable in that it exhibits a high pA2 value for M3 muscarinic receptors in guinea-pig ileum but a low value at muscarinic receptors in guinea-pig trachea. 2. The pA2 value in the trachea was found to be agonist independent since similar pA2 values were found when acetylcholine, carbachol, (+)-cis-dioxolane or OXA-22 were used (7.13, 7.03, 6.85 and 6.97, respectively). The pA2 value was not meaningfully increased when the equilibrium period was increased from 60 to 180 min. The pA2 value was unaffected by blockade of M1 or M2 receptors, using 0.1 μM pirenzepine or methoctramine (7.03 and 7.14, respectively). p-F-HHSiD and atropine appeared to act at the same site, as adjudged by combination concentration-ratio studies. 3. The pA2 values for p-F-HHSiD vary by 10 fold between ileal (8.0) and tracheal M3 receptors (7.0). The precise reason for this is unknown, but appears to be unrelated to conditions of disequilibrium that could be detected. The antagonist should therefore only be employed to distinguish M3 or M1 from M2 receptors. In this respect, although the M1/M3 VS M2 discrimination is relatively large (68 fold), p-F-HHSiD exhibits similar properties to other putative M3 selective antagonists such as 4-diphenylacetoxy-N-methyl piperidine methiodide (4-DAMP) or the parent compound, hexahydrosiladifenidol (HHSiD).

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00169455

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7

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Characterization of muscarinic receptors mediating release of epithelial derived relaxant factor (EpDRF) in guinea-pig isolated trachea (1991)

Eglen, R. M. ; Harris, G. C. ; Taylor, M. ; [et al.]

Springer

Naunyn-Schmiedeberg's archives of pharmacology 344 (1991), S. 29-35

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ISSN: 1432-1912

Keywords: Epithelial derived relaxant factor ; Muscarinic receptor subtypes ; Guinea-pig trachea

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary Muscarinic receptors mediating the release of epithelial derived relaxant factor (EpDRF) have been studied by using both contractions of the guinea-pig tracheal strip (with epithelium intact or denuded) or a coaxial bioassay assembly (rat anococcygeus-recipient; guinea-pig trachea-donor tissue). Indomethacin (1 μM/l) and physostigmine (0.1 μM/l) were both present throughout the study. In the tracheal strip studies, the potencies and maximal effects of all agonists studied (acetylcholine, arecoline, bethanechol, carbachol, (+)cis-dioxolane, ethoxyethyltrimethylammonium, L-660,863, (±)methacholine and OXA-22) were not affected or were only slightly (but significantly) reduced by removal of the epithelium. The -log KB for the muscarinic antagonists, atropine, pirenzepine, methoctramine and 4-DAMP (4-diphenyl-acetoxy-N-methylpiperidine) were also not affected and the -log KB values were consistent with M3 muscarinic receptor function. However, the -log KB value of para-fluoro-hexahydro-siladifendol (p-F-HHSiD) was significantly (P 〈 0.05) increased upon epithelial denudation (epithelium intact, 7.1; epithelium removed, 7.6). The coaxial bioassay assembly provided more convincing evidence for release of EpDRF in that all muscarinic agonists studied caused relaxations of a precontracted anococcygeus tissue. These relaxations were observed only in the presence of a tracheal tube possessing an intact epithelium. The rank order of potencies for agonists at receptors mediating EpDRF dependent relaxation were similar to those estimated at receptors causing contraction. These data suggested that a substantial receptor reserve was associated with the receptors mediating both EpDRF release and contraction. The affinities of the muscarinic antagonists (atropine, pirenzepine, methoctramine, p-F-HHSiD, 4-DAMP and gallamine) indicated that M3 receptors also mediated EpDRF release. It is concluded that EpDRF release in guinea-pig trachea is a general property of muscarinic agonists and that this process is mediated, like the contractile response, by M3 receptors.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00167379

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8

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Characterization of the interaction of the cervane alkaloid, imperialine, at muscarinic receptors in vitro (1992)

Eglen, R. M. ; Harris, G. C. ; Cox, H. ; [et al.]

Springer

Naunyn-Schmiedeberg's archives of pharmacology 346 (1992), S. 144-151

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ISSN: 1432-1912

Keywords: Imperialine ; Muscarinic receptor subtypes ; Cervane alkaloids

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Summary The action of the cervane alkaloid, imperialine, has been assessed at M1, M2 and M3 receptors in functional assays and at M1, M2, M3 and putative M4 sites in binding studies. In functional studies, imperialine acted as a selective surmountable antagonist at M2 receptors in guinea-pig isolated atria and uterus (−log KB = 7.7 and 7.4, respectively), in comparison to M1, receptors in canine isolated saphenous vein (−log KB = 6.9) or M3 receptors in a range of guinea-pig isolated smooth muscles including ileum, trachea, fundus, seminal vesicle or oesophagus (−log KB = 6.6–6.8). In rat aorta, the −log KB value at the M3 receptor (5.9) was slightly, but significantly, lower. In competition radioligand binding studies, imperialine was also selective toward to M2 sites in rat myocardium (−log Ki = 7.2) with respect to M1 and M3 sites (rat cerebral cortex, rat submaxillary gland; −log Ki = 6.1 and 5.7, respectively). However, it did not significantly discriminate between rat cardiac M2 sites and putative M4 sites in rabbit lung (−log Ki = 6.9). Imperialine resembles the alkaloid himbacine in terms of its pharmacological profile at muscarinic receptor subtypes in that it acts as an M2 selective antagonist with respect to M1 or M3 sites. It may also provide a second, commercially available, antagonist with which to discriminate between M1 and M4 receptors.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00165295

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9

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Dopamine D2-receptors mediate hypothermia in mice: ICV and IP effects of agonists and antagonists (1991)

Nunes, J. L. ; Sharif, N. A. ; Michel, A. D. ; [et al.]

Springer

Neurochemical research 16 (1991), S. 1167-1174

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ISSN: 1573-6903

Keywords: Dopamine receptors ; quinpirole hypothermia ; D2 receptors ; D1/D2 receptor interaction ; temperature regulation

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract The effect of centrally and peripherally administered dopamine D1 and D2 specific compounds on core body temperature in mice was investigated. Quinpirole (LY-17155), a D2 agonist, induced a dose-dependent fall in body temperature (2.4–11.6%; p〈0.003) when injected intraperitoneally (ip, 0.3–3.0 mg/kg) and intracerebroventricularly (icv, 0.1 mg/kg). This quinpirole-induced (1.0 mg/kg, ip) hypothermia was reversed by the central and peripheral administration of the D2 antagonists S-(−)-sulpiride (3.0–30.0 mg/kg, ip; 0.1–3.0 mg/kg, icv) and spiperone (0.03 and 0.1 mg/kg, ip; 0.03–3.0 mg/kg, icv). Domperidone, a D2 antagonist which does not cross the blood brain barrier, had no effect on quinpirole-induced hypothermia (1.0–10.0 mg/kg, ip). Domperidone partially reversed quinpirole-induced hypothermia at 0.1–30.0 mg/kg, icv. The D1 agonist, SKF-38393 at a high dose of 10.0 mg/kg, ip mildly attenuated quinpirole-induced hypothermia (a 1.8% increase in temperature). SKF-38393 at 10.0 mg/kg, icv potentiated quinpirole-induced hypothermia. SCH-23390 (0.1–3.0 mg/kg, ip), a D1 antagonist, had no effect on quinpirole-induced hypothermia and potentiated the hypothermia when administered icv. An ineffective icv dose of spiperone (0.01 mg/kg) in reversing quinpirole-induced hypothermia was rendered effective by prior administration of SCH-23390 (0.1–3.0 mg/kg, icv) but not by SKF-38393 (1.0–10.0 mg/kg, icv). These data suggest a central D2 receptor mechanism mediating hypothermia in mice which is capable of being modulated by the D1 receptor.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00966597

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10

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Analogs of thyrotropin-releasing hormone (TRH): Receptor affinities in brains, spinal cords, and pituitaries of different species (1991)

Sharif, N. A. ; To, Z. P. ; Whiting, R. L.

Springer

Neurochemical research 16 (1991), S. 95-103

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ISSN: 1573-6903

Keywords: Thyrotropin-releasing hormone ; TRH receptor ; TRH analogs ; CG3509 ; CG3703 ; RX77368 ; MK-771

Source: Springer Online Journal Archives 1860-2000

Topics: Medicine

Notes: Abstract [3H](3-Me-His2) thyrotropin-releasing hormone ([3H]MeTRH) bound to TRH receptors in rodent, rabbit and dog brain and spinal cord (SC), and in rat, sheep, bovine and dog anterior pituitary (PIT) glands, with high affinity (dissociation constants, Kds=5–9 nM; n=3–4) but to different densities of these sites (B max range 6–145 fmol/mg protein) (rabbit SC〉sheep PIT≫G.pig brain〉dog brain〉rat brain〉bovine and dog PIT). Various TRH analogs competitively inhibited [3H]MeTRH binding in these tissues with a similar rank order of potency: MeTRH〉TRH〉 CG3703≥RX77368≥MK-771〉TRH Glycinamide〉Glu1-TRH≫CG3509≥NVal2-TRH〉〉〉TRH free acid〉〉〉and cyclo-His-Pro, indicating a pharmacological similarity of CNS and pituitary TRH receptors. While most TRH analogs displaced [3H]MeTRH binding with a similar potency in the different species, TRH exhibited a 2-fold lower affinity in the rat and G.pig brain than in other tissues of other species. Similarly, CG3703 was 2.4–4.5 times more active in the rabbit brain than in the rodent and dog brain, and also more potent in the rabbit brain as compared to the sheep PIT. However, MK-771 and RX77368 had a similar affinity for the brain TRH receptors in the different species but RX77368 was 2-fold more active in the SC preparations and ≈3–4-fold less active in the sheep PIT when compared to the brain homogenates. RX 77368 exhibited the highest affinity for the dog PIT TRH receptor. In contrast, MK-771 showed a similar affinity for the brain, SC and PIT TRH receptor apart from in the rat PIT where it had the highest affinity. Similarly, TRH glycinamide was more active in the dog brain than rodent and rabbit brain. These data suggest that while the rank order of potency of TRH analogs is similar in the species examined, certain analogs appear to be more potent in certain tissues of some species than in others. In addition, the current results have shown that CG3703 is almost equipotent with RX77368 and MK-771 in most species but is substantially more active than its related analog, CG3509 in the brain, SC and PIT. Taken together, these observations may have some relevance to the future clinical applications of these metabolically stabilized TRH analogs.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1007/BF00965695

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