Possible role of cyclic GMP in stimulus-secretion coupling by salt gland of the duck

Stimulation of salt galnd secretion in domestic ducks in vivo increased the cyclic GMP concentration of the tissue, but had no effect on cyclic AMP levels. Methacholine, which is known to stimulate sodium transport by the glands both in vivo and in vitro, stimulated ouabain-sensitive respiration in salt gland slices. Cyclic GMP stimulated ouabain-sensitive respiration to the same extent as methacholine. Guanylate cyclase stimulators, hydroxylamine and sodium azide, also stimulated ouabain-sensitive respiration. The stimulation of ouabain-sensitive respiration by methacholine was blocked either by atropine or by removal of calcium from the incubation medium. The stimulation of ouabain-sensitive respiration by cyclic GMP still occurred in the absence of calcium. The above observations seem to indicate that cyclic GMP acts as a tertiary link in the process of stimulus-secretion coupling in the tissue.

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EFFECT OF LUTEINIZING HORMONE ON THE CONCENTRATION OF CYCLIC GMP IN RABBIT OVARIES

Journal of Endocrinology ◽

10.1677/joe.0.0790251 ◽

1978 ◽

Vol 79 (2) ◽

pp. 251-252

Author(s):

V. V. PATWARDHAN ◽

A. LANTHIER

Keyword(s):

Luteinizing Hormone ◽

Cyclic Amp ◽

Cyclic Gmp ◽

Ovarian Tissue ◽

Chorionic Gonadotrophin ◽

Human Chorionic Gonadotrophin ◽

Direction Opposite ◽

Stimulation Of

Laboratoire d'Endocrinologie, Hôpital Notre-Dame et Département de Medicine, Université de Montréal, Montréal, Canada (Received 28 June 1978) Cyclic AMP has been implicated as an intermediate in some of the actions of luteinizing hormone (LH) on ovarian tissues, such as stimulation of steroidogenesis (LeMaire & Marsh, 1975). Both in vitro (Marsh, Butcher, Savard & Sutherland, 1966) and in vivo (Armstrong, Dorrington & Robinson, 1976), stimulation with LH results in a rapid increase in the amount of cyclic AMP in ovarian tissues, which precedes the LH-induced increase in steroidogenesis. Recently, studies on rat ovaries (Grinwich, Ham, Hichens & Behrman, 1976; Ratner, 1976; Ratner & Sanborn, 1976) have indicated that the ovarian tissue content of cyclic GMP may also be regulated by LH, but in a direction opposite to that of cyclic AMP. In the rabbit, Goff & Major (1975) have shown that administration of human chorionic gonadotrophin (HCG) causes a biphasic increase

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Prostacyclin as a potent effector of adipose-cell differentiation

Biochemical Journal ◽

10.1042/bj2570399 ◽

1989 ◽

Vol 257 (2) ◽

pp. 399-405 ◽

Cited By ~ 101

Author(s):

R Négrel ◽

D Gaillard ◽

G Ailhaud

Keyword(s):

Arachidonic Acid ◽

Cyclic Amp ◽

Critical Role ◽

Terminal Differentiation ◽

Prostaglandin F2 Alpha ◽

Adipogenic Effect ◽

Adipose Cells

The terminal differentiation of Ob1771 pre-adipose cells induced by arachidonic acid in serum-free hormone-supplemented medium containing insulin, transferrin, growth hormone, tri-iodothyronine and fetuin (5F medium) was strongly diminished in the presence of inhibitors of prostaglandin synthesis, namely aspirin or indomethacin. Carbaprostacyclin, a stable analogue of prostacyclin (prostaglandin I2) known to be synthesized by pre-adipocytes and adipocytes, behaved as an efficient activator of cyclic AMP production and was able, when added to 5F medium, to mimic the adipogenic effect of arachidonic acid. Prostaglandins E2, F2 alpha and D2, unable to affect the cyclic AMP production, failed to substitute for carbaprostacyclin. However, prostaglandin F2 alpha, which is another metabolite of arachidonic acid in pre-adipose and adipose cells, able to promote inositol phospholipid breakdown and protein kinase C activation, potentiated the adipogenic effect of carbaprostacyclin. In addition, carbaprostacyclin enhanced both a limited proliferation and terminal differentiation of adipose precursor cells isolated from rodent and human adipose tissues maintained in primary culture. These results demonstrate the critical role of prostacyclin and prostaglandin F2 alpha on adipose conversion in vitro and suggest a paracrine/autocrine role of both prostanoids in the development of adipose tissue in vivo.

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Polar head groups are important for barrier-protective effects of oxidized phospholipids on pulmonary endothelium

AJP Lung Cellular and Molecular Physiology ◽

10.1152/ajplung.00395.2006 ◽

2007 ◽

Vol 292 (4) ◽

pp. L924-L935 ◽

Cited By ~ 52

Author(s):

Anna A. Birukova ◽

Panfeng Fu ◽

Santipongse Chatchavalvanich ◽

Dylan Burdette ◽

Olga Oskolkova ◽

...

Keyword(s):

Protective Effects ◽

Oxidized Phospholipids ◽

Barrier Dysfunction ◽

Polar Head ◽

Cell Counts ◽

Head Groups ◽

Stimulation Of

We have previously described protective effects of oxidized 1-palmitoyl-2-arachidonoyl- sn-glycero-3-phosphocholine (OxPAPC) on pulmonary endothelial cell (EC) barrier function and demonstrated the critical role of cyclopentenone-containing modifications of arachidonoyl moiety in OxPAPC protective effects. In this study we used oxidized phosphocholine (OxPAPC), phosphoserine (OxPAPS), and glycerophosphate (OxPAPA) to investigate the role of polar head groups in EC barrier-protective responses to oxidized phospholipids (OxPLs). OxPAPC and OxPAPS induced sustained barrier enhancement in pulmonary EC, whereas OxPAPA caused a transient protective response as judged by measurements of transendothelial electrical resistance (TER). Non-OxPLs showed no effects on TER levels. All three OxPLs caused enhancement of peripheral EC actin cytoskeleton. OxPAPC and OxPAPS completely abolished LPS-induced EC hyperpermeability in vitro, whereas OxPAPA showed only a partial protective effect. In vivo, intravenous injection of OxPAPS or OxPAPC (1.5 mg/kg) markedly attenuated increases in the protein content, cell counts, and myeloperoxidase activities detected in bronchoalveolar lavage fluid upon intratracheal LPS instillation in mice, although OxPAPC showed less potency. All three OxPLs partially attenuated EC barrier dysfunction induced by IL-6 and thrombin. Their protective effects against thrombin-induced EC barrier dysfunction were linked to the attenuation of the thrombin-induced Rho pathway of EC hyperpermeability and stimulation of Rac-mediated mechanisms of EC barrier recovery. These results demonstrate for the first time the essential role of polar OxPL groups in blunting the LPS-induced EC dysfunction in vitro and in vivo and suggest the mechanism of agonist-induced hyperpermeability attenuation by OxPLs via reduction of Rho and stimulation of Rac signaling.

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Cytoplasmic Dynein Nucleates Microtubules to Organize Them into Radial Arrays In Vivo

Molecular Biology of the Cell ◽

10.1091/mbc.e03-10-0770 ◽

2004 ◽

Vol 15 (6) ◽

pp. 2742-2749 ◽

Cited By ~ 34

Author(s):

Viacheslav Malikov ◽

Anna Kashina ◽

Vladimir Rodionov

Keyword(s):

Cytoplasmic Dynein ◽

Exact Function ◽

Necessary And Sufficient ◽

Stimulation Of ◽

In Cells

Numerous evidence demonstrates that dynein is crucial for organization of microtubules (MTs) into radial arrays, but its exact function in this process is unclear. Here, we studied the role of cytoplasmic dynein in MT radial array formation in the absence of the centrosome. We found that dynein is a potent MT nucleator in vitro and that stimulation of dynein activity in cytoplasmic fragments of melanophores induces nucleation-dependent formation of MT radial array in the absence of the centrosome. This new property of dynein, in combination with its known role as an MT motor that is essential for MT array organization in the absence and presence of the centrosome, makes it a unique molecule whose activity is necessary and sufficient for the formation and maintenance of MT radial arrays in cells.

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216: Role of extracellular S100A4 in stimulation of melanoma cells crossing the blood–brain barrier in vitro and in vivo

European Journal of Cancer ◽

10.1016/s0959-8049(14)50187-6 ◽

2014 ◽

Vol 50 ◽

pp. S49

Author(s):

N. Herwig ◽

S. Wolf ◽

C. Haase-Kohn ◽

J. Steinbach ◽

J. Pietzsch

Keyword(s):

Blood Brain Barrier ◽

Melanoma Cells ◽

Brain Barrier ◽

Blood Brain ◽

Stimulation Of

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Overexpression of membrane metalloendopeptidase inhibits substance P stimulation of cholangiocarcinoma growth

AJP Gastrointestinal and Liver Physiology ◽

10.1152/ajpgi.00018.2014 ◽

2014 ◽

Vol 306 (9) ◽

pp. G759-G768 ◽

Cited By ~ 11

Author(s):

Fanyin Meng ◽

Sharon DeMorrow ◽

Julie Venter ◽

Gabriel Frampton ◽

Yuyan Han ◽

...

Keyword(s):

Substance P ◽

Functional Role ◽

Xenograft Model ◽

Subsequent Increase ◽

Proliferation In Vitro ◽

Proteolytic Product ◽

Stimulation Of

Substance P (SP) promotes cholangiocyte growth during cholestasis by activating its receptor, NK1R. SP is a proteolytic product of tachykinin (Tac1) and is deactivated by membrane metalloendopeptidase (MME). This study aimed to evaluate the functional role of SP in the regulation of cholangiocarcinoma (CCA) growth. NK1R, Tac1, and MME expression and SP secretion were assessed in human CCA cells and nonmalignant cholangiocytes. The proliferative effects of SP (in the absence/presence of the NK1R inhibitor, L-733,060) and of L-733,060 were evaluated. In vivo, the effect of L-733,060 treatment or MME overexpression on tumor growth was evaluated by using a xenograft model of CCA in nu/nu nude mice. The expression of Tac1, MME, NK1R, PCNA, CK-19, and VEGF-A was analyzed in the resulting tumors. Human CCA cell lines had increased expression of Tac1 and NK1R, along with reduced levels of MME compared with nonmalignant cholangiocytes, resulting in a subsequent increase in SP secretion. SP treatment increased CCA cell proliferation in vitro, which was blocked by L-733,060. Treatment with L-733,060 alone inhibited CCA proliferation in vitro and in vivo. Xenograft tumors derived from MME-overexpressed human Mz-ChA-1 CCA cells had a slower growth rate than those derived from control cells. Expression of PCNA, CK-19, and VEGF-A decreased, whereas MME expression increased in the xenograft tumors treated with L-733,060 or MME-overexpressed xenograft tumors compared with controls. The study suggests that SP secreted by CCA promotes CCA growth via autocrine pathway. Blockade of SP secretion and NK1R signaling may be important for the management of CCA.

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Ventral pallidal GABAergic neurons control wakefulness associated with motivation through the ventral tegmental pathway

Molecular Psychiatry ◽

10.1038/s41380-020-00906-0 ◽

2020 ◽

Author(s):

Ya-Dong Li ◽

Yan-Jia Luo ◽

Wei Xu ◽

Jing Ge ◽

Yoan Cherasse ◽

...

Keyword(s):

Dopaminergic Neurons ◽

Gabaergic Neurons ◽

Population Activity ◽

Lateral Habenula ◽

Optogenetic Stimulation ◽

Ventral Tegmental ◽

Stimulation Of

Abstract The ventral pallidum (VP) regulates motivation, drug addiction, and several behaviors that rely on heightened arousal. However, the role and underlying neural circuits of the VP in the control of wakefulness remain poorly understood. In the present study, we sought to elucidate the specific role of VP GABAergic neurons in controlling sleep–wake behaviors in mice. Fiber photometry revealed that the population activity of VP GABAergic neurons was increased during physiological transitions from non-rapid eye movement (non-REM, NREM) sleep to either wakefulness or REM sleep. Moreover, chemogenetic and optogenetic manipulations were leveraged to investigate a potential causal role of VP GABAergic neurons in initiating and/or maintaining arousal. In vivo optogenetic stimulation of VP GABAergic neurons innervating the ventral tegmental area (VTA) strongly promoted arousal via disinhibition of VTA dopaminergic neurons. Functional in vitro mapping revealed that VP GABAergic neurons, in principle, inhibited VTA GABAergic neurons but also inhibited VTA dopaminergic neurons. In addition, optogenetic stimulation of terminals of VP GABAergic neurons revealed that they promoted arousal by innervating the lateral hypothalamus, but not the mediodorsal thalamus or lateral habenula. The increased wakefulness chemogenetically evoked by VP GABAergic neuronal activation was completely abolished by pretreatment with dopaminergic D1 and D2/D3 receptor antagonists. Furthermore, activation of VP GABAergic neurons increased exploration time in both the open-field and light–dark box tests but did not modulate depression-like behaviors or food intake. Finally, chemogenetic inhibition of VP GABAergic neurons decreased arousal. Taken together, our findings indicate that VP GABAergic neurons are essential for arousal related to motivation.

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Influence of mechanical stretch on growth and protein turnover of rat uterus

AJP Endocrinology and Metabolism ◽

10.1152/ajpendo.1988.254.5.e543 ◽

1988 ◽

Vol 254 (5) ◽

pp. E543-E548 ◽

Cited By ~ 3

Author(s):

A. J. Douglas ◽

E. W. Clarke ◽

D. F. Goldspink

Keyword(s):

Mechanical Stretch ◽

Rat Uterus ◽

Dna Contents ◽

Extensive Growth ◽

A New Technique ◽

Rna And Dna ◽

Stimulation Of

A new technique has been developed and used to distend the uterus of nonpregnant rats for up to 5 days. Continuous distension of the saline-filled uterus induced rapid and extensive growth of the whole uterus and the myometrium by a combination of hyperplasia and hypertrophy. In both cases, 1 day after this imposition of mechanical stretch significant increases (25-50%) in the protein, RNA, and DNA contents were found, with larger changes (100-250%) being progressively expressed up to 5 days. This stretch-induced growth primarily results from a stimulation of protein synthesis (measured both in vivo and in vitro), with little or no change being evident in the rate of protein breakdown. These findings have been discussed in relation to the role of stretch in the growth of the uterus during pregnancy and stretch-induced responses found in other types of muscle.

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EFFECTS OF ACTH AND ITS O-NITROPHENYL SULPHENYL DERIVATIVE ON ADRENOCORTICAL FUNCTION IN VIVO

Acta Endocrinologica ◽

10.1530/acta.0.0820587 ◽

1976 ◽

Vol 82 (3) ◽

pp. 587-599 ◽

Cited By ~ 15

Author(s):

J. Ramachandran ◽

Y. C. Kong ◽

Susanna Liles

Keyword(s):

Cyclic Amp ◽

Adrenal Weight ◽

Adrenocortical Function ◽

Tryptophan Residue ◽

Adult Rats ◽

Corticosterone Concentration ◽

Hypophysectomized Rats ◽

Stimulation Of

ABSTRACT Both ACTH and NPS-ACTH in which the single tryptophan residue of the hormone is modified were able to stimulate adrenal corticosterone concentration to the same extent in hypophysectomized rats, although a higher dose of NPS-ACTH was required. ACTH stimulated adrenal cyclic AMP levels 120-fold in hypophysectomized rats whereas NPS-ACTH caused a marginal increase. In the case of ACTH, low doses of the hormone capable of producing maximal stimulation of corticosterone synthesis did not produce any detectable change in cyclic AMP concentration. The rates of secretion of corticosterone induced by ACTH and NPS-ACTH in vivo were the same. NPS-ACTH was found to be 1.2% as potent as ACTH. The role of cyclic AMP in adrenal repair was investigated by administering equipotent doses of ACTH or NPS-ACTH to hypophysectomized rats. In adult rats both failed to produce a significant increase in adrenal weight. Adrenal function (measured by responsiveness to exogenous ACTH in vitro) was restored by NPS-ACTH but not to the same degree as ACTH. In hypophysectomized weanling rats, ACTH produced a small but significant increase in adrenal weight but NPS-ACTH did not. These results suggest that an increase in adrenal cyclic AMP may not be obligatory for the stimulation of steroidogenesis by ACTH and that some of the trophic actions of the hormone may be mediated by cyclic AMP.

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Antagonists of the antidiuretic activity of vasopressin

AJP Renal Physiology ◽

10.1152/ajprenal.1988.254.2.f165 ◽

1988 ◽

Vol 254 (2) ◽

pp. F165-F177 ◽

Cited By ~ 4

Author(s):

L. B. Kinter ◽

W. F. Huffman ◽

F. L. Stassen

Keyword(s):

Water Excretion ◽

Water Handling ◽

Water Salt ◽

Renal Responses ◽

Renal Water Excretion ◽

Adh Activity ◽

Stimulation Of

Competitive antagonists of the antidiuretic (ADH) activity of vasopressin were first described some six years ago. When studied in vitro, ADH antagonists displace vasopressin from specific renal binding sites and antagonize, in a competitive fashion, vasopressin stimulation of adenylate cyclase and transepithelial water, salt, and urea fluxes. When studied in vivo, the ADH antagonists increase renal water excretion and antagonize, in a competitive fashion, the ADH activity of vasopressin. Marked species heterogeneity is apparent with ADH antagonists in vivo, and inconsistencies between in vitro and in vivo findings within the same species are reported. Other renal responses associated with administration of ADH antagonists include changes in renal hemodynamics and renal salt and urea excretion. The effects on salt excretion appear to be limited to those species in which vasopressin stimulation of epithelial salt reabsorption has been demonstrated. In summary, the role of vasopressin as the principal factor regulating renal water handling is supported by experience with ADH receptor antagonists. However, that experience also indicates the emerging significance of autocoids, and other synergistic factors, to affect ADH receptor/effector mechanisms and to modulate renal ADH responses.

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