Membrane Permeation by Multidrug-resistance-modulators and Non-modulators: Effects of Hydrophobicity and Electric Charge

Castaing, Madeleine; Brouant, Pierre; Loiseau, Alain; Santelli‐Rouvier, Christiane; Santelli, Maurice; Alibert, Sandrine; Mahamoud, Abdallah; Barbe, Jacques

doi:10.1211/0022357001773977

Cited by 30 publications

(26 citation statements)

References 27 publications

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“…Moreover, pretreatment with nifedipine, an MDR PGP inhibitor, prevents the hippocampal GR upregulation induced by antidepressants (Przegalinski et al, 1993). Inhibition of PGP and other membrane steroid transporters is not receptor mediated and is related to the drugs' physiochemical properties, that is, lipophilicity, electric charge, and ability to accept hydrogen bonds (Ford, 1996;Castaing et al, 2000;Ekins et al, 2002).…”

Section: Discussionmentioning

confidence: 99%

The Antidepressant Clomipramine Regulates Cortisol Intracellular Concentrations and Glucocorticoid Receptor Expression in Fibroblasts and Rat Primary Neurones

Pariante

Hye

Williamson

et al. 2003

Neuropsychopharmacol

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Incubation of LMCAT fibroblasts cells with antidepressants potentiates glucocorticoid receptor (GR)-mediated gene transcription in the presence of cortisol, but not of corticosterone. We have suggested that antidepressants do so by inhibiting the LMCAT cells membrane steroid transporter and thus by increasing cortisol intracellular concentrations. We now confirm and extend this model to primary neuronal cultures. Clomipramine, a tricyclic antidepressant, increased the intracellular accumulation of 3 H-cortisol, but not 3 Hcorticosterone, in LMCAT cells (+80%) and primary rat neurones (+20%). The latter finding is the first demonstration that a membrane steroid transporter is present in neurones. Moreover, verapamil, a membrane steroid transporter inhibitor, reduced the effects of clomipramine on the intracellular accumulation of 3 H-cortisol in LMCAT cells. Finally, clomipramine also decreased GR expression (whole-cell Western blot) in LMCAT cells (50% reduction) and primary rat neurones (80% reduction). This GR downregulation can explain the reduced GR-mediated gene transcription previously described under experimental conditions that do not elicit the effects on the LMCAT cells steroid transporter. This work further supports the hypothesis that membrane steroid transporters regulating the access of glucocorticoids to the brain in vivo are a fundamental target for antidepressant action.

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Section: Discussionmentioning

confidence: 99%

The Antidepressant Clomipramine Regulates Cortisol Intracellular Concentrations and Glucocorticoid Receptor Expression in Fibroblasts and Rat Primary Neurones

Pariante

Hye

Williamson

et al. 2003

Neuropsychopharmacol

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“…Further work has clarified that most antidepressants, including SSRI's, enhance cortisol action in the brain and periphery by inhibiting membrane steroid transporters that regulate the intracellular concentration of cortisol, principally by expelling cortisol from the cell (Pariante et al, 1997(Pariante et al, , 2003aWeiss et al, 2003). Although membrane steroid transporter inhibition has been shown to occur independently of glucocorticoid-receptor mediation, and instead, is affected directly by the physiochemical properties of antidepressants (Ford, 1996;Castaing et al, 2000;Ekins et al, 2002), this action could result in an augmentation of negative feedback inhibition of the HPA axisFan effect consistent with the reversal of at least one known perturbation in MDDFreduced negative feedback inhibition (Nemeroff, 1996;Holsboer, 2000;McQuade and Young, 2000).…”

Section: Introductionmentioning

confidence: 99%

Effect of Sertraline on Glucocorticoid Sensitivity of Mononuclear Leukocytes in Post-Traumatic Stress Disorder

Yehuda

Yang

Golier

et al. 2005

Neuropsychopharmacol

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This study examined the effects of sertraline (SER) on glucocorticoid sensitivity in mononuclear leukocytes (MNL) from eight subjects with current post-traumatic stress disorder (PTSD) and nine comparison subjects. In all, 60 ml of blood was withdrawn by venipuncture at 0800, and MNL were isolated from blood and divided into two portions: the first contained live cells incubated with a series of concentrations of dexamethasone (DEX); the second contained cells incubated with similar concentrations of DEX þ 2 mM SER. Group difference in the concentrations of DEX required to inhibit lysozyme activity by 50% were evaluated under conditions of DEX-only and DEX þ SER using analysis of covariance (ANCOVA). A significant Group Â Condition interaction reflected that SER altered the lysozyme IC 50-DEX in the direction of decreasing sensitivity to glucocorticoids in PTSD while having no uniform effect in cells from comparison subjects. The data provide support for the idea that glucocorticoid receptors might be more responsive to antidepressants in PTSD than in persons without PTSD. Insofar as increased sensitivity to glucocorticoids has been linked with PTSD, the actions of SER on the lysozyme IC 50-DEX suggest that this medication may target a biologic alteration associated with PTSD pathophysiology.

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“…By this way, membrane permeability could be increased. In a study, it was reported that calmodulin antagonists such as clomipramine and thioridazine, calcium channel blocker such as verapamil, beta adrenergic receptor blocker, propranolol and also antiparasitic agents like quinine are very effective whereas steroids and antineoplastic agents are not effective in influencing the membrane permeability (Castaing et al, 2000). Furthermore, bioactive sphingolipid levels are also altered in anticancer drug-resistant cancer cells (Ogretmen & Hannun, 2004).…”

Section: Alterations In Membrane Lipidsmentioning

confidence: 99%

Molecular mechanisms of drug resistance and its reversal in cancer

Yandım

Adan-Gokbulut

Baran

2015

Critical Reviews in Biotechnology

277

178

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Chemotherapy is the main strategy for the treatment of cancer. However, the main problem limiting the success of chemotherapy is the development of multidrug resistance. The resistance can be intrinsic or acquired. The resistance phenotype is associated with the tumor cells that gain a cross-resistance to a large range of drugs that are structurally and functionally different. Multidrug resistance arises via many unrelated mechanisms, such as overexpression of energy-dependent efflux proteins, decrease in uptake of the agents, increase or alteration in drug targets, modification of cell cycle checkpoints, inactivation of the agents, compartmentalization of the agents, inhibition of apoptosis and aberrant bioactive sphingolipid metabolism. Exact elucidation of resistance mechanisms and molecular and biochemical approaches to overcome multidrug resistance have been a major goal in cancer research. This review comprises the mechanisms guiding multidrug resistance in cancer chemotherapy and also touches on approaches for reversing the resistance.

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Membrane Permeation by Multidrug-resistance-modulators and Non-modulators: Effects of Hydrophobicity and Electric Charge

Cited by 30 publications

References 27 publications

The Antidepressant Clomipramine Regulates Cortisol Intracellular Concentrations and Glucocorticoid Receptor Expression in Fibroblasts and Rat Primary Neurones

The Antidepressant Clomipramine Regulates Cortisol Intracellular Concentrations and Glucocorticoid Receptor Expression in Fibroblasts and Rat Primary Neurones

Effect of Sertraline on Glucocorticoid Sensitivity of Mononuclear Leukocytes in Post-Traumatic Stress Disorder

Molecular mechanisms of drug resistance and its reversal in cancer

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