Anti-inflammatory and antithrombotic effects of nicotine exposure in oral contraceptive-induced insulin resistance are glucocorticoid-independent

Lawrence Aderemi Olatunji; Olugbenga Samuel Michael; Oluwaseun Aremu Adeyanju; Emmanuel Damilare Areola; Ayodele Olufemi Soladoye

doi:10.1016/j.pharep.2016.12.010

Anti-inflammatory and antithrombotic effects of nicotine exposure in oral contraceptive-induced insulin resistance are glucocorticoid-independent

Pharmacol Rep. 2017 Jun;69(3):512-519. doi: 10.1016/j.pharep.2016.12.010. Epub 2016 Dec 19.

Authors

Lawrence Aderemi Olatunji¹, Olugbenga Samuel Michael², Oluwaseun Aremu Adeyanju², Emmanuel Damilare Areola², Ayodele Olufemi Soladoye²

Affiliations

¹ Cardiovascular Research Laboratory, Department of Physiology, College of Health Sciences University of Ilorin, Ilorin, Nigeria. Electronic address: tunjilaw@unilorin.edu.ng.
² Cardiovascular Research Laboratory, Department of Physiology, College of Health Sciences University of Ilorin, Ilorin, Nigeria.

PMID: 28349880
DOI: 10.1016/j.pharep.2016.12.010

Abstract

Background: Reports showed that estrogen-progestin oral contraceptive (COC) or tobacco smoking causes increased risk of cardiovascular diseases (CVD) in premenopausal women. Studies also suggest that nicotine, a major tobacco alkaloid, may worsen or improve atherothrombotic CVD. Altered hemorheology, prothrombotic and pro-inflammatory biomarkers, have been implicated in the development of atherothrombotic CVD events. However, the effect of non-smoking nicotine exposure on these biomarkers during COC treatment is not yet established. We therefore sought to determine the effects of nicotine exposure during COC treatment on these biomarkers, and also tested the hypothesis that the nicotine effects would be glucocorticoid-dependent.

Methods: Female Sprague-Dawley rats aged 10 weeks were given (po) vehicle, low-dose nicotine (0.1mg/kg) or high-dose nicotine (1.0mg/kg) with or without COC steroids (5.0μg/kg ethinylestradiol and 25.0μg/kg levonorgestrel) daily for 6 weeks.

Results: COC treatment or nicotine exposure led to increased insulin resistance (IR), hemorheological (blood viscosity, hematocrit and plasma viscosity), prothrombotic (plasminogen activator inhibitor-1), pro-inflammatory (uric acid, C-reactive protein, neutrophil/lymphocyte and platelet/lymphocyte ratios) biomarkers and corticosterone. However, these effects except that on corticosterone were abrogated by nicotine exposure during COC treatment.

Conclusions: Our study indicates that nicotine- or COC-induced IR may be mediated via inflammatory/thrombotic pathway. The results imply that nicotine exposure could impact negatively on atherothrombotic biomarkers in COC non-users, whereas the impact in COC users could be positive. The results also suggest that the anti-inflammatory, antithrombotic and blood viscosity-lowering effects of nicotine exposure during COC use is circulating glucocorticoid-independent.

Keywords: Atherothrombotic CVD; Corticosterone; Estrogen-progestin oral contraceptive; Proinflammatory biomarker.

MeSH terms

Animals
Anti-Inflammatory Agents / administration & dosage
Anti-Inflammatory Agents / pharmacology*
Blood Viscosity / drug effects
Contraceptives, Oral / administration & dosage
Contraceptives, Oral / toxicity*
Corticosterone / metabolism
Dose-Response Relationship, Drug
Drug Combinations
Ethinyl Estradiol / administration & dosage
Ethinyl Estradiol / toxicity
Female
Fibrinolytic Agents / administration & dosage
Fibrinolytic Agents / pharmacology
Glucocorticoids / metabolism
Insulin Resistance*
Levonorgestrel / administration & dosage
Levonorgestrel / toxicity
Nicotine / administration & dosage
Nicotine / pharmacology*
Nicotinic Agonists / administration & dosage
Nicotinic Agonists / pharmacology
Rats
Rats, Sprague-Dawley

Substances

Anti-Inflammatory Agents
Contraceptives, Oral
Drug Combinations
Fibrinolytic Agents
Glucocorticoids
Nicotinic Agonists
ethinyl estradiol, levonorgestrel drug combination
Ethinyl Estradiol
Levonorgestrel
Nicotine
Corticosterone