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Letter to the Editor in Response to ‘Population-based cohort study of oral contraceptive use and risk of depression’

Published online by Cambridge University Press:  01 February 2024

P. Kendall*
Affiliation:
Department of Obstetrics and Gynecology, Division of Family Planning, University of Colorado School of Medicine, Aurora, CO, USA
A. Lazorwitz
Affiliation:
Women’s Reproductive Health Research Scholar, Department of Obstetrics and Gynecology, Division of Family Planning, University of Colorado Anschutz Medical Campus, Aurora, CO, USA
*
Corresponding author: P. Kendall; Email: [email protected]
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Abstract

Type
Letter to the Editor
Creative Commons
Creative Common License - CCCreative Common License - BY
This is an Open Access article, distributed under the terms of the Creative Commons Attribution licence (http://creativecommons.org/licenses/by/4.0), which permits unrestricted re-use, distribution and reproduction, provided the original article is properly cited.
Copyright
© The Author(s), 2024. Published by Cambridge University Press.

Dear Editor-in-Chief,

We read with interest the article by Johansson et al. published first online on 12 June 2023 in Epidemiology and Psychiatric Sciences (Johansson et al., Reference Johansson, Vinther Larsen, Bui, Ek, Karlsson and Johansson2023). In this population-based cohort study, the authors evaluated for a causal relationship between depression and oral contraceptive (OC) use. While the authors included data from over 250,000 participants from the UK Biobank with extensive data points, the authors failed to adequately address two major limitations of their study: (1) reported OC use primarily from the 1970s and 1980s with outdated OC preparations and (2) no acknowledgment of a potential ‘nocebo’ effect.

OCs have changed dramatically over the decades since the first pill became available in 1961 (Dhont, Reference Dhont2010). As the authors mentioned, the majority of combined oral contraceptives (COCs) available in the United Kingdom during the majority of reported OC use in this study included 100–150 μg of the second-generation progestin, levonorgestrel, in combination with 20, 30 or 50 μg of ethinylestradiol. Levonorgestrel, a derivative of 19-nortestosterone, has one of the highest affinities for the progesterone receptor among progestins, but likewise also one of the highest affinities for the androgen receptor, leading to increased androgenic side effects (Dhont, Reference Dhont2010). Subsequently developed third- and fourth-generation progestins have anti-androgenic properties while maintaining beneficial properties such as potency and longer half-lives, making COC formulations containing third- and fourth-generation progestins better options for the vast majority of patients today (Dhont, Reference Dhont2010). While the exact relationship between OC and mood is poorly understood, the results of several studies have suggested that the androgenicity of the progestin in a COC may be the most influential factor (Schaffir et al., Reference Schaffir, Worly and Gur2016). Randomized trials have demonstrated higher rates of adverse mood symptoms among patients taking a pill with levonorgestrel compared to patients taking pills containing either desogestrel, a third-generation progestin, or drospirenone, a fourth-generation progestin (Kelly et al., Reference Kelly, Davies, Fearns, McKinnon, Carter, Gerlinger and Smithers2010; Sangthawan and Taneepanichskul, Reference Sangthawan and Taneepanichskul2005; Schaffir et al., Reference Schaffir, Worly and Gur2016; Shahnazi et al., Reference Shahnazi, Khalili, Kochaksaraei, Jafarabadi, Banoi, Nahaee and Payan2014). Further, the authors do not distinguish between the use of progestin-only OCs or COCs in their analyses. Progestin-only OCs were available during the time frame of this cohort study, and yet the authors provide no justification for lumping non-oestrogen containing OC formulations with oestrogen-containing formulations, despite the hypothesized effect of oestrogens on mood symptoms.

Finally, as first introduced by Grimes and Schulz in 2011, we know that placebo-controlled randomized trials have actually demonstrated that many mood-related symptoms reported by OC users are due to a ‘nocebo’ effect (Grimes and Schulz, Reference Grimes and Schulz2011). As patients prescribed OCs are counselled to expect adverse mood symptoms, they then experience higher rates of these adverse side effects (Grimes and Schulz, Reference Grimes and Schulz2011). As such, the appropriate comparison group for evaluating side effects, including mood disorders, due to OC use is a true placebo group (users of inert pills) and not a never OC user group as utilized by the authors.

We fully support the evaluation of safety and side-effects with hormonal contraceptive options as these studies can improve patient counselling. Unfortunately, research that demonstrates increased risks of side effects with hormonal contraceptive use, especially mood disorders, must be scientifically rigorous to avoid unnecessary public backlash and patient avoidance of reliable contraceptive options. We applaud the efforts by Johansson et al. to tackle this difficult area of research but must express caution in generalizing the findings from this study to more modern OC formulations, and these findings must be put into the context of the known ‘nocebo’ effect with hormonal contraception.

Sincerely,

Paige Kendall, MD

Aaron Lazorwitz, MD, PhD, MSCS

Financial support

This research received no specific grant from any funding agency, commercial or not-for profit sectors.

Competing interests

The authors declare none.

References

Dhont, M (2010) History of oral contraception. The European Journal of Contraception & Reproductive Health Care 15(Sup 2), S12S18.CrossRefGoogle ScholarPubMed
Grimes, DA and Schulz, KF (2011) Nonspecific side effects of oral contraceptives: Nocebo or noise? Contraception 83(1), 59.CrossRefGoogle ScholarPubMed
Johansson, T, Vinther Larsen, S, Bui, M, Ek, WE, Karlsson, T and Johansson, Å (2023) Population-based cohort study of oral contraceptive use and risk of depression. Epidemiology & Psychiatric Sciences 32, .CrossRefGoogle ScholarPubMed
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