Sertraline: Difference between revisions

Sertraline, marketed as Zoloft, is the most widely prescribed psychiatric medicine in the United States, accounting for roughly 40 million prescriptions annually as of recent years. It is the second selective serotonin reuptake inhibitor brought to market, approved by the United States Food and Drug Administration on 30 December 1991 and launched by Pfizer as Zoloft in the first quarter of 1992.^[3] It was discovered at Pfizer Central Research in Groton, Connecticut by a team led by the biochemist Kenneth Koe and the chemist Willard Welch, who in 1977 reopened a compound series their employer had previously discarded. Sertraline carries the broadest FDA-approved indication set of any SSRI, covering major depressive disorder, obsessive-compulsive disorder, panic disorder, posttraumatic stress disorder, social anxiety disorder, and premenstrual dysphoric disorder; it is also widely prescribed off-label for generalized anxiety disorder, where multiple international guidelines recommend it as a first-line choice.

The compound that became sertraline emerged from a Pfizer compound series that had been discarded. In the early 1970s the Pfizer chemist Reinhard Sarges synthesized a series of psychoactive tetrahydronaphthalenamines whose initial members, including lometraline, were modeled on the structural skeletons of the neuroleptics thiothixene and pinoxepin. Further work on the series produced tametraline, a norepinephrine and weaker dopamine reuptake inhibitor. Tametraline was set aside because its candidates produced an undesired stimulant effect in animals. In 1977 the biochemist Kenneth Koe took an interest in the discarded series and proposed that it might be modified to act selectively on serotonin reuptake rather than on the catecholamines. Koe and the chemist Willard Welch synthesized a second generation of compounds incorporating chlorine substituents on the phenyl ring. One of the otherwise inactive cis-analogs proved to be a serotonin reuptake inhibitor; Welch then prepared the stereoisomers, and the animal behavioral scientist Albert Weissman performed the in vivo screening that identified the most potent and selective candidate, the (1S,4S)-cis enantiomer of N-methyl-4-(3,4-dichlorophenyl)-1,2,3,4-tetrahydro-1-naphthylamine. The team published the founding paper on the compound, then designated sertraline, in 1983.^[3] The discovery was characterized at the time as emerging from a working group that operated outside Pfizer's mainstream research priorities, without a formal project team, and that had to overcome internal company reluctance to pursue sertraline because Pfizer was simultaneously considering licensing an antidepressant candidate from another firm.

Koe's biographical arc is worth recording. He was born in 1925 to Chinese immigrant parents in Astoria, Oregon. The family moved to Portland, where he attended Lincoln High School and washed dishes at the Hung Far Low restaurant in the city's Chinatown district to help support the family. He won a full scholarship to Reed College, completed a master's degree at the University of Washington, and earned his doctorate at the California Institute of Technology. He joined Pfizer in 1955, initially working on antibiotics in the company's Brooklyn laboratory, and was at Pfizer Central Research in Groton, Connecticut when the sertraline work took place. He died in 2015.

Sertraline reached the Food and Drug Administration as the second SSRI to be reviewed, four years behind Lilly's fluoxetine. The FDA approved sertraline for major depressive disorder on 30 December 1991 on the recommendation of the Psychopharmacological Drugs Advisory Committee; the medicine had already been available in the United Kingdom for a year by that point. The FDA approval was a closer call than the medicine's eventual commercial success would suggest. The treatment effect on outpatients with depression was characterized during committee discussion as modest, the effect on inpatients had not differed from placebo, and the trial design had been criticized for a 40 percent dropout rate that materially weakened the validity of the results. The committee nonetheless reached consensus that the medicine was safe and effective.^[4]

Pfizer launched sertraline as Zoloft in the first quarter of 1992. Subsequent FDA approvals expanded the indication list: obsessive-compulsive disorder in adults (1996), panic disorder (1997), posttraumatic stress disorder (1999, the first SSRI approved for PTSD), premenstrual dysphoric disorder (2002), pediatric OCD (2002), and social anxiety disorder (2003). Sertraline carries the broadest FDA-approved indication set of any SSRI. In 2003 the United Kingdom's Medicines and Healthcare products Regulatory Agency advised that, apart from fluoxetine, SSRIs were not suitable for treating depression in patients under 18, though sertraline retained its UK approval for pediatric OCD. In 2005 the FDA added a boxed warning to all antidepressants concerning increased risk of suicidal ideation and behavior in patients under 25; the warning was expanded in 2007 to include young adults aged 18 to 24.

Pfizer's US patent on sertraline expired in June 2006. Generic versions became available immediately, with Teva, Roxane, and several other manufacturers entering the market in the months that followed. Zoloft had been Pfizer's seventh-best-selling medicine in its final patent year, with sales of approximately $3.1 billion. The transition to generic supply reduced the cost per pill substantially without disrupting prescribing patterns; sertraline remained the leading SSRI through the 2010s and into the 2020s. Roughly 40 million prescriptions for sertraline were dispensed in the United States in 2019, and prescribing has continued to rise, with sertraline ranking as the most prescribed psychiatric medicine and the eleventh most prescribed medicine of any kind in the United States. The branded Zoloft franchise was transferred from Pfizer to Viatris following the Upjohn spinoff in 2020 and is now marketed under that label.

The serotonergic framing under which sertraline was discovered, marketed, and prescribed reflects the dominant model of depression pharmacology in the 1980s and 1990s. That framing has not aged uniformly well. The acute pharmacological action of sertraline, blockade of the serotonin transporter, occurs within hours, while the clinical antidepressant response classically requires weeks; the gap is the central puzzle in the modern mechanistic literature. The most consequential recent challenge to the orthodox account is the PANDA trial, a 655-patient pragmatic primary-care randomized controlled trial led by Gemma Lewis and colleagues and published in 2019. PANDA found that sertraline did not significantly reduce depression scores at six weeks in primary care patients with depressive symptoms, regardless of baseline severity or duration; secondary outcomes (anxiety, quality of life, self-rated mental health) did show improvement.^[5] The PANDA finding is consistent with the larger 21-drug network meta-analysis by Cipriani and colleagues showing modest absolute effects across the antidepressant class.^[4] Work in the 2000s and 2010s on BDNF-TrkB signaling and synaptic plasticity, and the 2021 demonstration by Casarotto and colleagues that fluoxetine and several other antidepressants bind directly to the TrkB neurotrophin receptor,^[6] have moved the field toward a mechanistic account in which SERT inhibition is the initiating event but downstream effects on neuronal plasticity are the therapeutically active mechanism.^[7] The page treats SERT inhibition as the canonical claim and the BDNF-TrkB account as the contemporary working model; the mechanism field above reflects this.

Sertraline is a prescription-only medicine in the United States; it is not a scheduled controlled substance. It is on the World Health Organization's Model List of Essential Medicines and is broadly available as a low-cost generic in essentially all major markets worldwide. + Add a problem

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• Anxiolysis👤 no reports yet⚕️ no reports yetRate×

  Classically starting at 3-4 weeks and improving for another 8-12.
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  Common, especially first 1-2 weeks. Take with food.
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  More common with sertraline than other SSRIs and dose-dependent; often improves over 2-4 weeks.
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  Reported in roughly two-thirds of men on sertraline versus ~18% before treatment.
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  Historically associated with SSRIs.
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  Some patients; consider morning dosing.
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  Other patients; consider evening dosing.
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  Recognized association with SSRIs broadly.
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Absorption

Oral bioavailability is not precisely characterized in humans (intravenous sertraline has not been administered for absolute bioavailability measurement). Absorption is essentially complete, with extensive first-pass metabolism limiting systemic availability. Peak plasma concentrations occur between 4.5 and 8.4 hours post-dose. Concomitant food modestly increases peak plasma levels and total exposure. Steady-state is reached within approximately one week of continuous dosing.^[8]

Distribution

Plasma protein binding is approximately 98.5%, primarily to alpha-1 acid glycoprotein and albumin. Volume of distribution is approximately 20 L/kg. Sertraline crosses the blood-brain barrier readily.^[8]

Metabolism

Sertraline undergoes extensive hepatic metabolism by N-demethylation, predominantly via CYP2C19 in vivo with secondary contribution from CYP2B6; CYP2C9, CYP3A4, and CYP2D6 also contribute. The principal metabolite, N-desmethylsertraline, is approximately 10- to 50-fold weaker than the parent compound as a serotonin reuptake inhibitor and is not thought to contribute meaningfully to clinical effect.^[8] CYP2C19 poor metabolizers have approximately 2.7-fold higher sertraline exposure than normal metabolizers, and intermediate metabolizers approximately 1.4-fold higher,^[9] with dose-relevant implications particularly in East Asian populations where CYP2C19 poor metabolism is more common. Sertraline itself is a moderate inhibitor of CYP2D6 (weaker than fluoxetine or paroxetine) and a moderate inhibitor of CYP2B6.^[10]

Elimination

Elimination is renal and biliary in approximately equal proportions (40-45% each), almost entirely as metabolites. Less than 0.2% of an oral dose is recovered unchanged in urine; approximately 12-14% of a dose appears unchanged in feces.^[8]

Sertraline inhibits the serotonin transporter (SERT) with high affinity (Ki 0.15-3.3 nM) and high selectivity over the norepinephrine transporter (Ki 420-925 nM). The dopamine transporter (DAT) is bound at intermediate affinity (Ki 22-315 nM); at doses of 200 mg daily and above, sertraline occupies approximately 20% of DAT receptors in human imaging studies, an effect that distinguishes it from other SSRIs and may contribute to motivational and cognitive effects. Sertraline is also an antagonist at sigma-1 receptors (Ki 32-57 nM in rat tissue). Affinity at histamine, acetylcholine, GABA, and benzodiazepine receptors is negligible. The acute mechanism, blockade of synaptic 5-HT reuptake, does not by itself explain the delayed clinical response, which classically begins at 2-4 weeks and continues to improve for 2-3 months. The contemporary mechanistic account places downstream effects on BDNF-TrkB signaling and synaptic plasticity at the center of the antidepressant response; on this view, SERT inhibition is the initiating event but not the therapeutically active one.^[7][6]

Sertraline has additional in vitro and ex vivo activities that have generated active research interest but whose clinical significance remains uncertain: REDD1-dependent mTOR inhibition with autophagy induction, antifungal activity (particularly against Candida species), antiparasitic effects against Leishmania and Trypanosoma species, and photosensitizing activity against some bacteria. None of these is part of the medicine's approved use; they are noted here for completeness.

The clinically important interactions for prescribers:

• MAO inhibitors and pimozide: contraindicated. Combination with non-selective MAOIs (isocarboxazid, phenelzine, tranylcypromine) or with linezolid or intravenous methylene blue may produce serotonin syndrome, which can be life-threatening. A 14-day washout is required in both directions. Combination with pimozide is contraindicated because of QT-prolongation risk.
• Methadone: sertraline increases methadone plasma levels by approximately 26% over six weeks via CYP2B6 inhibition, with stereoselective accumulation of the (S)-methadone enantiomer that carries the QT-prolongation risk.^[11] Clinically significant; monitor when starting sertraline in methadone-maintained patients.
• Lithium: combined use produced tremor in 35% of subjects in a placebo-controlled study (vs 0% on placebo). No specific contraindication, but warn the patient and monitor for tremor.
• Bupropion: sertraline inhibits CYP2B6, which metabolizes bupropion. The interaction is minor and clinically used combinations (sertraline plus bupropion for antidepressant augmentation, or for sexual-side-effect rescue) generally do not require dose adjustment.
• Proton pump inhibitors: esomeprazole (a CYP2C19 inhibitor) raises sertraline levels by approximately 40%. Common combination in primary care; consider lower sertraline starting dose or slower titration when initiating sertraline in patients on esomeprazole or omeprazole.
• NSAIDs, antiplatelets, anticoagulants: increased bleeding risk due to SSRI inhibition of platelet serotonin uptake. Consider gastric protection in patients on combined SSRI + NSAID + steroid.
• Tamoxifen, codeine, tramadol, metoprolol: sertraline is a moderate CYP2D6 inhibitor (weaker than fluoxetine or paroxetine but not negligible). Tamoxifen efficacy depends on CYP2D6 activation to endoxifen; sertraline is among the less problematic SSRIs in this context but is not preferred. Codeine analgesia depends on CYP2D6 activation; sertraline blunts this. Tramadol carries both a CYP2D6-substrate consideration and a serotonergic-toxicity consideration.
• Warfarin: small clinically uncertain effect on INR. Monitor INR more frequently when starting or stopping sertraline.
• Levothyroxine: sertraline may decrease the efficacy of levothyroxine through an incompletely characterized mechanism. Monitor TSH when starting sertraline in patients on thyroid replacement.

  Pregnancy and lactation

Sertraline is among the most extensively studied SSRIs in pregnancy, and the modern evidence base is broadly reassuring once depression and other confounders are accounted for. The largest and most rigorously confounding-adjusted study is the Huybrechts and colleagues 2014 cohort in the New England Journal of Medicine, which examined 949,504 Medicaid-enrolled pregnancies and was specifically designed to address concerns about a sertraline-cardiac-defect association. Unadjusted analyses showed a modest excess of cardiac defects in antidepressant-exposed pregnancies; once the analysis was restricted to women with depression and adjusted with propensity scores for severity of illness and other confounders, the association with major cardiac malformations was no longer statistically significant.^[12] Older meta-analyses that pooled mostly unadjusted cohorts have reported a 29-42% increased odds of congenital heart defects and a roughly 2.7-fold increase in septal defects with first-trimester sertraline exposure,^[13][14] but these estimates are largely attenuated by the better-adjusted evidence and should be interpreted with caution. The absolute risk is low. Use late in the third trimester may produce a neonatal adaptation syndrome (jitteriness, feeding difficulties, respiratory distress) lasting days to a few weeks. Untreated depression in pregnancy carries its own substantial risks for mother and infant. Sertraline is excreted in breast milk at low levels and is generally considered the first-choice SSRI in lactation. On the present evidence, sertraline is one of the preferred SSRIs for use in pregnancy and in breastfeeding. Boxed warning: monitor closely for worsening mood, suicidal ideation, and behavioral activation, especially during the first weeks of treatment, with any dose change, and particularly in patients under age 25. No routine laboratory monitoring required. Baseline weight, blood pressure, and a review of bleeding risk (particularly with concurrent NSAIDs or anticoagulants) are reasonable. Hyponatremia (SIADH) is a recognized risk in older patients; consider checking sodium if symptoms suggest it. For patients on methadone, consider serum methadone monitoring after starting sertraline. For patients on warfarin, monitor INR more frequently when starting or stopping. For patients on levothyroxine, monitor TSH at the next routine check. Watch for emergent manic or hypomanic symptoms throughout treatment and treat new rapid mood elevation, agitation, or pressured speech as a possible bipolar switch.

Before starting: screen for a personal or family history of bipolar disorder. Sertraline, like all antidepressants, can precipitate a manic or mixed switch in patients with bipolar diathesis; new activation or rapid mood elevation on treatment should be evaluated as a possible switch rather than treated as a side effect to wait out. Boxed warning: counsel patients (and family members, where appropriate) about the increased risk of suicidal ideation and behavioral activation in patients under 25, and ask them to contact you promptly with any worsening mood, intrusive thoughts of self-harm, agitation, irritability, or unusual behavioral changes, particularly in the first weeks of treatment and after any dose change.

Take with food to reduce nausea and improve absorption. Initial activation, insomnia, or anxiety in the first 1-2 weeks is common and usually self-limited. Sexual side effects are common and often persistent during treatment; persistent symptoms after discontinuation (PSSD) are reported with all SSRIs. Discontinuation should be tapered over weeks to months; sertraline's discontinuation syndrome is milder than with paroxetine or venlafaxine but more pronounced than with fluoxetine, and common symptoms include dizziness, insomnia, anxiety, agitation, and irritability lasting up to several weeks. The oral concentrate contains alcohol and must be diluted before administration; it is contraindicated in patients taking disulfiram. Avoid alcohol initially; once stable, modest use is reasonable for most patients. Patients on methadone should be told the sertraline may raise their methadone levels modestly and to report sedation or breathing changes.

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Fluoxetine, Escitalopram, Paroxetine, Duloxetine, Methadone