Higher S100B Levels Predict Persistently Elevated Anhedonia with Escitalopram Monotherapy Versus Antidepressant Combinations: Findings from CO-MED Trial

Jha, Manish K.; Minhajuddin, Abu; Gadad, Bharathi S.; Fatt, Cherise Chin; Trivedi, Madhukar H.

doi:10.3390/ph12040184

Cited by 11 publications

(8 citation statements)

References 40 publications

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“…Regarding inflammatory markers and their association with the antidepressant response, we found an inverse significant correlation between basal CRP levels and treatment response at week 4 but not at week 8. This is consistent with reports suggesting that elevated inflammatory markers, such as CRP, IL-1β, IL-6, IL-17, and TNF-α, predict poor antidepressant outcomes ( Baune et al, 2010 ; Jha et al, 2017 , 2018 ; Miller et al, 2017 ; Benedetti et al, 2021 ). However, baseline CRP levels did not predict treatment response at either week 4 or 8 by simple or multiple linear regression analysis.…”

Section: Discussionsupporting

confidence: 92%

“…Nevertheless, serum S100B levels are indicative of CSF concentrations even though extracranial sources secreted S100B (e.g., adipocytes) might interfere with the accurate interpretation of serum levels ( Reiber et al, 2001 ; Ambrée et al, 2016 ). As it was shown in a previous work, S100B levels displayed important value dispersion, generating a non-normal statistical distribution ( Jha et al, 2019 ). Results from the present study are compatible with this previous observation, being in the same range of values although with less data dispersion.…”

Section: Discussionsupporting

confidence: 54%

“…Supporting our results, previous studies have reported that high baseline S100B levels predict treatment response. Using different patient groups (i.e., melancholic/non-melancholic MDD), type of antidepressant treatments (serotoninergic, noradrenergic, dopaminergic) and assessment instruments (i.e., Hamilton Depression rating Scale), and endpoints (from 4 weeks to 6 months), 3 of 4 studies plead for a predictive effect of baseline S100B for antidepressant response ( Arolt et al, 2003 ; Jang et al, 2008 ; Ambrée et al, 2016 ; Jha et al, 2019 ). A recent meta-analysis of the 3 first studies that included 51 responders and 73 non-responders found that S100B levels at baseline were significantly elevated in responders ( Shi et al, 2020 ).…”

Section: Discussionmentioning

confidence: 99%

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High S100B Levels Predict Antidepressant Response in Patients With Major Depression Even When Considering Inflammatory and Metabolic Markers

Navinés

Oriolo

Horrillo

et al. 2022

International Journal of Neuropsychopharmacology

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Background The relationship between antidepressant response and glial, inflammatory, and metabolic markers is poorly understood in depression. This study assessed the ability of biological markers to predict antidepressant response in major depressive disorder (MDD). Methods We included 31 MDD outpatients treated with escitalopram or sertraline for 8 consecutive weeks. The Montgomery-Asberg Depression Rating Scale (MADRS) was administered at baseline and at week 4 and 8 of treatment. Concomitantly, blood samples were collected for the determination of serum S100B, CRP, and HDL-C levels. Treatment response was defined as ≥50% improvement in the MADRS score from baseline to either week 4 or 8. Variables associated with treatment response were included in a linear regression model as predictors of treatment response. Results Twenty-seven patients (87%) completed 8 weeks of treatment; 74% and 63% were responders at week 4 and 8, respectively. High S100B and low HDL-C levels at baseline were associated with better treatment response at both time-points. Low CRP levels were correlated with better response at week 4. Multivariate analysis showed that high baseline S100B levels and low baseline HDL-C levels were good predictors of treatment response at week 4 (R 2=0.457, p=0.001), while S100B was at week 8 (R 2=0.239, p=0.011). Importantly, baseline S100B and HDL-C levels were not associated with depression severity and did not change over time with clinical improvement. Conclusions Serum S100B levels appear to be a useful biomarker of antidepressant response in MDD even when considering inflammatory and metabolic markers.

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Section: Discussionsupporting

confidence: 92%

Section: Discussionsupporting

confidence: 54%

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

High S100B Levels Predict Antidepressant Response in Patients With Major Depression Even When Considering Inflammatory and Metabolic Markers

Navinés

Oriolo

Horrillo

et al. 2022

International Journal of Neuropsychopharmacology

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“…Emerging evidence highlights the role of immune response as a key factor in MDs. Immunological biomarkers seem to be related to illness progression and to treatment effectiveness; several studies suggest strong associations among IL-6, TNFa, S100b, IL 1b, and PCR with affective or schizophrenic disorders [ 6 , 7 , 8 , 9 , 10 , 11 ]. Yuan et al (2019) evaluated the meta-analysis considering inflammatory markers in mental disorders.…”

Section: Introductionmentioning

confidence: 99%

IL-33 in Mental Disorders

et al. 2021

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Mental disorders are common in the general population; every year about 25% of the total European population is affected by a mental condition. The prevalence of psychiatric disorders might be underestimated. Emerging evidence highlights the role of immune response as a key factor in MDs. Immunological biomarkers seem to be related to illness progression and to treatment effectiveness; several studies suggest strong associations among IL-6, TNFa, S100b, IL 1b, and PCR with affective or schizophrenic disorders. The purpose of this review is to examine and to understand the possible link between mental disorders and interleukin 33 to clarify the role of this axis in the immune system. We found 13 research papers that evaluated interleukin 33 or interleukin 31 levels in subjects affected by mental disorders. Eight studies investigated cytokines in affective disorders. Three studies measured levels of IL-33 in schizophrenia and two studies focused on patients affected by autism spectrum disorders. Alterations in brain structure and neurodevelopmental outcome are affected by multiple levels of organization. Disorders of the autoimmune response, and of the IL-33/31 axis, may therefore be one of the factors involved in this process. These results support the evidence that alarmins, particularly the IL-33/31 axis, need more consideration among researchers and practitioners.

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“…As far as we know, this was the rst study that investigated the effect of escitalopram on BBB integrity. On the other hand, there is a study that evidenced that BBB dysfunction results in poorer less response to escitalopram treatment (Jha et al 2019). It is worth mentioning that escitalopram was able to reverse the depressive-like behavior and the gut in ammation induced by a colitis protocol in ovariectomized rats, suggesting a potential anti-in ammatory effect of escitalopram (Abdo et al 2019).…”

Section: Discussionmentioning

confidence: 98%

Sex Differences in the Brain-Blood Barrier in Rats Exposed to Early life Stress and the Treatment with Antidepressants and Psychobiotic

Botelho

Carlessi

Manosso

et al. 2021

Preprint

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Major depressive disorder is a debilitating mental disorder. Although the etiology is not fully understood, the impairment to the blood-brain barrier (BBB) integrity may be involved. Maternal deprivation was performed in the first 10 postnatal days for 3h/day. Male and female rats were divided into control and maternal deprivation. Maternal deprivation animals were subdivided and received treatment with saline, escitalopram, ketamine, or probiotic. The integrity of BBB was evaluated in the prefrontal cortex and hippocampus at postnatal days 11, 21, 41, and 61. Maternal deprivation caused BBB breakdown in the prefrontal cortex and hippocampus in female and male rats in all ages evaluated, except in the prefrontal cortex of females at postnatal day 41. In females, escitalopram, ketamine, and probiotic reversed BBB breakdown in all ages evaluated, except probiotic at postnatal day 21 (prefrontal cortex), and ketamine at postnatal days 21 and 41 (hippocampus). In males, escitalopram, ketamine, and probiotic reversed BBB breakdown in the prefrontal cortex in all ages evaluated, except escitalopram at postnatal days 41 and 61. In the hippocampus of males, BBB damage was reversed by escitalopram at postnatal day 21 and ketamine at postnatal day 41. Treatment with escitalopram, ketamine, or probiotics can prevent changes in the BBB integrity, depending on the age and sex of the animal. Clinically it is important to evaluate different treatments depending on age and sex.

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Higher S100B Levels Predict Persistently Elevated Anhedonia with Escitalopram Monotherapy Versus Antidepressant Combinations: Findings from CO-MED Trial

Cited by 11 publications

References 40 publications

High S100B Levels Predict Antidepressant Response in Patients With Major Depression Even When Considering Inflammatory and Metabolic Markers

High S100B Levels Predict Antidepressant Response in Patients With Major Depression Even When Considering Inflammatory and Metabolic Markers

IL-33 in Mental Disorders

Sex Differences in the Brain-Blood Barrier in Rats Exposed to Early life Stress and the Treatment with Antidepressants and Psychobiotic

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