Mechanistic/mammalian target of rapamycin and side effects of antipsychotics: insights into mechanisms and implications for therapy

Zhuo, Chuanjun; Xu, Yong; Hou, Weihong; Chen, Jiayue; Li, Qianchen; Liu, Zhidong; Dou, Guangqian; Sun, Yun; Li, Ranli; Ma, Xiaoyan; Tian, Hongjun; Zhou, Chunhua

doi:10.1038/s41398-021-01778-w

Cited by 10 publications

(10 citation statements)

References 82 publications

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“…Third, SIRT1 and its deacetylation substrate, DNMT1, are both present in the most connected subnetwork and have a direct involvement in the regulation of p53 transcription. Finally, bibliographic evidence supports the proposed pathway in four aspects: (i) the implication of p53/MDM2 in the multidrug resistance process [80][81][82][83], (ii) the involvement of p53 in autophagy, a process known to be related to antipsychotic response [92][93][94][95]; (iii) the observed dysregulations of this pathway in schizophrenia patients [96][97][98], and (iv) the relationship of this pathway to negative symptoms, such as memory, learning ability impairment [99], and major depression [100].…”

Section: A Molecular Model For Treatment Resistant Schizophreniamentioning

confidence: 62%

MiRNA Differences Related to Treatment-Resistant Schizophrenia

Pérez-Rodríguez

Penedo

Rivera-Baltanás

et al. 2023

IJMS

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Schizophrenia (SZ) is a serious mental disorder that is typically treated with antipsychotic medication. Treatment-resistant schizophrenia (TRS) is the condition where symptoms remain after pharmacological intervention, resulting in long-lasting functional and social impairments. As the identification and treatment of a TRS patient requires previous failed treatments, early mechanisms of detection are needed in order to quicken the access to effective therapy, as well as improve treatment adherence. In this study, we aim to find a microRNA (miRNA) signature for TRS, as well as to shed some light on the molecular pathways potentially involved in this severe condition. To do this, we compared the blood miRNAs of schizophrenia patients that respond to medication and TRS patients, thus obtaining a 16-miRNA TRS profile. Then, we assessed the ability of this signature to separate responders and TRS patients using hierarchical clustering, observing that most of them are grouped correctly (~70% accuracy). We also conducted a network, pathway analysis, and bibliography search to spot molecular pathways potentially altered in TRS. We found that the response to stress seems to be a key factor in TRS and that proteins p53, SIRT1, MDM2, and TRIM28 could be the potential mediators of such responses. Finally, we suggest a molecular pathway potentially regulated by the miRNAs of the TRS profile.

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Section: A Molecular Model For Treatment Resistant Schizophreniamentioning

confidence: 62%

MiRNA Differences Related to Treatment-Resistant Schizophrenia

Pérez-Rodríguez

Penedo

Rivera-Baltanás

et al. 2023

IJMS

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“…mTORC1 activation interferes with lipid and energy metabolism, leading to the upregulation of lipid biosynthesis and the accumulation of TGs. Furthermore, activation of the mTOR pathway inhibits autophagy, thereby increasing intracellular lipid accumulation ( Zhuo et al, 2022 ). Enhanced mTOR activity disrupts hepatic lipid homeostasis by regulating the expression of the transcription factor SREBP-1c ( Takashima et al, 2009 ).…”

Section: Mechanisms Of Sga-induced Disorders Of Lipid Metabolism Medi...mentioning

confidence: 99%

The regulatory effects of second-generation antipsychotics on lipid metabolism: Potential mechanisms mediated by the gut microbiota and therapeutic implications

et al. 2023

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Second-generation antipsychotics (SGAs) are the mainstay of treatment for schizophrenia and other neuropsychiatric diseases but cause a high risk of disruption to lipid metabolism, which is an intractable therapeutic challenge worldwide. Although the exact mechanisms underlying this lipid disturbance are complex, an increasing body of evidence has suggested the involvement of the gut microbiota in SGA-induced lipid dysregulation since SGA treatment may alter the abundance and composition of the intestinal microflora. The subsequent effects involve the generation of different categories of signaling molecules by gut microbes such as endogenous cannabinoids, cholesterol, short-chain fatty acids (SCFAs), bile acids (BAs), and gut hormones that regulate lipid metabolism. On the one hand, these signaling molecules can directly activate the vagus nerve or be transported into the brain to influence appetite via the gut–brain axis. On the other hand, these molecules can also regulate related lipid metabolism via peripheral signaling pathways. Interestingly, therapeutic strategies directly targeting the gut microbiota and related metabolites seem to have promising efficacy in the treatment of SGA-induced lipid disturbances. Thus, this review provides a comprehensive understanding of how SGAs can induce disturbances in lipid metabolism by altering the gut microbiota.

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“…mTORC1 is key in promoting anabolism and suppressing catabolism . Zhou et al have extensively reviewed the literature demonstrating that mTOR signaling is crucial in the pathogenesis of SGA-induced side effects, including metabolic abnormalities . Olanzapine, an SGA, has been reported to extensively affect hepatic mTORC, thereby disrupting autophagy, lipid homeostasis, and insulin sensitivity, all of which could lead to dysregulation of the metabolism.…”

Section: Cracking the Code: All Roads Lead To Mtorcmentioning

confidence: 99%

“…Enhanced peripheral levels of glutamate have also been observed upon switching from conventional antipsychotics to olanzapine . Besides, mTORC1 is an enhancer of hepatic lipid biosynthesis by increasing the expression and phosphorylation of sterol regulatory binding-element protein 1 (SREBP-1c), a protein upregulated after treatment with olanzapine. ,, This evidence suggests that mTORC, especially mTORC1, could be a significant culprit to consider in SGA-induced metabolic syndrome.…”

Section: Cracking the Code: All Roads Lead To Mtorcmentioning

confidence: 99%

Modulation of Leucine Sensors to Mitigate Antipsychotics-Induced Metabolic Syndrome: A New Vista

Arjmand,

Biojone,

Wegener

2023

ACS Pharmacol. Transl. Sci.

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Second-generation antipsychotics (SGAs) are currently the mainstay in the pharmacotherapy of some psychiatric disorders, which have improved the quality of life of millions of patients globally. A broad spectrum of activity and diminished liabilities of extrapyramidal side effects have made SGAs better alternatives compared to first-generation antipsychotics. Nevertheless, they display a complex profile of activity by affecting an array of biological targets and, as a result, are associated with a constellation of metabolic abnormalities such as hyperglycemia, dyslipidemia, weight gain, and cardiovascular problems. The SGAsinduced metabolic syndrome's exact mechanism has remained nebulous, but some evidence points the finger at mTOR signaling. In this viewpoint, we propose potential strategies to prevent or alleviate the SGA-induced metabolic adverse effects by modulating the activity of the leucine sensors, Sestrins.

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Mechanistic/mammalian target of rapamycin and side effects of antipsychotics: insights into mechanisms and implications for therapy

Cited by 10 publications

References 82 publications

MiRNA Differences Related to Treatment-Resistant Schizophrenia

MiRNA Differences Related to Treatment-Resistant Schizophrenia

The regulatory effects of second-generation antipsychotics on lipid metabolism: Potential mechanisms mediated by the gut microbiota and therapeutic implications

Modulation of Leucine Sensors to Mitigate Antipsychotics-Induced Metabolic Syndrome: A New Vista

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