Abstract
Background: Suicide is a major public health problem on a global scale, with about 800.000 deaths every year. In particular, it represents one of the main causes of death among adolescents and young adults aged between 15 and 29 years. The World Health Organization (WHO) describes suicide as “an act of deliberate killing” and that is placed at the extreme end of the continuous spectrum of suicidal behaviors (SBs). These include suicidal ideation, attempted suicide and suicide itself.
Objective: The aim of the present review was to better clarify the suicide vulnerability genetic biomarkers and genetic variants correlated with the response to lithium and clozapine and to evaluate some correspondences.
Methods: We reviewed the current literature, focusing our attention on genetic molecular studies about neurobiological systems involved in SBs and pharmacogenetic studies about antisuicidal drugs (lithium and clozapine).
Results: The studies that we have reviewed have shown mixed results. Interestingly, rs1800532 polymorphism of the SLC6A4 gene, encoding for the serotonin transporter, is potentially correlated with both suicide vulnerability and a poor response to lithium and clozapine.
Conclusion: Due to the impact of suicide on public health, more studies are needed to open a promising route to prevent suicide in personalized and precise psychiatry.
Keywords: Suicide, genes, genetic polymorphisms, neurobiological systems, lithium, clozapine.
Current Pharmaceutical Design
Title:Suicide and Genetic Biomarkers: Toward Personalized Tailored-treatment with Lithium and Clozapine
Volume: 27 Issue: 30
Author(s): Domenico De Berardis*, Federica Vellante, Mauro Pettorruso, Lorenza Lucidi, Antonio Tambelli, Ilenia Di Muzio, Giulia Gianfelice, Antonio Ventriglio, Michele Fornaro, Gianluca Serafini, Maurizio Pompili, Giampaolo Perna, Silvia Fraticelli, Giovanni Martinotti and Massimo di Giannantonio
Affiliation:
- National Health Service, Department of Mental Health, Psychiatric Service of Diagnosis and Treatment, 'G. Mazzini' Hospital, Piazza Italia 1, 64100 Teramo,Italy
Keywords: Suicide, genes, genetic polymorphisms, neurobiological systems, lithium, clozapine.
Abstract:
Background: Suicide is a major public health problem on a global scale, with about 800.000 deaths every year. In particular, it represents one of the main causes of death among adolescents and young adults aged between 15 and 29 years. The World Health Organization (WHO) describes suicide as “an act of deliberate killing” and that is placed at the extreme end of the continuous spectrum of suicidal behaviors (SBs). These include suicidal ideation, attempted suicide and suicide itself.
Objective: The aim of the present review was to better clarify the suicide vulnerability genetic biomarkers and genetic variants correlated with the response to lithium and clozapine and to evaluate some correspondences.
Methods: We reviewed the current literature, focusing our attention on genetic molecular studies about neurobiological systems involved in SBs and pharmacogenetic studies about antisuicidal drugs (lithium and clozapine).
Results: The studies that we have reviewed have shown mixed results. Interestingly, rs1800532 polymorphism of the SLC6A4 gene, encoding for the serotonin transporter, is potentially correlated with both suicide vulnerability and a poor response to lithium and clozapine.
Conclusion: Due to the impact of suicide on public health, more studies are needed to open a promising route to prevent suicide in personalized and precise psychiatry.
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Cite this article as:
De Berardis Domenico *, Vellante Federica , Pettorruso Mauro , Lucidi Lorenza, Tambelli Antonio, Di Muzio Ilenia , Gianfelice Giulia , Ventriglio Antonio , Fornaro Michele , Serafini Gianluca, Pompili Maurizio , Perna Giampaolo, Fraticelli Silvia, Martinotti Giovanni and di Giannantonio Massimo, Suicide and Genetic Biomarkers: Toward Personalized Tailored-treatment with Lithium and Clozapine, Current Pharmaceutical Design 2021; 27 (30) . https://dx.doi.org/10.2174/1381612827666210603143353
DOI https://dx.doi.org/10.2174/1381612827666210603143353 |
Print ISSN 1381-6128 |
Publisher Name Bentham Science Publisher |
Online ISSN 1873-4286 |
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