The manifestations of chronic insomnia undergo age-related changes. In younger infants and children, behavioral insomnia emerges as the most prevalent form and typically responds to behavioral interventions. However, distinct clusters of clinical presentations suggest the presence of various phenotypes, potentially implicating the primary involvement of specific neurotransmitters. These conceptualizations, coupled with genetic studies on pleiotropy and polygenicity, may aid in identifying individuals at risk of persistent insomnia into adulthood and shed light on novel treatment options. In school-age children, the predominant presentation is sleep-onset insomnia, often linked with nighttime fears, anxiety symptoms, poor sleep hygiene, limit-setting issues, and inadequate sleep duration. The manifestations of insomnia in adolescence correlate with the profound changes occurring in sleep architecture, circadian rhythms, and homeostatic processes. The primary symptoms during adolescence include delayed sleep onset, sleep misperception, persistent negative thoughts about sleep, and physiological hyperarousal—paralleling features observed in adult insomnia. An approach centered on distinct presentations may provide a framework for precision-based treatment options. Enhanced comprehension of insomnia's manifestations across diverse developmental stages can facilitate accurate assessment. Efforts to subtype insomnia in childhood align with this objective, potentially guiding the selection of appropriate treatments tailored to individual neurobiological, clinical, and familial features.

Individualized approaches to pediatric chronic insomnia: Advancing precision medicine in sleep disorders / Bruni, O.; Angriman, M.; Miano, S.; Delrosso, L. M.; Spruyt, K.; Mogavero, M. P.; Ferri, R.. - In: SLEEP MEDICINE REVIEWS. - ISSN 1087-0792. - 76:(2024). [10.1016/j.smrv.2024.101946]

Individualized approaches to pediatric chronic insomnia: Advancing precision medicine in sleep disorders

Bruni O.
Primo
;
2024

Abstract

The manifestations of chronic insomnia undergo age-related changes. In younger infants and children, behavioral insomnia emerges as the most prevalent form and typically responds to behavioral interventions. However, distinct clusters of clinical presentations suggest the presence of various phenotypes, potentially implicating the primary involvement of specific neurotransmitters. These conceptualizations, coupled with genetic studies on pleiotropy and polygenicity, may aid in identifying individuals at risk of persistent insomnia into adulthood and shed light on novel treatment options. In school-age children, the predominant presentation is sleep-onset insomnia, often linked with nighttime fears, anxiety symptoms, poor sleep hygiene, limit-setting issues, and inadequate sleep duration. The manifestations of insomnia in adolescence correlate with the profound changes occurring in sleep architecture, circadian rhythms, and homeostatic processes. The primary symptoms during adolescence include delayed sleep onset, sleep misperception, persistent negative thoughts about sleep, and physiological hyperarousal—paralleling features observed in adult insomnia. An approach centered on distinct presentations may provide a framework for precision-based treatment options. Enhanced comprehension of insomnia's manifestations across diverse developmental stages can facilitate accurate assessment. Efforts to subtype insomnia in childhood align with this objective, potentially guiding the selection of appropriate treatments tailored to individual neurobiological, clinical, and familial features.
2024
Cognitive-behavioral therapy; Drugs; Insomnia; Over-the-counter; Pediatric; Personalized medicine
01 Pubblicazione su rivista::01a Articolo in rivista
Individualized approaches to pediatric chronic insomnia: Advancing precision medicine in sleep disorders / Bruni, O.; Angriman, M.; Miano, S.; Delrosso, L. M.; Spruyt, K.; Mogavero, M. P.; Ferri, R.. - In: SLEEP MEDICINE REVIEWS. - ISSN 1087-0792. - 76:(2024). [10.1016/j.smrv.2024.101946]
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11573/1711761
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