Abstract
Multiple sclerosis (MS) is primarily a disease diagnosed in young and middle-aged adults. Although MS is a rare condition in pediatric age, an increasing rate of patients is diagnosed under the age of 18. The disabling nature of the disease cannot be reduced only to physical symptoms. Several additional symptoms such as cognitive impairment, fatigue, and psychological symptoms are common features of pediatric MS. The reviewed literature suggests that, despite the lower physical disability, children and adolescents diagnosed with MS are vulnerable to cognitive impairment even in the early stage of the disease. The neuropsychological profile of pediatric MS may resemble that of adult MS, including an impairment in attention/information processing speed, learning, verbal, and visuospatial memory. However, cognitive difficulties in children and adolescents are more likely to involve also general intelligence and linguistic abilities, presumably due to patients’ younger age and cognitive growth stage. Cognitive difficulties, beyond physical disability and relapses, may have a considerable impact on learning and school achievement. Depression and fatigue are other highly prevalent disturbances in pediatric MS and may contribute to patients’ low functional outcomes. Overall, these manifestations may cause considerable functional impairment on daily activities and quality of life that may require individualized rehabilitative treatment and extensive psychosocial care. Additional neuropsychological research evaluating larger samples, using more homogenous methods, and exploring the role of MS treatment on cognitive and psychological development is required.
Similar content being viewed by others
Avoid common mistakes on your manuscript.
Introduction
Multiple sclerosis (MS) is a chronic, unpredictable, inflammatory disease that affects the central nervous system [1]. It is characterized by lesions in the brain and spinal cord that may lead to both physical and cognitive impairment [2]. Although MS is usually considered an adult disease (adult-onset multiple sclerosis (AOMS)), approximately 3–5% of all patients with MS experience their first demyelinating episode before the age of 18 (pediatric-onset multiple sclerosis (POMS)) [3, 4]. The incidence and prevalence of pediatric MS are not completely known. It has been estimated that the overall prevalence and incidence of POMS may range respectively from 0.7 to 26.9 and from 0.05 to 2.85 per 100,000 children a year [3]. The sex distribution (female/male) of POMS is relatively equivalent in prepubertal children, while in post-puberty, the distribution shows a more pronounced female dominance, similar to AOMS [3]. This marked female disparity with age suggests a possible connection between the onset of menstruation and disease expression.
Pediatric MS may show different clinical presentations according to age at onset. While younger children (< 11 years old) often show multifocal symptoms, patients aged > 12 years, as the adults, usually have a monosymptomatic onset [3]. The most common clinical presentations in childhood are optic neuritis (ON), transverse myelitis (TM), and acute demyelinating encephalomyelitis (ADEM) [5]. In particular, ADEM at onset occurs more often in children under 10 years [5]. At onset, children very often show brainstem symptoms (25–41%), sphincter dysfunction, motor problems (30%), and sensory disturbances (15–30%) [4]. Younger patients with MS are also more likely to show cerebellar dysfunction [6]. POMS has a highly inflammatory course and is clinically more active than AOMS [6]. Most children (over 90%) are diagnosed as having relapsing–remitting form and show a higher relapse rate compared to AOMS, especially during the first 2 years [3, 6]. Due to the greater plasticity in the developing nervous tissue and the higher myelin repair ability, pediatric patients have better relapse recovery with less neurologic impairment [7, 8]. Pediatric patients have a slower progression of disability [9]. However, they reach a significant disability earlier in adult life (as early as the third decade of life) than patients with AOMS [9, 10].
The disabling nature of the disease cannot be reduced only to physical symptoms. Several additional symptoms such as cognitive impairment, fatigue, and psychological symptoms are common features of MS [7]. Overall, these manifestations may cause considerable functional impairment on daily and social activities, academic achievement, and quality of life that may require individualized rehabilitative treatment and extensive psychosocial care [7, 11, 12]. Given the unpredictability of the disease course and its heterogeneous features, MS has a potential impact not only on patients’ cognitive and psychological development, but it may also lead to longstanding adaptive problems involving the entire family functioning.
Considering that childhood and adolescence are critical periods for appropriate educational attainment, social and personal growth, an analysis of the impact of the disease on patients is essential for an appropriate management.
Aims
The aim of this narrative review article was to provide an extensive and up-to-date perspective of the impact of MS on affected children and adolescents. In particular, we investigated the current literature on neuropsychological impairment of children and adolescents who suffer from this disease, attempting to describe their long-term neuropsychological profile. In order to better understand patients’ global needs, we investigated the current literature data on common symptoms associated with MS such as fatigue, psychiatric comorbidity, and the impact of the disease on patients’ quality of life (QoL).
This review provides a comprehensive and current perspective on the impact of MS on children and adolescents affected by MS. Our paper contributes to the literature by offering an extensive and up-to-date exploration of the neuropsychological impact of the disease on children and adolescents. By delving into long-term effects, including fatigue, psychiatric comorbidities, and the impact of MS on quality of life, our paper enriches the understanding of pediatric MS. Beyond contributing to the current understanding of multiple sclerosis in this age cohort, this work establishes a robust framework for future studies and targeted interventions. Our results underscore the critical need for appropriate management and comprehensive care for POMS patients during these pivotal developmental stages, emphasizing the necessity of tailored interventions to address their cognitive and psychological challenges.
Methods
In this narrative review, the research of appropriate papers was carried out using MEDLINE and Web of Science. Our research considered studies published up to February 2023. We considered only papers published in English language. Search terms included “Pediatric Multiple Sclerosis” or “Pediatric Onset Multiple Sclerosis” and “Cognitive impairment”, “Cognitive performance” or “Neuropsychology”, “Attention”, “Memory”, “Language”, “Processing speed” and “Intelligence”. Moreover, we included in our research “Social cognition”, “Psychiatric comorbidity”, “Fatigue”, and “Quality of life”. Our search included patients of an age ranging from 0 to 18 years. We considered also articles involving adult patients diagnosed before 18 years old. Observational, prospective, and retrospective studies were analyzed as well as clinical trials and multicentric studies (Fig. 1).
Flow diagram of the study methodology
Results
Cognitive impairment
Cognitive impairment and neuropsychological dysfunctions are common and debilitating symptoms of MS [2]. It is assumed that cognitive dysfunction is not a late symptom of progressed MS, but it may be already detected even in the early stage of the disease [13, 14]. Cognitive dysfunctions have been found in all MS phases and may occur even in a pre-clinical stage or in the absence of major physical dysfunction [8, 15]. Moreover, research on both adult and pediatric age evidenced that low performance in selected cognitive domains may predict relapse and also disability progression [16].
Due to the onset of the disease during a crucial period for central nervous system maturation and development, pediatric patients with MS may be particularly vulnerable to cognitive impairment [7, 17, 18].
So far, there is lack of specific consensus on the assessment tools to be used, and the definition of cognitive impairment shows a large variability among several studies (Table 1) [7]. Despite this heterogeneity, research data consistently showed that approximately one third of patients under 18 years show cognitive impairment [7, 13, 16, 19]. The neuropsychological profile of pediatric MS may resemble that of adult MS, including an impairment in attention/information processing speed, learning, verbal, and visuospatial memory [7, 19]. However, cognitive difficulties in children and adolescents are more likely to involve also general intelligence and linguistic abilities, presumably due to patients’ younger age and cognitive growth stage [8, 17, 20,21,22].
In an early study [23], Kalb et al. described low intelligence performance, weakened verbal fluency, and perceptual motor difficulties among a small sample of patients with MS (n = 9). This early study, however, did not explore other cognitive functions commonly affected in adults, such as memory and attention. Several years later, MacAllister et al. examined the neuropsychological profile of 37 pediatric patients with MS [22]. Cognitive impairment, defined as a performance falling 1.5 or more standard deviation below normative range on at least two cognitive tasks, was found in one third of patients (35.1%). Moreover, 59% of patients had a low performance on at least one neuropsychological test. The most impaired domains were complex attention (e.g., rapidly shifting attention between competing stimuli) (29.7%) and delayed recall of verbal and visual information (respectively, 18.9% and 11%). Language abilities were frequently affected, with low performances in naming (18.9%) and receptive language (13.5%) [22]. The study described an association between cognitive functioning and the total disease duration, total number of relapses and disability (measured by Expanded Disability Status Scale, EDSS).
These studies, however, were limited by the lack of a matched control group. In a multicenter study, Amato et al. compared the neuropsychological functioning of pediatric patients diagnosed with MS (n = 63) with that of a control healthy group (n = 57), confirming the vulnerability to cognitive impairment in MS group [24]. The neuropsychological evaluation showed significant cognitive impairment (defined by scores falling below the 5th percentile of healthy control on at least three tests) in 19 patients (31%), whereas 32 patients (53%) showed a failure at least in two tests. As in other studies, prominent weakness was found in memory, attention, information processing speed, and executive functions. Exploring the global intelligence profile, the authors found lower scores in MS group in both verbal and performance IQ. In particular, the neuropsychological profile was characterized by low performance in verbal comprehension and, in a lower degree, semantic and phonemic fluency, thus confirming the peculiar impairment in language [24]. Among the possible variables associated with the low cognitive skills in these patients, the only significant predictor was the IQ score in the inferior range (lower than 90) which, in turn, was related to younger age at onset [24]. These findings were confirmed by Till et al., who described a reduction of attention and processing speed (38%), visuomotor integration (23.5%), and expressive vocabulary abilities in MS group compared with control group [25]. Moreover, the study showed an association between higher IQ and older age at disease onset, shorter MS duration and lower EDSS. Using a computerized neurocognitive battery, a more recent study demonstrated reduced accuracy on tests of attention/inhibition, visuospatial processing working memory and verbal memory (after adjusting for response time), in adolescents and young adults with POMS, compared with healthy control [26]. On the other hand, the absence of significant differences between cognitive performances among pediatric patients compared with a control healthy group was described in a recent study by Krupp et al. [27]. When compared with a group of adult patients with MS, the pediatric sample showed a better performance. A higher repair ability and better relapse recovery have been suggested as causal mechanisms.
However, beyond the age-conferred resilience, differences in the study groups could explain the discrepancies in comparison to older studies [28, 29]. In particular, patients in Krupp et al. study had shorter disease duration and were almost all (93%) treated with disease modifying therapies (50% using high efficacy drugs). These results support the role of DMT in improving the disability progression outcomes in individuals recently diagnosed [30].
Results on the influence of clinical factors on cognitive impairment are inconsistent and far from being conclusive [7]. Although a consistent body of research in POMS described lower cognitive performance in patients with neurological disability [13, 14, 25], other studies have shown a weak relationship between cognitive dysfunctions and the level of disability, indicating that low cognitive skills may occur independently from neurological disability [7, 11, 21]. Some authors supposed that cognitive functioning may be considered an early marker of disease activity and a prognostic factor for disease progression. Interestingly, cognitive decline can even predict the presence of structural abnormalities in the magnetic resonance imaging (MRI) [31].
The role of age of onset and disease duration on cognitive decline is still debated. In recent years, an increasing body of research examined the long-term evolution of cognitive functioning in pediatric MS, but the results are still inconclusive, showing heterogeneous outcomes over the time [7, 32,33,34]. A growing body of research showed higher risk of cognitive impairment in adults with POMS [28, 35].
Banwell et al. compared a small group of children with recent (disease onset within 12 months of testing; n = 3) and remote first MS attack (n = 7) [36]. The study demonstrated not only a cognitive decline on at least one test in all patients (n = 10) but also a higher risk of neuropsychological impairment in children with longer disease duration and younger age at onset. These findings were in accordance with two later studies of MacAllister et al. who reported a worsening of cognitive performance, in particular attention and memory, even in a relatively short time interval [14, 22]. Moreover, the authors highlighted the role of the disease duration, disability, and total number of relapses on cognitive disturbances [22]. In a 2-year follow-up study by Öztürk et al. [37], the authors observed a high percentage of cognitive impairment in pediatric patients with MS (47.8%), with significant differences with a control healthy group. The most affected skills were non-verbal reasoning and attention/concentration. Exploring the main clinical factors associated with the cognitive performance, the authors found that age at disease onset and EDSS appeared as important factors predicting cognitive functions. A 15-month follow-up by Till et al. showed that, although most patients had a relatively stable cognitive performance, healthy controls were more likely to have improvement in multiple cognitive domains [38]. A deterioration in cognitive skills, defined as significant decline on three or more tests, was found in 25% of patients as compared to only 3.8% of controls. The most commonly impaired skills were spelling, verbal fluency, visual memory, processing speed, and calculation. Longer disease duration was associated with greater deterioration in visuomotor integration. These findings led the authors to suppose that the cognitive decline of pediatric MS patients could be attributable to a lack expected maturational trajectory compared with healthy peers. While cognitive deterioration appears to be relatively frequent in pediatric MS, some studies evidenced little changes or even an improvement in cognitive skills over the time. In a follow-up of 1.8 months involving 383 patients with POMS or clinically isolated syndrome (CIS), Wallach et al. found that most patients (85.9%) did not show clinically meaningful change in processing speed [13]. Impaired processing speed occurred in 14.1% of POMS at the second assessment (14.0% of CIS). Factors associated with clinically neuropsychological decline included older age at MS onset and male gender. A low incidence of cognitive decline was also described by Charvet et al. [39], who found a relatively stable impairment from baseline (37% of patients) to follow-up (33%) (mean interval of 1.64 years) in a pediatric population of 62 MS and 5 CIS patients.
Heterogeneous results emerged over time in a 12-year-long follow-up by Portaccio et al. [15]. In a cohort of patients with MS assessed at 4 time points (baseline, 2, 5, and 12 years), a global worsening of cognitive performance was noticed at year 2, while there was an improvement at years 5 and 12 (with no significant variation between them). The most impaired domain was the verbal learning, with 41.9% of the sample showing difficulties in these skills. In disagreement to other studies, both disease duration and age of onset did not impact neuropsychological functioning. Higher clinical disease activity before the baseline evaluation was predictive of cognitive worsening. The study described the role of cognitive reserve against neuropsychological deterioration. Indeed, having an IQ ≥ 90 at baseline and a lower number of relapses in 2 years before the baseline were associated with better cognitive performances.
Social cognition
Social cognition refers to a complex set of mental processes necessary to perceive, process, and interpreter social stimuli and the environment [40]. One essential domain of social cognition is the Theory of Mind (ToM), which is defined as the ability to understand others’ mental state and ascribe intents, desires, and beliefs of others [40]. Over the last decades, a growing body of research explored social cognition in several neurodegenerative conditions, evidencing defective social cognition, in particular emotional processing and ToM [40]. Data investigating social cognition in MS patients are sparse [40, 41]. To the best of our knowledge, only three studies included patients with POMS. In a pilot study, Charvet et al. evidenced that social cognition may be an area of cognitive functioning affected in POMS population [40]. Comparing a group of 28 patients with POMS with 32 healthy controls, the authors found worse scores on ToM tasks in patients. In particular, lower performance in both cognitive and affective domains of ToM was found. Results on the affective task were similar to those emerged in other clinical disorders (i.e., psychiatric impairment). The impairment in ToM was not influenced by low cognitive abilities suggesting that, in pediatric MS, these deficits may be independent. The clinical factors showing a weak to moderate negative correlation with ToM were the total number of relapses and a longer history of disease. In 2018, Neuhaus et al. confirmed low social cognition abilities in pediatric patients with MS, but no correlation with both disease duration and EDSS was found [41]. Moreover, these authors described a particular impairment of complex social situations and facial affect recognition. More recently, Massano et al. compared classical and social cognition in 30 patients with POMS with two groups of patients with AOMS: the first matched for disease duration, and the second matched for age [42]. While the study confirmed the frequent cognitive impairment in POMS, no difference emerged in ToM skills between patients with POMS and AOMS. However, analyzing ToM abilities according to the age of MS onset, the authors found significant lower performances in patients with age of disease onset ≤ 15 years.
Psychiatric comorbidity
Psychiatric comorbidity in patients with MS was initially noticed by Charcot, who described hallucinations, depression, and mania among other manifestations of the disease [43]. Despite a large body of research on adults with MS, data on pediatric age are so far limited. However, an increasing number of studies suggest that psychiatric disorders may be common also in pediatric MS [7, 15, 19, 20, 44, 45]. In an early study by MacAllister et al. on pediatric patients with MS, nearly half of the patients who underwent a psychiatric evaluation received a formal diagnosis, most of them suffering from anxiety and/or depression [22]. The high prevalence of anxiety and mood disorders in pediatric patients with MS was confirmed in later studies. In 2010, Goretti et al. observed that about 30% of pediatric MS cases fulfilled criteria for a formal diagnosis of affective disorders which included anxiety, panic, major depression, and bipolar disorders [45]. On the other hand, on a self-report questionnaire exploring depression symptoms, only 17% of the patients had scores in the clinical range. The authors supposed that self-report inventories could be not sufficiently sensitive to detect subclinical psychiatric symptoms and highlighted the importance of structured interviews for a more precise evaluation of affective disorders in children and adolescents. Aiming at investigating the prevalence and risk factors associated with emotional and behavioral outcomes in adolescents with MS, Till et al. evaluated a sample of 31 pediatric patients with MS and 31 healthy subjects [12]. Compared with controls, patients more frequently showed problems of lower self-reliance and inattention/hyperactivity. Although a significant difference was not found, the adolescents with MS showed also elevated symptoms of anxiety (31%), depression, and somatization (24.1%). Similar results emerged from the parents, who described elevated symptoms of depression (29%), but also difficulties in adaptive behavior and somatization. The study also examined how emotional and behavioral functioning related with clinical factors. Psychosocial outcomes were not associated with brain lesion volume, IQ, disease duration, or number of relapses. On the other hand, functional status (evaluated by the EDSS) positively correlated with parent-reported internalizing symptoms in their children. Also, later studies showed the tendency of parents to describe higher rate of mood disorders in their children with MS as compared with patients’ self-report. In a study by Charvet et al., 140 pediatric patients with MS or CIS were evaluated with BASC-2 (Behavior Assessment System for Children-2). The study evidenced that all BASC-2 scales were in the typical range in both self and parents’ reports [46]. However, about 33% of the sample reported a clinically significant problem on at least one scale. Although mood and behavioral problems were rated by patients as slightly lower than parents’ reports, both indicated anxiety, somatization, and attention problems as the most common disorders. While no association between these problems and disease features or fatigue was found, the authors described a higher rate of emotional and behavioral problems in patients with cognitive impairment. These results agree with a previous study on 45 pediatric MS patients, where a higher rate of cognitive impairment was found in patients diagnosed with anxiety or mood disorder [47].
Very few studies explored the comorbidity between pediatric MS and psychiatric disorders, such as psychosis, autism, or ADHD. In a retrospective study, Pakpoor provided the first evidence of an association between childhood MS (and other demyelinating diseases) with psychotic disorders [48]. The study evidenced that while psychotic disorders did not significantly precede the demyelinating disease, autism and ADHD were associated with it. These results may reflect the different typical age in which psychosis, ADHD, and autism are diagnosed. One year later, in a nationwide population-based study, Boesen explored the presence of psychiatric comorbidity before and after onset of MS [49]. A higher rate of psychiatric comorbidity was described among patients with MS, especially girls, compared with children without MS. While an increasing rate of anxiety and depression was found compared with the pre-MS age, no significant higher risk for MS was found among children exposed to psychiatric morbidity during the last 2 years. According to these findings, psychiatric comorbidity may start after MS onset, although undiagnosed cognitive/psychiatric problems preceding the illness onset cannot be excluded.
Fatigue
Fatigue related to MS is defined as “a subjective lack of physical and/or mental energy that is perceived by the individual or caregiver to interfere with usual or desired activities” [50]. The MS International Federation recognized fatigue as either physical or cognitive [51]. With an estimated prevalence ranging from 9 to 76%, fatigue is a common, pervasive, and disabling symptom of MS [52]. Unfortunately, since there are few validated questionnaires for children/adolescents’ fatigue, this symptom is often assessed by multi-rater perspectives which may lead to discrepant results. Indeed, parents are more prone to report higher fatigue than children or adolescents [18, 34, 52, 53]. This disagreement may be influenced by parents’ moods or excessive parental worry [52,53,54].
Although both fatigue and cognitive problems may have a negative impact on quality of life, data on their relationship in pediatric patients with MS are sparse and far from conclusive.
Comparing the levels of fatigue in pediatric patients with MS, chronic fatigue syndrome (CFS), and healthy subjects, Carrol et al. reported similar levels in both patient groups [55]. Cognitive difficulties emerged in both non-fatigued and fatigued children with MS, suggesting that neuropsychological impairment is independent of fatigue, as confirmed by a more recent study [15].
While fatigue is not related to the overall cognitive functioning, it can correlate with the scores obtained in individual neuropsychological tasks [34]. Goretti et al. found an association between cognitive fatigue and performance in individual neuropsychological tasks [53]. Higher scores of self-reported cognitive fatigue were associated with low performance in a problem-solving task, whereas higher levels of parent-reported cognitive fatigue were associated with low scores in tests of processing speed, complex attention verbal comprehension, and verbal learning.
Consistent evidence supports the reciprocal relationship between fatigue and depressed mood in pediatric MS. Several studies described a moderate to strong association between fatigue and depression [12, 52,53,54, 56]. Also a moderate association between fatigue and self-reported anxiety has been reported [57].
As in patients with AOMS, also in those with POMS, fatigue is independent of age at MS onset, disease duration, relapse rate, and number of relapses [52, 54, 56].
Quality of life
MS may impair participation of children and adolescents in curricular and social activities, leading to a low QoL. In an earlier study, Boyd and MacMillan identified developmental, psychological, and social experiences adversely affected by the diagnosis of MS [58]. The most common stressors were unpredictable relapses, unresolved symptoms, uncertainty about the future, demanding treatment regime, changes in peer relationships, and family conflicts (Table 2).
Children and adolescents with MS may have worse QoL in all areas of life, compared not only with healthy subjects but also with children suffering from other neurological diseases [59]. The disease most frequently affects school and emotional domains, while a smaller impact on the social and physical areas has been reported [54, 59,60,61,62,63,64]. MS patients show worse scores in the emotional and school areas, compared to children with neuromuscular diseases [59, 62]. In pediatric patients with MS, some studies reported a high number of absences from school [21,22,23, 59]. They can be associated with sick days, relapses, hospital admissions, medical appointments, and therapy side effects [3, 6, 19, 59, 65]. However, other factors, such as disease course, cognitive impairment, and fatigue, may explain the changes in school QoL [13, 17, 22, 54, 56, 59, 66]. The importance of cognitive impairment in this contest is suggested by the association between higher cognitive scores and higher total QoL score [67]. Also, fatigue may contribute to a poor school QoL [56, 59]. As described by Carroll, tiredness in children and adolescents with MS reduces cognitive functions and causes daytime sleepiness, thus worsening their performance at school [55]. Parrish et al. showed that most patients with pediatric MS require special education plans or classroom accommodations (e.g., reduced workload or extended time on exams) [19]. Compared with the general population, patients with POMS show higher level of school dropout, lower educational achievement, and lower salaries [7, 15]. Beyond cognitive impairment and fatigue, psychiatric comorbidity may have an adverse influence on quality of life in children and adolescents with MS [11, 56, 58, 68]. Patients with MS suffering from depression have significant lower QoL, compared to healthy subjects [56, 68].
Studies on social sphere of QoL did not provide homogenous results. According to Goretti et al., impairment in social relationships may be found in 28% of patients, particularly due to tendency to isolation and behavioral changes, such as aggressiveness [45]. On the other hand, in a study by Storm Van’s Gravesande [56], the social functioning dimension was the least affected. In a more recent paper, Rosa et al. described increased social functioning over a 4-year follow-up [64].
Several studies showed that physical dimension of QoL is altered in pediatric patients with MS [54, 56, 59, 67]. In pediatric age, every type of physical impairment or change, though with mild disability, may lead to lower QoL [56]. However, the low levels of disability, typical of children and adolescents with MS, may explain the low impact of the disease on physical QoL [59, 60, 62, 64].
Disease modifying therapies, cognitive, and quality of life outcomes
Studies investigating the impact of pharmacologic interventions on cognitive outcomes in children and adolescents affected by MS are limited [11, 21, 69]. However, most patients included in studies on neuropsychological outcome of POMS were receiving disease modifying therapies (DMT) [8, 15, 17, 37]. In the study by Portaccio et al., the percentage of patients treated with highly effective DMT was higher in cognitively preserved patients (60% vs 38.9%), although the difference was not significant [15]. While no significant effect of the type of DMT on processing speed has been found by Wallach et al. [13], the protective role of natalizumab and fingolimod on progressive cognitive decline has been described [70, 71]. In a 24-month follow-up of pediatric patients treated with natalizumab, an improvement of EDSS relapses rate and MRI measures, but also an increase of cognitive functions (evaluate by SDMT) was described by Margoni et al. [70]. In a 2.5-year follow-up by Johnen et al., cognitive performances were preserved or even ameliorated in patients who escalated to highly effective drugs (natalizumab or fingolimod); on the other hand, a deterioration of cognitive performance was observed in patients who remained in first-line platform therapy (β-interferon or glatiramer acetate) [71].
In addition to the effects of DMT on cognitive performance, there is a growing scientific interest in the effects of immunomodulatory therapies on psychosocial outcomes. Ghezzi et al. evaluated the QoL changes in adolescents receiving interferon-β1 administered using electronic autoinjection [72]. The authors showed potential long-term benefits and increased quality of life over time in both self (except for emotional sphere) and parent reports. In particular, school functioning showed the greatest increase in patients’ and parents’ self-reports. In another study by Krupp et al., fingolimod demonstrated greater efficacy than interferon-β1 in improving QoL [73]. These results led the authors to suggest that treatments demonstrating substantial efficacy in reducing relapse rates and favorable tolerability also have beneficial effects on the QoL of patients with POMS.
Discussion
Pediatric MS is a progressive disease with an unpredictable course and a negative impact on patients’ physical, cognitive, and psychological well-being, with a significant consequence on family life as well [1, 7, 19, 20, 44, 63]. Children and adolescents with MS, in addition to facing physiological developmental tasks, may undergo cognitive sequelae, neurological symptoms, and treatment regimens. Childhood and adolescence are critical periods for appropriate academic achievements, personal and social growth [74]. All these factors suggest that the impact of the disease in developmental age may be more severe than in adulthood independently of physical disability [15, 17, 21].
The reviewed literature suggests that, despite the lower physical disability, children and adolescents diagnosed with MS are vulnerable to cognitive impairment even in the early stage of the disease [7, 13, 14]. It has been hypothesized that, in pediatric age, cognitive decline may be considered a sensitive measure of MS severity [16]. Even the failure to reach the age-expected cognitive maturation has been considered a sign of disease progression [18].
Cognitive difficulties, beyond physical disability and relapses, may have a considerable impact on learning and school achievement [8, 19, 22, 67].
The mechanisms underlining the high prevalence of cognitive impairment in pediatric MS are not fully understood. Pediatric age is characterized by brain growth, neural network maturation, and ongoing myelination in the central nervous system [20, 74]. Since in children the neuropathological process of MS occurs in a critical period, it is not surprising that cognitive capabilities, in particular language, are particularly vulnerable [19]. While the possible role of age of onset, length of the disease, and disability as vulnerability factors of cognitive decline is controversial, the importance of brain plasticity, cognitive reserve (estimated through a higher IQ at baseline), and parental education level as protective factors against neuropsychological impairment has been suggested [7, 15, 33, 70, 75]. Over the last decades, emerging research focused on MRI correlates of neuropsychological deficits [7, 19]. Although data are so far sparse and often incongruent, several MRI studies described abnormalities in specific brain areas (i.e., thalamus, hippocampus, amygdala, and cerebellum) of children with cognitive impairment [7, 19]. In an early study in POMS, Till et al. found an association between cognitive impairment (global IQ, processing speed, and expressive vocabulary) and reduced thalamic volume [25].
Beyond cognitive impairment, psychiatric factors and fatigue may contribute to patients’ low functional outcomes. The high prevalence of depression among children and adolescents with MS has been explained with both a direct pathogenic effect of the disease on brain networks and a psychological reaction to the disease [12, 47, 49]. Also, the influence of the disease modifying treatment has been suggested with inconsistent results [12, 43]. Myelin alterations may play a key role in the development of neuropsychiatric disorders [76]. MRI studies suggested that depressive mood disorder may be associated to brain atrophy and demyelinating lesions in temporal [77], parietal [77], and frontal lobes [77]. On the other hand, fatigue, depression, and anxiety may be the result of psychological adjustment to having a chronic illness [78]. A maladaptive response to the high pressures of dealing with this chronic disease may lead to feelings of helplessness and hopelessness and contribute to an increased sense of social isolation [59].
Limitations
The reviewed literature has several limitations. First, since diagnosis of MS in pediatric age is rare, most studies include small samples. Second, psychological and neuropsychological tools used for patients’ evaluation are extremely heterogeneous. Although research on cognitive profile of POMS has increased over the time and the cognitive assessment has been recommended, the best assessment tools for pediatric MS are still to be determined. Third, a structured assessment of pre-morbid neuropsychological functioning is generally lacking.
Conclusions
The present review suggests that cognitive dysfunctions are frequent and debilitating symptoms in children and adolescents with MS. They can be worsened by fatigue and psychiatric symptoms, which are also common. Overall, these manifestations may cause considerable functional impairment on daily activities, academic achievement, and quality of life that may require individualized rehabilitative treatment and extensive psychosocial care.
References
Alroughani R, Boyko A (2018) Pediatric multiple sclerosis: a review. BMC Neurol 18(1):27. https://doi.org/10.1186/s12883-018-1026-3
Sumowski JF, Benedict R, Enzinger C, Filippi M, Geurts JJ, Hamalainen P, Hulst H, Inglese M, Leavitt VM, Rocca MA, Rosti-Otajarvi EM, Rao S (2018) Cognition in multiple sclerosis: state of the field and priorities for the future. Neurology 90(6):278–288. https://doi.org/10.1212/WNL.0000000000004977
Brola W, Steinborn B (2020) Pediatric multiple sclerosis - current status of epidemiology, diagnosis and treatment. Neurol Neurochir Pol 54(6):508–517. https://doi.org/10.5603/PJNNS.a2020.0069
Fisher KS, Cuascut FX, Rivera VM, Hutton GJ (2020) Current advances in pediatric onset multiple sclerosis. Biomedicines 8(4):71. https://doi.org/10.3390/biomedicines8040071
Bigi S, Banwell B (2012) Pediatric multiple sclerosis. J Child Neurol 27(11):1378–1383. https://doi.org/10.1177/0883073812452784
Gorman MP, Healy BC, Polgar-Turcsanyi M, Chitnis T (2009) Increased relapse rate in pediatric-onset compared with adult-onset multiple sclerosis. Arch Neurol 66(1):54–59. https://doi.org/10.1001/archneurol.2008.505
Portaccio E, De Meo E, Bellinvia A, Amato MP (2021) Cognitive issues in pediatric multiple sclerosis. Brain Sci 11(4):442. https://doi.org/10.3390/brainsci11040442
Martins C, Samões R, Silva AM, Santos E, Figueiroa S (2023) Pediatric multiple sclerosis-experience of a tertiary care center. Neuropediatrics 54(1):58–63. https://doi.org/10.1055/s-0042-1759843
Ness JM, Chabas D, Sadovnick AD, Pohl D, Banwell B, Weinstock-Guttman B, International Pediatric MS Study Group (2007) Clinical features of children and adolescents with multiple sclerosis. Neurology 68(16 Suppl 2):S37-45. https://doi.org/10.1212/01.wnl.0000259447.77476.a9
Trojano M, Liguori M, Bosco Zimatore G, Bugarini R, Avolio C, Paolicelli D, Giuliani F, De Robertis F, Marrosu MG, Livrea P (2002) Age-related disability in multiple sclerosis. Ann Neurol 51(4):475–480. https://doi.org/10.1002/ana.10147
Lanzillo R, Chiodi A, Carotenuto A, Magri V, Napolitano A, Liuzzi R, Costabile T, Rainone N, Freda MF, Valerio P, Brescia Morra V (2016) Quality of life and cognitive functions in early onset multiple sclerosis. Eur J Paediatr Neurol 20(1):158–163. https://doi.org/10.1016/j.ejpn.2015.08.005
Till C, Udler E, Ghassemi R, Narayanan S, Arnold DL, Banwell BL (2012) Factors associated with emotional and behavioral outcomes in adolescents with multiple sclerosis. Mult Scler 18(8):1170–1180. https://doi.org/10.1177/1352458511433918
Wallach AI, Waltz M, Casper TC, Aaen G, Belman A, Benson L et al (2020) Cognitive processing speed in pediatric-onset multiple sclerosis: baseline characteristics of impairment and prediction of decline. Mult Scler 26(14):1938–1947. https://doi.org/10.1177/1352458519891984
MacAllister WS, Christodoulou C, Milazzo M, Krupp LB (2007) Longitudinal neuropsychological assessment in pediatric multiple sclerosis. Dev Neuropsychol 32(2):625–644. https://doi.org/10.1080/87565640701375872
Portaccio E, Bellinvia A, Razzolini L, Pastò L, Goretti B, Niccolai C et al (2022) Long-term cognitive outcomes and socioprofessional attainment in people with multiple sclerosis with childhood onset. Neurology 98(16):e1626–e1636. https://doi.org/10.1212/WNL.0000000000200115
Carotenuto A, Moccia M, Costabile T, Signoriello E, Paolicelli D, Simone M, Lus G, Brescia Morra V, Lanzillo R, Cogniped study group, (2019) Associations between cognitive impairment at onset and disability accrual in young people with multiple sclerosis. Sci Rep 9(1):18074. https://doi.org/10.1038/s41598-019-54153-7
Amato MP, Goretti B, Ghezzi A, Hakiki B, Niccolai C, Lori S et al (2014) Neuropsychological features in childhood and juvenile multiple sclerosis: five-year follow-up. Neurology 83(16):1432–1438. https://doi.org/10.1212/WNL.0000000000000885
Suppiej A, Cainelli E (2014) Cognitive dysfunction in pediatric multiple sclerosis. Neuropsychiatr Dis Treat 10:1385–1392. https://doi.org/10.2147/NDT.S48495
Parrish JB, Fields E (2019) Cognitive functioning in patients with pediatric-onset multiple sclerosis, an Updated Review and Future Focus. Children (Basel) 6(2):21. https://doi.org/10.3390/children6020021
Amato MP, Krupp LB, Charvet LE, Penner I, Till C (2016) Pediatric multiple sclerosis: cognition and mood. Neurology 87(9 Suppl 2):S82-87. https://doi.org/10.1212/WNL.0000000000002883
Amato MP, Goretti B, Ghezzi A, Lori S, Zipoli V, Moiola L, Falautano M, De Caro MF, Viterbo R, Patti F, Vecchio R, Pozzilli C, Bianchi V, Roscio M, Martinelli V, Comi G, Portaccio E, Trojano M, Multiple sclerosis study group of the Italian Neurological Society (2010) Cognitive and psychosocial features in childhood and juvenile MS: two-year follow-up. Neurology 75(13):1134–1140. https://doi.org/10.1212/WNL.0b013e3181f4d821
MacAllister WS, Belman AL, Milazzo M, Weisbrot DM, Christodoulou C, Scherl WF, Preston TE, Cianciulli C, Krupp LB (2005) Cognitive functioning in children and adolescents with multiple sclerosis. Neurology 64(8):1422–1425. https://doi.org/10.1212/01.WNL.0000158474.24191.BC
Kalb RC, DiLorenzo TA, LaRocca NG, Caruso LS, Shawaryn MA, Elkin R et al (1999) The impact of early onset multiple sclerosis on cognitive and social indices. Int J MSCare 1:1–6. http://mscare.com [Accessed December 15, 2004]
Amato MP, Goretti B, Ghezzi A, Lori S, Zipoli V, Portaccio E, Moiola L, Falautano M, De Caro MF, Lopez M, Patti F, Vecchio R, Pozzilli C, Bianchi V, Roscio M, Comi G, Trojano M, Multiple Sclerosis Study Group of the Italian Neurological Society (2008) Cognitive and psychosocial features of childhood and juvenile MS. Neurology 70(20):1891–1897. https://doi.org/10.1212/01.wnl.0000312276.23177.fa
Till C, Ghassemi R, Aubert-Broche B, Kerbrat A, Collins DL, Narayanan S, Arnold DL, Desrocher M, Sled JG, Banwell BL (2011) MRI correlates of cognitive impairment in childhood-onset multiple sclerosis. Neuropsychology 25(3):319–332. https://doi.org/10.1037/a0022051
Barlow-Krelina E, Fabri TL, O’Mahony J, Gur RC, Gur RE, De Somma E, Bolongaita L, Dunn CL, Bacchus M, Yeh EA, Marrie RA, Bar-Or A, Banwell BL, Till C (2021) Examining cognitive speed and accuracy dysfunction in youth and young adults with pediatric-onset multiple sclerosis using a computerized neurocognitive battery. Neuropsychology 35(4):388–398. https://doi.org/10.1037/neu0000729
Krupp LB, Waubant E, Waltz M, Casper TC, Belman A, Wheeler Y et al (2023) A new look at cognitive functioning in pediatric MS. Mult Scler 29(1):140–149. https://doi.org/10.1177/13524585221123978
McKay KA, Manouchehrinia A, Berrigan L, Fisk JD, Olsson T, Hillert J (2019) Long-term cognitive outcomes in patients with pediatric-onset vs adult-onset multiple sclerosis. JAMA Neurol 76(9):1028–1034. https://doi.org/10.1001/jamaneurol.2019.1546
Portaccio E, Simone M, Prestipino E, Bellinvia A, Pastò L, Niccolai M, Razzolini L, Fratangelo R, Tudisco L, Fonderico M, Ghezzi A, Pippolo L, Marrosu MG, Cocco E, Fenu G, Patti F, Chisari C, Falautano M, Moiola L, Minacapelli E, Viterbo RG, Margari L, Goretti B, Amato MP (2020) Cognitive reserve is a determinant of social and occupational attainment in patients with pediatric and adult onset multiple sclerosis. Multiple sclerosis and related disorders 42:102145. https://doi.org/10.1016/j.msard.2020.102145
Baroncini D, Simone M, Iaffaldano P, Brescia Morra V, Lanzillo R, Filippi M, Romeo M, Patti F, Chisari CG, Cocco E, Fenu G, Salemi G, Ragonese P, Inglese M, Cellerino M, Margari L, Comi G, Zaffaroni M, Ghezzi A, Italian MS registry (2021) Risk of persistent disability in patients with pediatric-onset multiple sclerosis. JAMA Neurol 78(6):726–735. https://doi.org/10.1001/jamaneurol.2021.1008
Kalb R, Beier M, Benedict RH, Charvet L, Costello K, Feinstein A et al (2018) Recommendations for cognitive screening and management in multiple sclerosis care. Mult Scler 24(13):1665–1680. https://doi.org/10.1177/1352458518803785
Marin SE, Banwell BB, Till C (2013) Cognitive trajectories in 4 patients with pediatric-onset multiple sclerosis: serial evaluation over a decade. J Child Neurol 28(12):1577–1586. https://doi.org/10.1177/0883073812465010
Akbar N, Signori A, Amato MP, Sormani MP, Portaccio E, Niccolai C, Goretti B, Till C, Banwell B (2017) Maturational trajectory of processing speed performance in pediatric multiple sclerosis. Dev Neuropsychol 42(5):299–308. https://doi.org/10.1080/87565641.2017.1351974
Holland AA, Graves D, Greenberg BM, Harder LL (2014) Fatigue, emotional functioning, and executive dysfunction in pediatric multiple sclerosis. Child Neuropsychol 20(1):71–85. https://doi.org/10.1080/09297049.2012.748888
Ruano L, Branco M, Portaccio E, Goretti B, Niccolai C, Patti F, Chisari C, Gallo P, Grossi P, Ghezzi A, Roscio M, Mattioli F, Stampatori C, Simone M, Viterbo RG, Amato MP (2018) Patients with paediatric-onset multiple sclerosis are at higher risk of cognitive impairment in adulthood: an Italian collaborative study. Mult Scler 24(9):1234–1242. https://doi.org/10.1177/1352458517717341
Banwell BL, Anderson PE (2005) The cognitive burden of multiple sclerosis in children. Neurology 64(5):891–894. https://doi.org/10.1212/01.WNL.0000152896.35341.51
Öztürk Z, Gücüyener K, Soysal Ş, Konuşkan GD, Konuşkan B, Dikmen AU, Anlar B (2020) Cognitive functions in pediatric multiple sclerosis: 2-years follow-up. Neurol Res 42(2):159–163. https://doi.org/10.1080/01616412.2019.1710417
Till C, Racine N, Araujo D, Narayanan S, Collins DL, Aubert-Broche B, Arnold DL, Banwell B (2013) Changes in cognitive performance over a 1-year period in children and adolescents with multiple sclerosis. Neuropsychology 27(2):210–219. https://doi.org/10.1037/a0031665
Charvet LE, O’Donnell EH, Belman AL, Chitnis T, Ness JM, Parrish J, Patterson M, Rodriguez M, Waubant E, Weinstock-Guttman B, Krupp LB, US Network of Pediatric MS Centers (2014) Longitudinal evaluation of cognitive functioning in pediatric multiple sclerosis: report from the US Pediatric Multiple Sclerosis Network. Mult Scler 20(11):1502–1510. https://doi.org/10.1177/1352458514527862
Charvet LE, Cleary RE, Vazquez K, Belman AL, Krupp LB, Network US, for Pediatric MS, (2014) Social cognition in pediatric-onset multiple sclerosis (MS). Mult Scler 20(11):1478–1484. https://doi.org/10.1177/1352458514526942
Neuhaus M, Bagutti S, Yaldizli Ö, Zwahlen D, Schaub S, Frey B, Fischer-Barnicol B, Burgunder JM, Martory MD, Pöttgen J, Annoni JM, Penner IK (2018) Characterization of social cognition impairment in multiple sclerosis. Eur J Neurol 25(1):90–96. https://doi.org/10.1111/ene.13457
Massano C, Lima M, Monteiro I, Machado R, Correia I, Nunes CC, Macário C, Sousa L, Santana I, Batista S (2021) Outcomes on social and classic cognition in adults with pediatric-onset multiple sclerosis. Mult Scler Relat Disord 53:103071. https://doi.org/10.1016/j.msard.2021.103071
Skokou M, Soubasi E, Gourzis P (2012) Depression in multiple sclerosis: a review of assessment and treatment approaches in adult and pediatric populations. ISRN Neurol 2012:427102. https://doi.org/10.5402/2012/427102
Boesen MS, Blinkenberg M, Thygesen LC, Eriksson F, Magyari M (2021) School performance, psychiatric comorbidity, and healthcare utilization in pediatric multiple sclerosis: a nationwide population-based observational study. Mult Scler 27(2):259–267. https://doi.org/10.1177/1352458520959673
Goretti B, Ghezzi A, Portaccio E, Lori S, Zipoli V, Razzolini L, Moiola L, Falautano M, De Caro MF, Viterbo R, Patti F, Vecchio R, Pozzilli C, Bianchi V, Roscio M, Comi G, Trojano M, Amato MP, Study Group of the Italian Neurological Society (2010) Psychosocial issue in children and adolescents with multiple sclerosis. Neurol Sci 49. 31(4):467–470. https://doi.org/10.1007/s10072-010-0281-x
Charvet L, Cersosimo B, Schwarz C, Belman A, Krupp LB (2016) Behavioral symptoms in pediatric multiple sclerosis: relation to fatigue and cognitive impairment. J Child Neurol 31(8):1062–1067. https://doi.org/10.1177/0883073816636227
Weisbrot D, Charvet L, Serafin D, Milazzo M, Preston T, Cleary R, Moadel T, Seibert M, Belman A, Krupp L (2014) Psychiatric diagnoses and cognitive impairment in pediatric multiple sclerosis. Mult Scler 20(5):588–593. https://doi.org/10.1177/1352458513504249
Pakpoor J, Goldacre R, Schmierer K, Giovannoni G, Waubant E, Goldacre MJ (2018) Psychiatric disorders in children with demyelinating diseases of the central nervous system. Mult Scler 24(9):1243–1250. https://doi.org/10.1177/1352458517719150
Boesen MS, Thygesen LC, Uldall PV, Eriksson F, Born AP, Blinkenberg M, Koch-Henriksen N, Greisen G, Magyari M (2018) Psychiatric morbidity develops after onset of pediatric multiple sclerosis: a Danish nationwide population-based study. Mult Scler Relat Disord 19:30–34. https://doi.org/10.1016/j.msard.2017.10.018
Multiple Sclerosis Council for Clinical Practice Guidelines (1998) Fatigue and multiple sclerosis: evidence based management strategies for fatigue in multiple sclerosis. Paralyzed Veterans of America, Washington DC
Multiple Sclerosis International Federation (MSIF) (2011) Fatigue and MS, in MS in Focus. Multiple Sclerosis International Federation, London
Carroll S, Chalder T, Hemingway C, Heyman I, Moss-Morris R (2016) Understanding fatigue in paediatric multiple sclerosis: a systematic review of clinical and psychosocial factors. Dev Med Child Neurol 58(3):229–239. https://doi.org/10.1111/dmcn.12964
Goretti B, Portaccio E, Ghezzi A, Lori S, Moiola L, Falautano M, Viterbo R, Patti F, Vecchio R, Pozzilli C, Bianchi V, Cappiello S, Comi G, Trojano M, Amato MP, Multiple Sclerosis Study Group of the Italian Neurological Society (2012) Fatigue and its relationships with cognitive functioning and depression in paediatric multiple sclerosis. Mult Scler 18(3):329–334. https://doi.org/10.1177/1352458511420846
MacAllister WS, Christodoulou C, Troxell R, Milazzo M, Block P, Preston TE, Bender HA, Belman A, Krupp LB (2009) Fatigue and quality of life in pediatric multiple sclerosis. Mult Scler 15(12):1502–1508. https://doi.org/10.1177/1352458509345902
Carroll S, Chalder T, Hemingway C, Heyman I, Bear H, Sweeney L, Moss-Morris R (2019) Adolescent and parent factors related to fatigue in paediatric multiple sclerosis and chronic fatigue syndrome: a comparative study. Eur J Paediatr Neurol 23(1):70–80. https://doi.org/10.1016/j.ejpn.2018.10.006
Storm Van’s Gravesande K, Blaschek A, Calabrese P, Rostásy K, Huppke P, Kessler JJ, Kalbe E, Mall V, MUSICADO Study group (2019) Fatigue and depression predict health-related quality of life in patients with pediatric-onset multiple sclerosis. Mult Scler Relat Disord 36:101368. https://doi.org/10.1016/j.msard.2019.08.010
Parrish JB, Weinstock-Guttman B, Smerbeck A, Benedict RH, Yeh EA (2013) Fatigue and depression in children with demyelinating disorders. J Child Neurol 28(6):713–718. https://doi.org/10.1177/0883073812450750
Boyd JR, MacMillan LJ (2005) Experiences of children and adolescents living with multiple sclerosis. J Neurosci Nurs 37(6):334–342. https://doi.org/10.1097/01376517-200512000-00007
Mrosková S, Klímová E, Majerníková Ľ, Tkáčová Ľ (2021) Quality of life of children and adolescents with multiple sclerosis-a literature review of the quantitative evidence. Int J Environ Res Public Health 18(16):8645. https://doi.org/10.3390/ijerph18168645
Florea A, Maurey H, Le Sauter M, Bellesme C, Sevin C, Deiva K (2020) Fatigue, depression, and quality of life in children with multiple sclerosis: a comparative study with other demyelinating diseases. Dev Med Child Neurol 62(2):241–244. https://doi.org/10.1111/dmcn.14242
Schwartz CE, Grover SA, Powell VE, Noguera A, Mah JK, Mar S, Mednick L, Banwell BL, Alper G, Rensel M, Gorman M, Waldman A, Schreiner T, Waubant E, Yeh EA (2018) Risk factors for non-adherence to disease-modifying therapy in pediatric multiple sclerosis. Mult Scler 24(2):175–185. https://doi.org/10.1177/1352458517695469
Mowry EM, Julian LJ, Im-Wang S, Chabas D, Galvin AJ, Strober JB, Waubant E (2010) Health-related quality of life is reduced in pediatric multiple sclerosis. Pediatr Neurol 43(2):97–102. https://doi.org/10.1016/j.pediatrneurol.2010.03.007
O’Mahony J, Marrie RA, Laporte A, Bar-Or A, Yeh EA, Brown A, Dilenge ME, Banwell B (2019) Pediatric-onset multiple sclerosis is associated with reduced parental health-related quality of life and family functioning. Mult Scler 25(12):1661–1672. https://doi.org/10.1177/1352458518796676
Rosa L, Petracca M, Carotenuto A, Dolce P, Piscopo K, Dicé F et al (2022) Quality of life changes in early-onset multiple sclerosis: a 4-year follow-up study. J Clin Med 11(17):5226. https://doi.org/10.3390/jcm11175226
Marrie RA, O’Mahony J, Maxwell C, Ling V, Till C, Barlow-Krelina E, Yeh EA, Arnold DL, Bar-Or A, Banwell B, Network CPDD (2020) Factors associated with health care utilization in pediatric multiple sclerosis. Mult Scler Relat Disord 38:101511. https://doi.org/10.1016/j.msard.2019.101511
Toussaint-Duyster LC, Wong YYM, Van der Cammen-van Zijp MH, Van Pelt-Gravesteijn D, Catsman-Berrevoets CE, Hintzen RQ, Neuteboom RF (2018) Fatigue and physical functioning in children with multiple sclerosis and acute disseminated encephalomyelitis. Mult Scler 24(7):982–990. https://doi.org/10.1177/1352458517706038
Lulu S, Julian L, Shapiro E, Hudson K, Waubant E (2014) Treatment adherence and transitioning youth in pediatric multiple sclerosis. Mult Scler Relat Disord 3(6):689–695. https://doi.org/10.1016/j.msard.2014.09.088
Ostojic S, Stevanovic D, Jancic J (2016) Quality of life and its correlates in adolescent multiple sclerosis patients. Mult Scler Relat Disord 10:57–62. https://doi.org/10.1016/j.msard.2016.08.013
Luchesa Smith A, Benetou C, Bullock H, Kuczynski A, Rudebeck S, Hanson K, Crichton S, Mankad K, Siddiqui A, Byrne S, Lim M, Hemingway C (2020) Progress in the management of paediatric-onset multiple sclerosis. Children (Basel) 7(11):222. https://doi.org/10.3390/children7110222
Margoni M, Rinaldi F, Riccardi A, Franciotta S, Perini P, Gallo P (2020) No evidence of disease activity including cognition (NEDA-3 plus) in naïve pediatric multiple sclerosis patients treated with natalizumab. J Neurol 267(1):100–105. https://doi.org/10.1007/s00415-019-09554-z
Johnen A, Elpers C, Riepl E, Landmeyer NC, Krämer J, Polzer P, Lohmann H, Omran H, Wiendl H, Göbel K, Meuth SG (2019) Early effective treatment may protect from cognitive decline in paediatric multiple sclerosis. Eur J Paediatr Neurol 23(6):783–791. https://doi.org/10.1016/j.ejpn.2019.08.007
Ghezzi A, Bianchi A, Baroncini D, Bertolotto A, Malucchi S, Bresciamorra V, Lanzillo R, Milani N, Martinelli V, Patti F, Chisari C, Rottoli M, Simone M, Paolicelli D, Visconti A, FUTURE Study Group (2017) A multicenter, observational, prospective study of self- and parent-reported quality of life in adolescent multiple sclerosis patients self-administering interferon-β1a using RebiSmart™-the FUTURE study. Neurol sci 38(11):1999–2005. https://doi.org/10.1007/s10072-017-3091-6
Krupp L, Banwell B, Chitnis T, Deiva K, Gaertner J, Ghezzi A, Huppke P, Waubant E, DeLasHeras V, Azmon A, Karan R (2022) Effect of fingolimod on health-related quality of life in paediatric patients with multiple sclerosis: results from the phase 3 PARADIGMS Study. BMJ Neurol Open 4(1):e000215. https://doi.org/10.1136/bmjno-2021-000215
Larsen B, Luna B (2018) Adolescence as a neurobiological critical period for the development of higher-order cognition. Neurosci Biobehav Rev 94:179–195. https://doi.org/10.1016/j.neubiorev.2018.09.005
Pastò L, Portaccio E, Goretti B, Ghezzi A, Lori S, Hakiki B et al (2016) The cognitive reserve theory in the setting of pediatric-onset multiple sclerosis. Mult Scler 22(13):1741–1749. https://doi.org/10.1177/1352458516629559
Fields RD (2008) White matter in learning, cognition and psychiatric disorders. Trends Neurosci 31(7):361–370. https://doi.org/10.1016/j.tins.2008.04.001
Bakshi R, Czarnecki D, Shaikh ZA, Priore RL, Janardhan V, Kaliszky Z, Kinkel PR (2000) Brain MRI lesions and atrophy are related to depression in multiple sclerosis. NeuroReport 11(6):1153–1158. https://doi.org/10.1097/00001756-200004270-00003
Hards E, Orchard F, Khalid S, D’souza C, Cohen F, Gowie E, Loades M (2023) Self-evaluation and depression in adolescents with a chronic illness: a systematic review. Clin Child Psychol Psychiatry 28(1):382–397. https://doi.org/10.1177/13591045221115287
Funding
This work was supported by the Italian Ministry of Health with Current Research funds.
Author information
Authors and Affiliations
Contributions
ST and MV: conceptualization; ST and MPC: literature search data and writing—original draft preparation; LP, GM, and MANF: writing—review and editing; and MV: supervision. All authors have read and agreed to the published version of the manuscript.
Corresponding author
Ethics declarations
Ethical approval
The manuscript does not contain unpublished clinical studies or patient data. This manuscript reviews published clinical studies that compile to the required Ethical Guidelines.
Conflict of interest
The authors declare no competing interests.
Additional information
Publisher's Note
Springer Nature remains neutral with regard to jurisdictional claims in published maps and institutional affiliations.
Rights and permissions
Open Access This article is licensed under a Creative Commons Attribution 4.0 International License, which permits use, sharing, adaptation, distribution and reproduction in any medium or format, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons licence, and indicate if changes were made. The images or other third party material in this article are included in the article's Creative Commons licence, unless indicated otherwise in a credit line to the material. If material is not included in the article's Creative Commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use, you will need to obtain permission directly from the copyright holder. To view a copy of this licence, visit http://creativecommons.org/licenses/by/4.0/.
About this article
Cite this article
Tarantino, S., Proietti Checchi, M., Papetti, L. et al. Neuropsychological performances, quality of life, and psychological issues in pediatric onset multiple sclerosis: a narrative review. Neurol Sci 45, 1913–1930 (2024). https://doi.org/10.1007/s10072-023-07281-y
Received:
Accepted:
Published:
Issue Date:
DOI: https://doi.org/10.1007/s10072-023-07281-y