Neuropathic pain in children: Steps towards improved recognition and management

Walker, Suellen M.

doi:10.1016/j.ebiom.2020.103124

Cited by 22 publications

(39 citation statements)

References 76 publications

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“…Indeed, the diagnosis of neuropathic pain during VOC raises the problem of fine descriptions of the characteristics of the pain, which are sometimes difficult in young children, especially during an intensely painful episode where many sensations are mixed, including anxiety, fear of parental separation, and adverse effects of treatment (pain related to infusion devices, opioid-induced pruritus or hyperalgesia, etc.). Moreover, the diagnosis between “pure neuropathic” and “mixed pain” in children and adolescents is very difficult for several reasons: We do not dispose of many diagnostic tools, as questionnaires validated for adults and the electrophysiologic methods, such as quantitative sensory testing (QST) or electromyography (EMG), cannot be easily used in children [ 22 , 23 ]. In a recent survey study among members of learned societies or groups whose members are known to treat pediatric pain, de Leeuw et al [ 11 ] observed that only 45.3% of the respondents used the IASP criteria for establishing the diagnosis of neuropathic pain in children, while 18 (15.4%) explicitly answered that they did not use these criteria; 46 persons (39.3%) left this question unanswered.…”

Section: Discussionmentioning

confidence: 99%

Neuropathic Pain in Children with Sickle Cell Disease: The Hidden Side of the Vaso-Occlusive Crisis

et al. 2021

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The majority of hospitalizations of patients with sickle cell disease (SCD) are related to painful vaso-occlusive crises (VOCs). Although the pain of VOC is classically nociceptive, neuropathic pain (NP) has also been demonstrated in SCD patients. The aim of our study is to specify the prevalence of NP during VOCs in SCD children using a dedicated scale and to measure its characteristics. We performed a prospective study that included SCD children hospitalized for an acute VOC. The presence of NP was sought with the DN4 scale on the second and fourth days of hospitalization. A total of 54 SCD children were included in the study. Overall, 41% of the patients (n = 22) experienced neuropathic pain during the VOC, mostly at an early stage (Day 2). The median age, the sex ratio, the location of the pain, and the morphine consumption were similar for patients with and without NP. Our study shows that neuropathic pain is very common during VOCs in SCD children. The absence of identified risk factors should prompt us to be vigilant regardless of the patient’s age, sex, and clinical presentation.

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Section: Discussionmentioning

confidence: 99%

Neuropathic Pain in Children with Sickle Cell Disease: The Hidden Side of the Vaso-Occlusive Crisis

et al. 2021

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“…Sinir sisteminin hasar görmesiyle nöropatik ağrı ortaya çıkmaktadır. Nöropatik ağrı, dokunma, basınç, ağrı, sıcaklık, titreşim algısını oluşturan somatosensör sistemin hasarlanmasıyla birlikte ortaya çıkan ağrı olarak tanımlanmaktadır (22). Çocuklarda kansere bağlı görülen nöropatik ağrının genel prevelansı bilinmemektedir (10,22).…”

Section: Kemoterapiyle İlişkili Periferik Nöropati Semptomlarıunclassified

Kanser Tedavisi Alan Çocuklarda Kemoterapiyle İlişkili Periferik Nöropatinin Değerlendirilmesinde Hemşirenin Rolü

Özdemir

Gerçeker

2022

Dokuz Eylül Üniversitesi Hemşirelik Fakültesi Elektronik Dergisi

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Kemoterapiyle ilişkili periferik nöropati, kanser tedavisinde kullanılan kemoterapik ajanların yol açtığı ciddi bir yan etkidir. Alınan kemoterapi kürleriyle giderek kötüleşen nöropati semptomları periferik sinir sisteminin duyu-motor-otonom bölgelerine hasar verebilmektedir. Bu derlemenin amacı kanser tedavisi alan çocuklara bakım veren hemşirelerin kemoterapiyle ilişkili periferik nöropati değerlendirmesindeki rolüne dikkat çekmektir. Kemoterapiyle ilişkili periferik nöropatinin ellerde-ayaklarda uyuşma, karıncalanma, kas/eklem ağrıları, yanma hissi, periferik reflekslerde azalma ve konstipasyon gibi belirtileri vardır. Bu belirtiler çocukların günlük yaşamını ve yaşam kalitelerini olumsuz yönde etkilemektedir. Kemoterapi ile ilişkili periferik nöropati görülme sıklığı kanserin tipine ve kullanılan kemoterapik ajana bağlı olarak değişmektedir. Vinkristin, sisplatin, taksan bazlı kemoterapik ajanların periferik nöropati geliştirdiği bilinmektedir. Kemoterapi tedavisi tamamlandıktan sonra bazı kemoterapik ajanların neden olduğu periferik nöropatiler azalsa da bazı ilaçların neden olduğu periferik nöropati bulguları uzun süre devam etmektedir. Hemşirelerin periferik nöropatiye yol açan kemoterapi ajanlarını bilmesi önemlidir. Hematoloji ve onkoloji servisinde çalışan pediatri hemşirelerinin, çocukların periferik nöropati semptomlarını nesnel olarak değerlendirebilecek ölçme araçlarından faydalanmaları gerekir. Nöropati değerlendirmesi hemşirelik bakımında bir rutin haline gelmelidir. Türkiye’de henüz kemoterapiyle ilişkili periferik nöropatiyi iyi bir şekilde değerlendiren bir ölçüm aracı bulunmamaktadır. Periferik nöropatiyi değerlendiren ölçüm araçlarının dilimize kazandırılması, hemşirelerin periferik nöropatinin semptomlarını (el ayaklarda karıncalanma, düğme ilikleme, merdiven inip çıkmada güçlük, yürürken sendeleme gibi duyusal, fonksiyonel ve otonom semptomlar, kas gücü ve derin tendon reflekslerinde azalmayı içeren fizik muayene bulguları) bilmesi ve nöropati değerlendirme araçlarıyla nöropatiyi değerlendirmesi önemlidir. Periferik nöropatinin yönetilmesinde farmakolojik yöntemlerin yanı sıra akupunktur, refleksoloji, masaj, ayak banyosu, kriyoterapi, scrambler terapi, progresif kas gevşeme egzersizleri, fiziksel aktivite gibi birçok farmakolojik olmayan yaklaşım bulunmaktadır ancak kanıtlar halen yetersizdir. Nöropatinin değerlendirilmesi ve yönetimi için klinik temelli çalışmalara ihtiyaç vardır.

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“… 83 , 84 Although multiple mechanisms including inflammation and pain arising from muscles, joints, and viscera may also contribute to CPSP, 85 this section will focus on neuropathic pain, because this can be difficult to recognize in children and has specific implications for management. 86 In pediatric studies, there is significant variability in the diagnostic criteria and reported prevalence of neuropathic CPSP (e.g., 10%–89% with CPSP following scoliosis surgery 87–89 ). Outcomes used to support possible or probable neuropathic pain have included history and clinical descriptors, neuropathic screening tool questionnaires, somatosensory testing, conditioned pain modulation, and response to treatment (e.g., topical lidocaine patch) 35 , 87 , 88–91 .…”

Section: Nerve Injury and Neuropathic Cpspmentioning

confidence: 99%

“… 23 Delayed emergence of neuropathic pain has also been reported following traumatic or surgical nerve injury in children. 35 , 86 , 94 The potential for preclinical studies to also link specific sensory modalities and mechanisms to efficacy of pharmacological interventions has been highlighted 95 and warrants further assessment at different developmental stages. In addition, more complex behavioral tasks in adult rodents have evaluated alterations in motivational–affective response (e.g., conditioned place preference, social interaction, anxiety) and cognitive function (e.g., memory and attention) 95–98 and have identified long-term effects following surgical injury in early life (increased anxiety, impaired attentional performance and learning 99 ).…”

Section: Nerve Injury and Neuropathic Cpspmentioning

confidence: 99%

Developmental mechanisms of CPSP: Clinical observations and translational laboratory evaluations

Walker

2021

Canadian Journal of Pain

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Understanding mechanisms that underly the transition from acute to chronic pain and identifying potential targets for preventing or minimizing this progression have specific relevance for chronic postsurgical pain (CPSP). Though it is clear that multiple psychosocial, family, and environmental factors may influence CPSP, this review will focus on parallels between clinical observations and translational laboratory studies investigating the acute and long-term effects of surgical injury on nociceptive pathways. This includes data related to alterations in sensitivity at different points along nociceptive pathways from the periphery to the brain; age- and sex-dependent mechanisms underlying the transition from acute to persistent pain; potential targets for preventive interventions; and the impact of prior surgical injury. Ongoing preclinical studies evaluating age- and sex-dependent mechanisms will also inform comparative efficacy and preclinical safety assessments of potential preventive pharmacological interventions aimed at reducing the risk of CPSP. In future clinical studies, more detailed and longitudinal peri-operative phenotyping with patient- and parent-reported chronic pain core outcomes, alongside more specialized evaluations of somatosensory function, modulation, and circuitry, may enhance understanding of individual variability in postsurgical pain trajectories and improve recognition and management of CPSP.

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Neuropathic pain in children: Steps towards improved recognition and management

Cited by 22 publications

References 76 publications

Neuropathic Pain in Children with Sickle Cell Disease: The Hidden Side of the Vaso-Occlusive Crisis

Neuropathic Pain in Children with Sickle Cell Disease: The Hidden Side of the Vaso-Occlusive Crisis

Kanser Tedavisi Alan Çocuklarda Kemoterapiyle İlişkili Periferik Nöropatinin Değerlendirilmesinde Hemşirenin Rolü

Developmental mechanisms of CPSP: Clinical observations and translational laboratory evaluations

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