Neurofibromatosis Type 1: Pediatric Aspects and Review of Genotype–Phenotype Correlations
Abstract
:Simple Summary
Abstract
1. Background
2. Clinical Features of NF1 in Children and Adolescents
2.1. Cutaneous Findings
2.2. Eye Findings
2.3. Tumors
2.4. Other Complications Affecting the Nervous System
2.5. Vascular Diseases
2.6. Cardiovascular Involvement
2.7. Skeletal Manifestations
2.8. Miscellaneous
3. Follow-Up and Management
4. Genetics
4.1. Genotype–Phenotype Correlations
4.2. Association with Other Genetic Disorders
4.3. Molecular Diagnosis
5. Conclusions
Author Contributions
Funding
Acknowledgments
Conflicts of Interest
References
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Revised Diagnostic Criteria for Neurofibromatosis Type 1 (NF1) |
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A: The diagnostic criteria for NF1 are met in an individual who does not have a parent diagnosed with NF1 if two or more of the following are present: |
• Six or more café-au-lait macules over 5 mm in greatest diameter in prepubertal individuals and over 15 mm in greatest diameter in post-pubertal individuals 1 |
• Freckling in the axillary or inguinal region 2 |
• Two or more neurofibromas of any type or one plexiform neurofibroma |
• Optic pathway glioma (OPG) |
• Two or more iris Lisch nodules identified by slit lamp examination or two or more choroidal abnormalities (CAs)—defined as bright, patchy nodules imaged by optical coherence tomography (OCT)/near-infrared reflectance (NIR) imaging |
• A distinctive osseous lesion such as sphenoid dysplasia 3, anterolateral bowing of the tibia 4, or pseudarthrosis of a long bone 5 |
• A heterozygous pathogenic NF1 variant with a variant allele fraction of 50% in apparently normal tissue such as white blood cells |
B: A child of a parent who meets the diagnostic criteria specified in A merits a diagnosis of NF1 if one or more of the criteria in A are present |
1 If only café-au-lait macules and freckling are present, the diagnosis is most likely NF1 but exceptionally the person might have another diagnosis such as Legius syndrome. At least one of the two pigmentary findings (café-au-lait macules or freckling) should be bilateral. 2 If only café-au-lait spots and freckles are present, the diagnosis is probably NF1 but exceptionally the person may have another diagnosis such as Legius syndrome. At least one of the two pigment findings (café-au-lait spots or freckles) should be bilateral. 3 Sphenoid wing dysplasia is not a separate criterion in case of an ipsilateral orbital plexiform neurofibroma. 4 Congenital bowing is usually associated with thickening of the cortex of the long bone. 5 Pseudarthrosis is usually preceded by congenital curvature of a long bone and only rarely by thinning of the cortex. |
NF1 Additional Features | |
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Dystrophic scoliosis | Typical and should be clearly defined |
Juvenile xanthogranuloma | Present in up to 30% of very young patients Not reported in Legius syndrome |
Anemic nevus | Present in up to 50% of children with NF1 and may allow for clinical diagnosis at young age, but may also be seen in other conditions and in the general population |
Choroidal anomalies | Present in 60–70% of children with NF1 |
Focal areas of signal intensity (FASI) | Previously known as unidentified bright objects (UBOs) Common neuroradiological findings in brain MRI and may disappear over time |
Screening for Major NF1 Complications | |||
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Sought Complications | Affected Patients | Screening Modality | |
Dermatological manifestations | Subcutaneous, internal, and plexiform NF: malignant transformation? Esthetic or functional problems? | Children, adults | Clinical examination: Pain, neurological deficit, increase in size, functional and psychological repercussions. Additional examinations: optional Indications: suspicion of malignancy, preoperative, internal NF risk factor |
Juvenile xanthogranuloma (JXG) | Children | Physical examination: If JXG present: palpation of ganglionic areas and complete blood count * | |
Orthopedic manifestations | Bone dysplasia and pseudarthrosis of the long bones, fractures | Children, adults | Clinical examination: search for gibbosity, bone deformity. X-ray if abnormalities found on clinical examination. |
Scoliosis | Children, adults | Physical examination Additional examinations (optional): Front and profile X-ray views of the spine if clinical abnormalities found (1st line) MRI should be reserved for forms with vertebral and/or costal dysplasia (expert consensus) Pulmonary function tests to evaluate the impact of severe scoliosis | |
Bone mineralization disorder, osteoporosis | Children, adults | Consider bone densitometry scans based on clinical examination, vitamin D levels and X-ray results | |
Endocrinological manifestations | Pubertal and growth disorders | Children | Follow pubertal development and the growth curve, measure head circumference |
Cardiac and vascular manifestations | Essential and secondary hypertension | Children, adults | Physical examination: Blood pressure measurement at each consultation (at least annually), discuss the possibility of ambulatory measurement. Look for signs suggestive of pheochromocytoma. Additional examinations if high blood pressure. As a first-line examination: angio-CT scan of the renal arteries and abdominal CT. Plasma and/or urinary determination of metanephrines in adults. |
Cardiac abnormalities | Children, adults | Clinical examination | |
Hemorrhagic manifestations | Children, adults | Assess hemostasis before any surgical, dental, or obstetric procedure. | |
Pain, psychological repercussions, quality of life | Children, adults | Clinical examination Offer psychological counseling, pain specialist referral | |
Otolaryngologic manifestations | Deafness, neurinoma, phonatory disorder, laryngeal NF | Children, adults | Otolaryngologic examination with tuning fork |
Neurological manifestation | OPG | Children | Interview: repeated falls leading to suspicion of decrease visual acuity or visual field amputation Neurological and ocular examination: strabismus, nystagmus, low visual acuity, neurological deficit, signs of intracranial hypertension. Early puberty, deviation from the growth curve, measurement of head circumference Ophthalmological screening at least once per year until the age of 13 years and then if signs appear. MRI of the optic and cerebral pathways is not systematic and should be performed only if suspicion of OPG |
Epilepsy, hydrocephalus, intracranial, hypertension, stroke, headache | Children, adults | Neurological examination Cerebral MRI and electroencephalogram guided by the abnormalities detected on clinical examination | |
Developmental delay, learning difficulties, behavioral problems | Children | Evaluation of psychomotor development and academic proficiency at each consultation Search for learning difficulties Comprehensive neuropsychomotor assessment before entering elementary school, support for school integration. | |
Medullary and nerve compression, peripheral neuropathy, socio-professional integration | Adults | Clinical examination | |
Cancers | MPNST (60% of cancers in NF1 patients) | Children, adults | Clinical examination: recent increase in size of plexiform NF, appearance of pain. Additional examinations if signs appear. If high NF1 score: screening for internal neurofibromas by imaging (preferably by MRI). |
All other cancers | Children, adults | Clinical examination: asthenia, high blood pressure, intracranial hypertension symptoms, abdominal mass, bladder signs, appearance of mass, compressive syndrome Screening identical to that of the general population except for earlier breast screening (>40 years) |
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Peduto, C.; Zanobio, M.; Nigro, V.; Perrotta, S.; Piluso, G.; Santoro, C. Neurofibromatosis Type 1: Pediatric Aspects and Review of Genotype–Phenotype Correlations. Cancers 2023, 15, 1217. https://doi.org/10.3390/cancers15041217
Peduto C, Zanobio M, Nigro V, Perrotta S, Piluso G, Santoro C. Neurofibromatosis Type 1: Pediatric Aspects and Review of Genotype–Phenotype Correlations. Cancers. 2023; 15(4):1217. https://doi.org/10.3390/cancers15041217
Chicago/Turabian StylePeduto, Cristina, Mariateresa Zanobio, Vincenzo Nigro, Silverio Perrotta, Giulio Piluso, and Claudia Santoro. 2023. "Neurofibromatosis Type 1: Pediatric Aspects and Review of Genotype–Phenotype Correlations" Cancers 15, no. 4: 1217. https://doi.org/10.3390/cancers15041217
APA StylePeduto, C., Zanobio, M., Nigro, V., Perrotta, S., Piluso, G., & Santoro, C. (2023). Neurofibromatosis Type 1: Pediatric Aspects and Review of Genotype–Phenotype Correlations. Cancers, 15(4), 1217. https://doi.org/10.3390/cancers15041217