Study Group on the development of clinical practice and research systems for rare and refractory renal diseases in pediatric nephrology
Study Group on the development of clinical practice and research systems for rare and refractory renal diseases in pediatric nephrology
Nail–patella syndrome is a hereditary disease characterized by dysplastic nails (nails with abnormal shape), absent or hypoplastic patellae (small or missing knee caps), elbow dysplasia (elbow deformities), and iliac horns (bony outgrowths of ilium). Patients often develop concurrent kidney disease. The syndrome is caused by mutations of a gene called LMX1B. The renal lesions typical of NPS have also been found in patients with kidney disease alone without skeletal or nail abnormalities. This condition is called LMX1B-associated nephropathy (kidney disease).
Nail-pateila syndrome is characterized by abnormal nail shape, knee abnormalities such as missing kneecaps, and limitation of elbow joint extension. X-ray may show bony out growths of the ilium. Patients may have only one or some of these symptoms, but nail abnormalities are observed in almost all patients. In addition, glaucoma and increased intraocular pressure are observed more often and at a younger age than the general population. Kidney disease ranging from mild urinary abnormality (hematuria or proteinuria) to end-stage kidney disease (ESKD) also occurs in individuals with NPS, and can be a significant threat to quality of life.
In LMX1B-associated nephropathy, patients only have kidney disease that occurs in nail-patela syndrome,without extrarenal manifestations.
There is no specific treatment for nail, knee, or elbow joint abnormalities in nail-patella syndrome. Analgesics or appliances (called braces) may be used in some patients. There are also patients who require surgical treatment for joint symptoms or glaucoma. For kidney disease, treatment for chronic kidney disease may apply, depending on kidney function.
The prevalence has been estimated to be 1 in 50,000. However, the estimation is not based on the number of patients reported in Japan. The frequency in Japan is presently unknown.
No racial differences in incidence rates have been reported. Because it is a genetic disease,it may be more common in families with patients.
Mutations in the LMXIB gene cause nail-patella syndrome. However, there are patients with typical symptoms in whom no abnormalities in LMX1B can be detected.
It is an autosomal dominant hereditary disease. If one of the parents is affected by this disease, their child has a 1 in 2 chance of inheriting the disease. However, it also occur in patients with no apparent family history because the disease can be caused by a de novo mutation. Furthermore, individuals within the same pedigree carrying the same mutation may have different symptoms and severity.
Nail, knee, or elbow joint abnormalities generally do not improve with aging. The severity of nephropathy varies among patients, with some progressing to end-stage kidney disease.
In some patients who have joint abnormalities, exercise restriction may be required. To test for concurrent nephropathy, periodic urine tests should be performed. If abnormal urinary findings are observed, kidney function tests are recommended.
Nail hypoplasia or dysplasia
(It is often present in the fingers, prominently on the thumb side. If it is present in the toes, the condition is more prominent in the little toe side. Severity varies from complete absence to hypoplasia. In some individuals, minor abnormality such as triangular lanulae, spoon nail, discoloration, or splits are the only feature. The condition is often observed from birth. The mild abnormalities can be easily missed.)
Heterozygous mutation in the LMXIB gene
All the following differential diagnoses are excluded
Definite: (A) + (at least one criterion of B or C) + (D)(exclude differential diseases in D)
Characteristic electron microscopic findings of the glomerular basement membrane
(Kidney biopsy is considered in patients with kidney impairment, but it is not essential for diagnosis of nephropathy of this disease. Characteristic histopathological findings are thickening or a moth-eaten appearance of the glomerular basement membrane. The deposition of type III collagen fibers can observed in the lamina densa in the thickened glomerular basement membrane or in the mesangial matrix. Fibril clusters in glomerular basement membrane can be stained with phosphotungstic acid, tannic acid, or uranyl acetate/lead citrate staining.)
Heterozygous mutation in the LMXIB gene
(Genetic testing for the LMXIB gene mutation is considered for patients with abnormal urinary findings or renal dysfunction whose kidney biopsy demonstrates characteristic findings of the glomerular basement membrane by electron microscopy, or who have family history of kidney disease consistent with autosomal dominant inheritance.)
Definite: (Both criteria of A) + (at least one criterion of B or C)
Cases with other causes for kidney impairment (morphological abnormalities of kidney, or kidney diseases due to other known gene abnormalities, other than LMXIB gene) should be excluded.
Cases are categorized as “severe” by the Chronic Kidney Disease
Severity Classification (categorized as “Red” in the chart below) or by urinary protein/creatinine ratio greater or equal to 0.5g/gCr regardless of kidney function.
*Points to be considered when applying the diagnostic criteria and the severity classification
*The diagnostic criteria was developed by a research group supported by Health and Labour Sciences Research Grant (H26-015).
