Norrbottnian congenital insensitivity to pain.

Acta orthopaedica. Supplementum Pub Date : 2006-04-01
Jan K Minde
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Abstract

Congenital insensitivity to pain is a rare hereditary neuropathy. We present patients from a large family in Norrbotten, Sweden with a mutation in the nerve growth factor beta gene (NGFbeta). Using a model of recessive inheritance, we identified an 8.3-Mb region on chromosome 1p11.2-p13.2 shared by the affected individuals in the family. Analysis of candidate genes in the disease-critical region revealed a mutation in the coding region of the NGFbeta gene specific for the disease haplotype. All three severely affected individuals were homozygous for the mutation. The disease haplotype was also observed in both unaffected and mildly affected family members, but in heterozygote form. We have identified 43 patients, 3 homozygous and 40 heterozygous. The homozygous patients have a severe congenital form with onset of symptoms at an early age, most often affecting the lower extremities with insidious progressive joint swellings or painless fractures. Fracture healing was normal, but the arthropathy was progressive, resulting in disabling Charcot joints with gross deformity and instability. These patients lacked deep pain perception in bones and joints and had no protective reflexes, leading to gross bone and joint complications. They also had abnormal temperature perception but normal ability to sweat. There was no mental retardation. Clinically, they fit best into the group HSAN type V. Sural nerve biopsies showed a moderate loss of thin myelinated fibers (Adelta-fibers) and a severe reduction of unmyelinated fibers (C-fibers). 14 of the 40 heterozygous adult patients had mild or moderate problems with joint deformities, usually with only slight discomfort. Treatment was conservative with (if needed) different kinds of orthosis and in three cases joint replacement. Nine patients had neuropathy, and nine patients had no symptoms. In congenital disorders like these, it is important to evaluate the age and also the slowly progressive nature, when considering treatment. There is an increased risk of growth disturbances in the very young. The orthopedic operations should therefore be planned from a long-term point of view, but patient education and orthosis are cornerstones in the treatment--to delay the development of neuropathic arthropathy. Arthrodesis, limb lengthening and spinal decompression with fusions are the only elective procedures that seem reasonable. This Norrbottnian disease is also interesting as a model system for the study of pain.

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北爱尔兰人天生对疼痛不敏感。
先天性疼痛不敏感是一种罕见的遗传性神经病变。我们介绍了来自瑞典Norrbotten的一个大家庭的患者,他们的神经生长因子β基因(ngfβ)发生了突变。利用隐性遗传模型,我们发现家族中受影响个体在染色体1p11.2-p13.2上共有8.3 mb区域。对疾病关键区候选基因的分析显示,该疾病单倍型特异性ngf - β基因编码区发生突变。所有三个受严重影响的个体都是突变的纯合子。在未受影响和轻度受影响的家庭成员中也观察到该疾病的单倍型,但以杂合子形式存在。共鉴定43例,其中纯合子3例,杂合子40例。纯合子型患者有严重的先天性形式,早期出现症状,最常影响下肢,伴有潜伏的进行性关节肿胀或无痛性骨折。骨折愈合正常,但关节病变是进行性的,导致Charcot关节失能,伴有明显畸形和不稳定。这些患者缺乏骨骼和关节的深度痛觉,没有保护性反射,导致骨和关节的严重并发症。他们也有异常的温度感知,但正常的出汗能力。没有智力障碍。临床上,他们最适合HSAN v型组。腓肠神经活检显示薄髓鞘纤维(adelta纤维)中度丢失,无髓鞘纤维(c -纤维)严重减少。40例杂合子成年患者中有14例有轻度或中度关节畸形问题,通常只有轻微的不适。治疗是保守的(如果需要)不同种类的矫形器和三例关节置换术。9例有神经病变,9例无症状。对于像这样的先天性疾病,在考虑治疗时,重要的是要评估患者的年龄和缓慢进展的性质。在非常年轻的时候,生长障碍的风险会增加。因此,骨科手术应从长远的角度进行规划,但患者教育和矫形器是治疗的基石,以延缓神经性关节病的发展。关节融合术、肢体延长术和脊柱减压融合术是唯一合理的选择。这种北方疾病作为疼痛研究的模型系统也很有趣。
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