A Research of Pachyonychia Congenita Type 1 and Literature Analysis

Pachyonychia congenital (PC), consist of a group of rare autosomal-dominant ectodermal disorders. Symmetrically thickened, dystrophic fingernails and toenails are the defining characteristic of pachyonychia congenita. There are two main clinical subtypes of pachyonychia congenita: Pachyonychia congenita-1 and pachyonychia congenita-2. Pachyonychia congenita-U is another subtypes of pachyonychia congenita, where either a mutation has not been found or has not been investigated. Objectives: The present aim was to indentify the mutation of keratin 6a or keratin 16 gene in the pachyonychia congenita patient. Methods: The proband, her parents and 100 unrelated controls were subjected to mutation detection in keratin 6a or keratin 16 gene. Direct sequencing of all PCR products of the whole coding regions of keratin 6a or keratin 16 was performed to identify the mutation. Results: No mutation was found in keratin 6a or keratin 16 in the proband, her parents, and 100 unrelated and unaffected people. Conclusion: This study reported a Chinese female affected with pachyonychia congenita-1 without mutation in keratin gene.

Special electromyographic features in a child with paramyotonia congenita: A case report and review of literature

BACKGROUND Paramyotonia congenita(PMC)stands as a rare sodium channelopaty of skeletal muscle,initially identified by Eulenburg.The identification of PMC often relies on electromyography(EMG),a diagnostic technique.The child’s needle EMG unveiled trains of myotonic discharges with notably giant amplitudes,alongside irregular wave trains of myotonic discharges.This distinctive observation had not surfaced in earlier studies.CASE SUMMARY We report the case of a 3-year-old female child with PMC,who exhibited la-ryngeal stridor,muffled speech,myotonia from birth.Cold,exposure to cool water,crying,and physical activity exacerbated the myotonia,which was relieved in warmth,yet never normalized.Percussion myotonia was observable in bilateral biceps.Myotonia symptoms remained unchanged after potassium-rich food consumption like bananas.Hyperkalemic periodic paralysis was excluded.Cranial magnetic resonance imaging yielded normal results.Blood potassium remained within normal range,while creatine kinase showed slight elevation.Exome-wide genetic testing pinpointed a heterozygous mutation on chromosome SCN4A:c.3917G>A(p.G1306E).After a six-month mexiletine regimen,symptoms alleviated.CONCLUSION In this case revealed the two types of myotonic discharges,and had not been documented in other studies.We underscore two distinctive features:Giant-amplitude potentials and irregular waves.

Surgical treatment of atlantoaxial dysplasia and scoliosis in spondyloepiphyseal dysplasia congenita:A case report

BACKGROUND Spondyloepiphyseal dysplasia congenita(SEDC)is a rare autosomal dominant hereditary disease caused by COL2A1 mutations.SEDC primarily involves the skeletal system,with typical clinical manifestations,including short stature,hip dysplasia,and spinal deformity.Due to the low incidence of SEDC,there are only a few case reports regarding the surgical treatment of SEDC complicated with spinal deformities.CASE SUMMARY We report a case of a 16-year-old male patient with SEDC.He presented with typical short stature,atlantoaxial dysplasia,scoliosis,and hip dysplasia.Cervical magnetic resonance imaging showed spinal canal stenosis at the atlas level and cervical spinal cord compression with myelopathy.The scoliosis was a right thoracic curve with a Cobb angle of 65°.He underwent atlantoaxial reduction,decompression,and internal fixation from C1–C2 to relieve cervical myelopathy.Three months after cervical surgery,posterior correction surgery for scoliosis was performed from T3 to L4.Scoliosis was corrected from 66°to 8°and remained stable at 2-year follow-up.CONCLUSION This is the first case report of a patient with SEDC who successfully underwent surgery for atlantoaxial dysplasia and scoliosis.The study provides an important reference for the surgical treatment of SEDC complicated with spinal deformities.

Type VI Aplasia Cutis Congenita: About a Case Report at University Teaching Hospital of Bouaké

Introduction: Aplasia cutis congenita is a rare congenital dermatosis of which type VI represents the Bart’s syndrome. The aim of this case is to describe the epidemiological, clinical, therapeutic and prognostic characteristics of this condition in a country with limited resources, for the improvement of prognosis and professional practice. Observation: This is a eutrophic newborn, born at term by vaginal delivery, who presented at birth with a unilateral absence of skin on the anteromedial aspect of the right leg starting from the knee and extending to the medial aspect of the right foot, with a dystrophy of the nail of the right big toe without any other visible physical malformation. The evolution was marked at D3 of life by the appearance of bullae on the right hand and elbow as well as on the posterior aspect of the neck, making epidermolysis bullosa suspect. The mother was 38 years old, 8th gesture, 7th pare with history of consanguinity and collodion baby. The association of a localized congenital absence of skin on the lower limbs, epidermolysis bullosa and a nail anomaly led to the diagnosis of congenital cutaneous aplasia of type VI of Frieden’s classification or Bart’s syndrome. The evolution was satisfactory on the 7th day of life with the beginning of scarring. The management was medical. The outcome was unfavorable with the appearance of sepsis and hemorrhage leading to death. Conclusion: Although rare, the clinical diagnosis of Bart’s syndrome is simple. However, the management is complex and the prognosis is reserved. To improve this prognosis, the treatment must guarantee excellent control of the infectious and hemorrhagic risks, an adhesion and good therapeutic compliance by the parents and a rigorous monitoring.

A Case of Coexistence of Aplasia Cutis Congenita and Giant Congenital Melanocytic Nevus:Coexistence of Two Rare Skin Diseases

Aplasia cutis congenita(ACC)is a rare disease that is characterized by complete or partial absence of skin at birth,either in a localized or widespread region.Melanocytic nevi refers to tumor-like malformations of the skin or mucous membrane caused by benign proliferation of melanocytes.It is classified as a giant congenital melanocytic nevus(GCMN)when the diameter of the largest nevus exceeds 20 cm.The co-occurrence of ACC and GCMN is extremely rare,to the best of our knowledge.We report a case of coexistence of ACC and GCMN of infancy in a 2-month-old male infant.The lesions consisted of a large hyperpigmented plaque occupying most of the trunk and pelvic region,and smaller hyperpigmented plaques on the trunk,head,and extremities.Additionally,there were large,sharply marginated,triangular,depressed atrophic plaques covered by thin,translucent,glistening epithelial membranes in the center of the GCMN on the back.The presumptive diagnosis was coexistence of GCMN and ACC.This could be a manifestation of SCALP syndrome,a rare neuro-cutaneous condition characterized by the presence of Sebaceous nevus,Central nervous system(CNS)malformations,Aplasia cutis congenita,Limbal dermoid and Pigmented(giant melanocytic)nevus.

Treating aplasia cutis congenita in a newborn with the combination of ionic silver dressing and moist exposed burn ointment: A case report

BACKGROUND Aplasia cutis congenita (ACC) in newborns is a condition in which congenital defects or hypoplasia is present in part of the epidermis,dermis and even subcutaneous tissue (including muscle and bones).First reported by Cordon in 1767,ACC is a rare disease with a low incidence of 1/100000 to 3/10000.Currently,there are 500 cases reported worldwide.ACC can be accompanied by other malformations.The onset mechanism of the disease remains unknown but is thought to be correlated to factors such as genetics,narrow uterus,foetal skin and amniotic membrane adhesion,use of teratogenic drugs in early pregnancy and viral infection.CASE SUMMARY In August 2018,we treated a newborn with ACC on the left lower limbs using a combination of ionic silver dressing and moist exposed burn ointment (MEBO) and achieved a satisfactory treatment outcome.The skin defects were observed on the external genitals and on areas from the left foot to 3/4 of the upper left side.Subcutaneous tissue and blood vessels were observed in the regions with skin defects.The following treatments were provided.First,the wound was rinsed with 0.9% sodium chloride solution followed by disinfection with povidone-iodine twice.And then MEBO was applied to the wound at a thickness of approximately 1 mm.After applying ionic silver dressing,the wound was covered with sterile gauze.The wound dressing was replaced every 2-3 d.At the 4-mo follow-up,the treatment outcome was satisfactory.There was minimal scar tissue formation,and limb function was not impaired.CONCLUSION The combination of ionic silver dressing and MEBO to ACC is helpful.

Clinical characteristics of myotonia congenita in China Literature analysis of the past 30 years

AIM： To understand the distinct, clinical features of myotonia congenita in China. METHODS： Case reports of myotonia congenita were retrieved from the Chinese Journal Full-text database, dating between 1980 and 2007, and analyzed for clinical characteristics of myotonia congenita. RESULTS： There were 35 published reports and 258 cases about myotonia congenita. Six reports （62 cases） were excluded due to lack of clinical data, imprecise diagnosis, or duplication. Finally, 29 published reports and 196 cases （140 males and 56 females） were included in this analysis. About 78.6% of patients were diagnosed with myotonia congenita before the age of 20, and among these, 86.1% were classified as dominant inheritance. Lower and upper extremities were frequently affected with severe symptoms. Eyelids, mouth and lingual muscles, and trunk muscles and cervical muscles were less frequently involved. However, muscles for swallowing, sphincter muscles, and smooth muscles were not involved. There were no reports of cataracts, cardiac conduction block, or dyscrinism. myotonia congenita symptoms were induced or aggravated by cold temperatures in 71.9% of the patients and warming-up effect occurred in 95.6% of the patients. Muscle hypertrophy was observed in 69.6% and percussion of muscles in 76.5% of the patients. Myotonia potential or myotonia-like potential was detected in all patients using electromyography. Muscle fiber swelling or hypertrophy was frequently detected through muscular biopsy. CONCLUSION： Myotonia congenita frequently occurs in males before the age of 20, in particular as the autosomal dominant form of myotonia congenita. Skeletal muscles throughout the body, especially the lower and upper extremities, are involved. However, muscles for swallowing, sphincter muscles, and smooth muscles are not involved. Warming-up effect is the main characteristic of myotonia congenita.

A Novel NR0B1 Gene Mutation Causes Different Phenotypes in Two Male Patients with Congenital Adrenal Hypoplasia

X-linked congenital adrenal hypoplasia is characterised by the acute onset of primary adrenal insufficiency in infancy or early childhood and hypogonadotropic hypogonadism(HH)at puberty,arising from mutations of the nuclear receptor subfamily 0 group B member 1(NR0B1)gene.This study investigated an extended family with two affected males(patient A:23 years and patient B:2 months old)and three carrier females.Sequencing analysis of the NR0B1 gene coding region from the family revealed a novel hemizygous deletion[c.604delT;p.(C202Afs*62)]in the two male patients.Furthermore,the patients'respective mothers and their common grandmother had this heterozygous mutation,but it was not present in the Human Gene Mutation Database.The two male patients showed inconsistent clinical features at onset,particularly in early childhood;however,it is possible that the younger patient will eventually show a delay of puberty,feminisation,and nonspermatogenesis in adulthood,similar to that in the older patient.Identification of a novel NR0BI mutation in this family is important for the diagnosis and genetic counselling of children with primary adrenal insufficiency and HH,and will be helpful for predicting long-term clinical symptoms.

Novel TINF2 gene mutation in dyskeratosis congenita with extremely short telomeres:A case report

BACKGROUND Dyskeratosis congenita is a rare disease characterized by bone marrow failure and a clinical triad of oral leukoplakia,nail dystrophy,and abnormal skin pigmentation.The genetics of dyskeratosis congenita include mutations in genes involved in telomere maintenance,including TINF2.CASE SUMMARY Here,we report a female patient who presented thrombocytopenia,anemia,reticulate hyperpigmentation,dystrophy in fingernails and toenails,and leukoplakia on the tongue.A histopathological study of the skin showed dyskeratocytes;however,a bone marrow biopsy revealed normal cell morphology.The patient was diagnosed with dyskeratosis congenita,but her family history did not reveal significant antecedents.Whole-exome sequencing showed a novel heterozygous punctual mutation in exon 6 from the TINF2 gene,namely,NM_001099274.1:-c.854delp.(Val285-Alafs*32).An analysis of telomere length showed short telomeres relative to the patient’s age.CONCLUSION The disease in this patient was caused by a germline novel mutation of TINF2 in one of her parents.

A patient with dyskeratosis congenita and portal hypertension

Portal hypertension(PH)refers to a collection of syndromes characterized by an increase in pressure within the portal venous system and/or elevated portal venous blood flow,most commonly caused by cirrhosis.This condition is frequently associated with viral hepatitis and chronic alcohol abuse,and its complications,such as ascites,hepatic encephalopathy,and esophageal varices,have a considerable impact on mortality.Dyskeratosis congenita(DC)is a rare genetic disorder that affects multiple systems,most notably manifesting as dystrophy of the fingernails and toenails,skin pigmentation,and mucosal leukoplakia.While cirrhotic PH is an uncommon complication of DC,we present a case of a young patient who presented with PH and had no history of hepatitis or heavy alcohol use.The patient underwent splenectomy and devascularization to treat hypersplenism and esophagogastric varices caused by PH but developed portal vein thrombosis following the surgery.Given the patient's cutaneous manifestations and cirrhosis that could not be attributed to common causes,we continued to search for the underlying cause of PH until the diagnosis of DC was finally made.The patient was subsequently treated with carvedilol to prevent variceal rebleeding and showed no significant complications or bleeding during follow-up.

Paroxysmal kinesigenic dyskinesia and myotonia congenita in the same family:coexistence of a PRRT2 mutation and two CLCN1 mutations

Paroxysmal kinesigenic dyskinesia（PKD） and myotonia congenita（MC） are independent disorders that share some clinical features. We aimed to investigate the sequences of PRRT2 and CLCN1 in a proband diagnosed with PKD and suspected MC. Clinical evaluation and auxiliary examinations were performed. Direct sequencing of the entire coding regions of the PRRT2 and CLCN1 genes was conducted. Haplotype analysis confirmed the relationships among the family members. The proband suffered choreoathetosis attacks triggered by sudden movements, and lower-limb weakness a n d s t i ff n e s s t h a t w o r s e n e d i n c o l d w e a t h e r. Carbamazepine monotherapy completely controlled his choreoathetosis and significantly relieved his limb weakness and stiffness. His father, when young, had similar limb stiffness, while his mother and brother were asymptomatic. Genetic analysis revealed that the proband and his father harbored a PRRT2 c.649 dup C mutation, and CLCN1 c.1723C〉T and c.2492A〉G mutations. His brother carried only the two CLCN1 mutations. None of these mutations were identified in his mother and 150 unrelated controls. This is the first report showing the coexistence ofPRRT2 and CLCN1 mutations. Our results also indicate that both the PRRT2 and CLCN1 genes need to be screened if we fail to identify PRRT2 mutations in PKD patients or CLCN1 mutations in MC patients.

先天性多发性关节挛缩症康复专家共识

先天性多发性关节挛缩症(Arthrogryposis multiplex congenita,AMC)是累及身体多个部位挛缩和畸形的疾病,致残率高,严重影响患者的日常生活。本共识以循证医学证据为依据,经全国肢体畸形专家组反复研讨,结合近年来国内外研究成果,基于渐进式精准康复理念,为AMC患者制定个性化康复策略,规范康复流程,制定全周期康复管理标准,有效提高患者康复疗效。本共识主要包括康复目标、康复团队组成与职责、康复治疗方法、康复工程技术以及定期随访,可供临床医师、康复医师、康复治疗师、康复工程师、护师等在工作中参考及应用。

Aplastic anemia associated with dyskeratosis congenita treated with antilymphocyte globulin and cyclosporine: a case report

Dyskeratosis congenita (DC) is a severe inherited disease characterized by a triad of clinical manifestations including abnormal skin pigmentation, nail dystrophy, and mucosal leukoplakia. 1 Bone marrow failure is the principal cause of early mortality, together with an increased predisposition to malignancy and fatal pulmonary complications. According to the dyskeratosis congenita registry, a peripheral blood cytopenia of one or more lineages is reported in 93% of patients, with 51% developing pancytopenia before the age of 10 years. 2 In patients with DC, bone marrow failure or bone marrow failure treatment-associated complications account for 67% of total mortality. 3 Therefore, management of bone marrow failure syndrome is crucial in patients with DC.

异基因造血干细胞移植治疗儿童先天性角化不良3例并文献复习

目的 初步探讨异基因造血干细胞移植(HSCT)治疗儿童先天性角化不良(DKC)的疗效,为探索优化移植方案提供依据。方法 回顾性分析自2019年6月至2022年6月在医院行HSCT的3例DKC患儿的临床资料并复习相关文献。结果 3例患儿预处理方案为以氟达拉滨(Flu)为主的减低剂量预处理。回输单个核细胞(MNC)中位计数为13.7(8.3~17.3)×10^(8)/kg,CD 34+细胞中位计数为8.2(6.3~13.1)×10^(6)/kg。采用甲氨蝶呤、环孢素和吗替麦考酚酯联合预防移植物抗宿主病(GVHD)。HSCT预处理过程中3例患儿均能耐受;中性粒细胞植入中位时间11(10~11)d,血小板植入中位时间11(10~13)d,未发生原发性植入失败;2例发生不同程度急性GVHD,1例发展为慢性GVHD,1例移植后出现可逆性后部脑白质综合征(RPLS)。随访至2023年1月,随访中位时间19(11~42)个月,3例均存活,1例存在慢性GVHD,目前3例患儿均脱离输血,移植后血细胞未再检测出DKC相关基因突变,生长发育同正常同龄儿童,目前尚未发现合并实体肿瘤。结论 DKC患者HSCT治疗采用“Flu+低剂量环磷酰胺(CTX)+抗人胸腺淋巴细胞球蛋白(ATG)”预处理方案耐受性尚可,无原发性植入失败发生;GVHD仍是影响患儿生存主要因素,探索个体化方案治疗DKC的临床研究非常必要。

Bone Defect of the Cranial Vault: Difficulty of the Diagnostic about a Case, and Revew of Literature

The bone defects of the cranial vault encompassed rare malformations including acalvaria, hypocalvaria, acrania, hypocrania, anencephaly and exencephaly. They are also described in some pathological entities such as aplasia cutis congenita of the scalp. We report an unusual case of cephalic malformation which combine defects of the skin, the dura mater, and the bones of the vault, with a malformation of the central nervous system. This unique case emphasizes a problem of nosological definition between the terms mentioned above. acalvaria, the acrania, the hypocalvaria and the aplasia cutis congenita. Thus, herein, we proceed to a literature review of bone defects of the skull and their differential diagnosis.

自发突变致先天性厚甲症-K6a

患儿女,4个月。因双手指甲增厚4个月就诊。患儿出生后3 d即开始出现双手指甲增厚、变黄;4个月龄时,双手足20甲均增厚,呈爪状;随访至8个月龄时,双手指甲下充满硬性角质样物质,呈楔形增厚,右手食指、左足拇趾掌侧出现角化;基因检测:KRT6A基因第7外显子存在一个杂合突变c.1390A>C(p.T464P),患儿父母及其他家属均无相关症状,且其父母基因检测回报未发现该突变位点,结合本患儿临床表现和基因结果,诊断先天性厚甲症(PC-K6a)。

合并椎体或椎管内异常对后路矫形手术治疗伴先天性关节挛缩症脊柱侧凸疗效的影响

目的:分析椎体或椎管内异常对后路矫形手术治疗伴有先天性关节挛缩症(arthrogryposis multiplex congenita,AMC)脊柱侧凸患者效果的影响。方法:回顾性分析2001年8月~2021年11月于我院行后路矫形手术治疗的伴AMC脊柱侧凸的患者30例,其中男18例,女12例,年龄6~32(15.9±5.8)岁。根据是否伴有椎体或椎管内异常,将患者分为异常组(15例)和对照组(15例)。记录异常组患者椎体或椎管内异常的类型,比较两组患者融合节段个数、手术时间及术中出血量,记录随访过程中的并发症。结合仰卧位Bending片计算两组患者主弯柔韧度,于术前、术后2周及术后2年的立位全脊柱正侧位X线片上测量主弯侧凸Cobb角、冠状面平衡(C7PL-CSVL)、矢状面平衡(SVA)、胸椎后凸角(TK)和腰椎前凸角(LL),计算术后2周及末次随访的主弯矫正率。结果:在异常组中单纯分节不良10例(66.6%),分节不良合并脊髓拴系2例(13.3%),分节不良合并蛛网膜囊肿、单纯半椎体、单纯楔形椎各1例(6.7%)。两组间融合节段个数、手术时间及术中出血量均无统计学差异(P>0.05)。异常组术中未发生并发症,术后发现椎弓根螺钉位置不良2例,胸腔积液及右侧臂丛神经麻痹1例;对照组术中出现恶性高热及心搏骤停1例,术后发现椎弓根螺钉位置不良3例,胸腔积液及置钉失败1例,两组并发症发生率无统计学差异(P=0.628)。两组患者术前主弯柔韧度无统计学差异(P>0.05);术前、术后2周及术后2年时的主弯侧凸Cobb、C7PL-CSVL、SVA、TK及LL均无统计学差异(P>0.05);术后2周和术后2年的主弯矫正率亦无统计学差异(P>0.05)。结论:椎体或椎管内异常对后路矫形手术治疗伴AMC脊柱侧凸患者效果无明显影响,且术中和术后并发症发生率无明显差异。

以明显脾大及低氧血症为首发表现的先天性角化不良1例

先天性角化不良是临床上一种罕见的遗传性疾病。本文报道滨州医学院附属医院1例以明显脾肿大、门静脉高压、低氧血症为首发表现的先天性角化不良的青少年病例,并且就先天性角化不良的诊断思维及本病例的疑点、难点展开讨论。

先天性厚甲症2型一家系的基因突变研究

目的研究先天性厚甲症的基因突变,从而探讨基因型与表现型之间的关系。方法提取1个先天性厚甲症家系中先证者及其家人的外周血基因组DNA,用聚合酶链反应扩增,产物测序检测。取先证者母亲的皮损做组织病理检查,观察皮损组织的角蛋白17的表达。结果家系中两患者的角蛋白17的1号外显子第275位碱基发生A→G的杂合突变,其突变导致其编码角蛋白17的第92位氨基酸的密码子发生改变,使其编码的氨基酸由天冬酰胺变为丝氨酸(N92S)。先证者母亲皮损组织病理检查为多发性脂囊瘤,免疫组化显示角蛋白17阳性表达。结论验证了角蛋白17的1号外显子α螺旋1A区突变在先天性厚甲症发病机制中的重要作用。角蛋白17 1A区突变对脂囊瘤的早发可能存在一定影响,基因型与表型存在一定关联。

伴皮角样损害的先天性厚甲症

报告1例伴有皮角样损害的先天性厚甲症。患者男,17岁。因指、趾甲增厚伴全身出现泛发皮角样改变就诊。患者自3岁起逐渐出现20甲变黄、增厚、分离,伴发严重掌跖角化,以及多发性皮角样损害。患者角蛋白基因KRT6A、KRT6B、KRT16、KRT17以及连接蛋白基因GJB6编码区的全部外显子及其侧翼序列均未检测到致病性突变。