Clinical Characteristics of Hereditary Multiple Exostoses: A Retrospective Study of Mainland Chinese Cases in Recent 23 Years

Hereditary multiple exostoses（HME） are an autosomal dominant skeletal disease with wide variations in clinical manifestations among different ethnic groups. This study investigated the epidemiology, clinical presentations, pathogenetic features and treatment strategies of HME in China's Mainland. We searched and reviewed the related cases published since 1990 by searching electronic databases, namely SinoMed database, Wanfang database, CNKI, Web of Science and PubMed as well as Google search engines. A total of 1051 cases of HME（male-to-female ratio 1.5：1） were investigated and the diagnosis was made in 83% before the age of 10 years. Approximately 96% patients had a family history. Long bones, ribs, scapula and pelvis were the frequently affected sites. Most patients were asymptomatic with multiple palpable masses. Common complications included angular deformities, impingement on neighbouring tissues and impaired articular function. Chondrosarcomas transformation occurred in 2% Chinese cases. Among the cases examined, about 18% had mutations in EXT1 and 28% in EXT2. Frameshift, nonsense and missense mutations represented the majority of HME-causing mutations. Diagnosis of HME was made based on the clinical presentations and radiological documentations. Most patients needed no treatment. Surgical treatment was often directed to remove symptomatic exostoses, particularly those of suspected malignancy degeneration, and correction of skeletal deformities. This study shows some variance from current literature regarding other ethnic populations and may provide valuable baseline assessment of the natural history of HME in China's Mainland.

Hereditary Multiple Exostoses (HME) with Peroneal Nerve Compresion: A Case Report

Introduction: Hereditary multiple exostosis (HME) is a hereditary disorder characterized by multiple osteochondromas. Clinical symptoms can result from compression of adjacent structures such as peripheral nerves. In Indonesia, HME with nerve compression cases have rarely reported. Presentation of Case: An eleven-year-old female with complaining of left knee joint pain and progressive masses in left lower leg since 6 years ago. This complains followed by numbness and difficulty to dorso flexion motion on left ankle joint since four months ago. Physical examination showed of the bony masses was detected at the left lateral upper third lower leg with measuring about six into eight centimeters. Range of motion of left ankle joint patient had difficult to dorso flexion. X-ray imaging viewed demonstrates multiple exostosis appearance involving distal femoral, proximal fibula, proximal tibia and distal fibula bone. MR Imaging revealed cartilage cap of head fibula is thin less 1.5 cm and the axially specimen showed peroneal nerve compression. The patient underwent left head fibula wide resection. Intraoperative findings peripheral nerve peroneal compression and was decompression. Medical rehabilitation for physiotherapy was advised. The results of the follow-up after 2 years, no pain feels and the patient was able to dorso flexion of left ankle joint and no additional bumps in other areas of the body. These lesions may arise from any bone which was pre-formed in the cartilage. Nerve compression syndromes are the neurological complex symptom caused by the mechanical or dynamic compression of a specific single segment. MRI was excellent demonstration of blood vessels compromise and represents choices with peripheral nerves structures and to measuring cartilage cap thickness for criterion of osteochondromas differentiation and exostotic grade. Complete resection was importance of the cartilaginous cap to prevent recurrence. The decompressing the peroneal nerve that pressured by the masses and vascular problems occured. Conclusion: Hereditary multiple exostosis is an inherited disorder characterized by multiple osteochondromas. It is important to monitor all cases of HME especially if the patient complains of pain or growth of an osteochondroma. The surgical excision, with complete resection of the cartilaginous cap of the tumor, is important in preventing recurrence.

遗传性多发性骨软骨瘤致病基因EXT1和EXT2的多态性研究

【目的】研究EXT1与EXT2基因在我国南方正常人及致病性突变已明确的遗传性多发性骨软骨瘤病人中的多态性。【方法】选取50例中国南方健康汉族个体及13例致病突变已明确的遗传性多发性骨软骨瘤病人,提取基因组DNA,对包含5’UTR区、编码区、外显子-内含子交界区及3’UTR区的PCR产物进行直接测序。鉴定基因内的遗传变异,并将结果和国际数据库中的数据进行对比。【结果】在所有研究对象中共发现15个不同的EXT1基因的单核苷酸多态性(SNPs):3个在编码区,为同义突变,11个在内含子区,1个在3’UTR区;其中有3个SNPs为数据库未报道的新发现多态位点。22个EXT2基因的SNPs:3个在编码区,也为同义突变,16个在内含子区,3个在3’UTR区;其中有7个SNPs为本研究新发现多态位点。【结论】中国南方汉族人与遗传性多发性骨软骨瘤病人EXT1和EXT2基因的多态性与dbSNP数据库登记资料不完全一致,某些SNPs可能存在种族差异。本研究不仅有利于了解EXT1和EXT2基因结构,也为其多态性与致病性突变的鉴定提供了依据。

遗传性多发性骨软骨瘤EXT基因的一种新突变

目的:对1个遗传性多发性骨软骨瘤(HME)家系的EXT1和EXT2基因编码序列进行突变检测,寻找引起该家系HME的致病基因突变。方法:应用PCR扩增先证者EXT1和EXT2各外显子及其侧翼序列,产物经割胶纯化后,直接测序分析。结果:DNA测序分析发现,先证者EXT1基因第7外显子区有一杂合缺失突变,为1564-7delC,导致522位后编码氨基酸发生移码突变,并在546位引入终止密码,使编码的EXT1蛋白为截断型蛋白。经家系调查发现,该突变来自先证者的母亲。先证者EXT2基因未发现突变。结论:EXT1基因1564-7delC杂合突变是引起该家系HME的分子机制。

Spontaneous pneumothorax in a 17-year-old male patient with multiple exostoses:A case report and review of the literature

BACKGROUND Multiple exostoses generally develop in the first decade of life.They most frequently arise from the distal femur,proximal tibia,fibula,and proximal humerus.Costal exostoses are rare,contributing to 1%-2% of all exostoses in hereditary multiple exostoses(HME).They are usually asymptomatic,but a few cases have resulted in severe thoracic injuries.Pneumothorax caused by costal exostoses is rare,with only 13 previously reported cases.We report a new case of pneumothorax caused by costal exostoses.CASE SUMMARY A 17-year-old male with HME underwent surgery for removal of exostoses around his right knee.Four months following the operation,he felt chest pain when he was playing the trumpet;however,he did not stop playing for a week.He was referred to our hospital with a chief complaint of chest pain.The computed tomography(CT)scan revealed right pneumothorax and multiple exostoses in his right ribs.The CT scan also revealed visceral pleura thickness and damaged lung tissues facing the exostosis of the seventh rib.We diagnosed that exostosis of the seventh rib induced pneumothorax.Costal exostosis resection was performed by video-assisted thoracoscopic surgery(VATS)2 wk after the onset.The patient’s postoperative course was uneventful,and there was no recurrence of pneumothorax for 2 years.CONCLUSION Costal exostoses causing thoracic injuries should be resected regardless of age.VATS must be considered in cases with apparently benign and relatively small exostoses or HME.

遗传性多发性骨软骨瘤临床及影像学特征观察与分析

目的: 探讨遗传性多发性外生骨软骨瘤 (hereditarymultipleexostosis, HME) 的临床及影像学特征, 以说明发病部位特点及规律。方法: 分析经临床诊断及病理证实的 2个HME家系。结果: 男性患者占 51. 6%, 女性患者占 48. 4%; 其临床表现有随遗传代次增加而加重的现象; 肿瘤好发部位位于长骨的干骺段, 颅面骨没有发现。结论: HME的发病率无性别差异, 其临床表现有遗传递增性, 发病部位具有选择性。该研究有利于进一步探索其发病机制及基因型与表现型的关系。

蛋白多糖在遗传性多发性骨软骨瘤形成中的重要作用

目的 :了解遗传性多发性骨软骨瘤 (HereditaryMultipleExostosis ,EXT )中硫酸肝素 (HeparanSulfate ,HS)链及蛋白多糖 (Perlecan)的表达 ,探讨蛋白多糖在遗传性多发性骨软骨瘤发病机制中的作用。方法 :采用免疫组织化学方法 (SABC)对 4例EXT患者骨软骨瘤软骨组织标本中HS及Perlecan的表达进行检测。与正常髂骨嵴软骨 (2例 )及小关节突软骨 (2例 )对照。结果 :遗传性多发性骨软骨瘤软骨组织不具有典型生长板软骨分层结构 ,细胞呈巢状分布 ;4例骨软骨瘤软骨细胞及基质组织中几乎都没有HS的表达 ;Perlecan定位及表达异常 :主要表达于细胞膜内侧 ,而细胞膜表面及细胞外基质表达明显减少。结论 :蛋白多糖侧链HS链及Perlecan的表达改变说明蛋白多糖在遗传性多发性骨软骨瘤发病中起重要作用。

遗传性多发性骨软骨瘤基因突变检测:附一家系报告

目的对1例遗传性多发性骨软骨瘤(HME)家系的EXT1和EXT2基因编码序列进行突变检测,寻找引起该家系HME的致病基因突变。方法PCR扩增先证者EXT1和EXT2的各外显子及其侧翼序列,PCR产物经割胶纯化后,直接测序分析。结果DNA测序分析发现,先证者EXT1基因第1外显子有一新的杂合缺失-插入突变(651-664delinsTTT),致使EXT1基因编码蛋白218位后的氨基酸发生移码突变,在220位处提前出现终止密码(K218fsX220),使编码的EXT1蛋白为截断型蛋白。家系调查发现,该突变来自于先证者母亲。先证者EXT2基因没有发现变异。结论EXT1基因651-664delinsTTT杂合突变,是引起该家系HME的分子机制。

遗传性多发性骨软骨瘤研究进展

遗传性多发性骨软骨瘤是一种常染色体显性遗传性疾病,主要表现为多发的、位于四肢长骨干骺端或扁骨表面的、由软骨帽覆盖的良性肿瘤。由于肿瘤可干扰正常骨骺的生长导致骨骼畸形,患者大多身材矮小、肢体力线异常以及功能障碍。目前研究发现,EXT基因突变与软骨瘤的形成有关,EXT基因参与硫酸乙酰肝素的合成,突变基因将导致软骨分化异常。文章综述遗传性多发性骨软骨瘤的临床症状、病理生化机制、基因型和表型相关性以及治疗方法等方面的研究进展。

骨痂延长术治疗尺骨远端遗传性多发性骨软骨瘤致前臂畸形的疗效分析

目的探讨骨痂延长术治疗尺骨远端遗传性多发性骨软骨瘤（HME）致前臂畸形的临床效果。方法 选取2013年4月-2014年4月三峡大学人民医院诊治的19例尺骨远端HME致前臂畸形患者,入选患者均采用骨痂延长术治疗,手术前后患者均使用X线进行评定,观察入选患者关节功能、相对尺骨缩短长度、桡骨关节面尺倾角、腕骨偏差率、Krimmer腕关节功能等指标。结果 患者术后相对尺骨缩短长度、桡骨关节面尺倾角、腕骨偏差率、屈肘、伸肘、前臂旋前等功能均较术前明显改善,差异有统计学意义（P〈0.05）。患者术后屈腕、伸腕及桡偏均显著大于术前,差异有统计学意义（P〈0.05）;患者手术前后尺偏比较,差异无统计学意义（P〉0.05）。患者术后Krimmer腕关节功能评分评价符合率为100.0%,高于术前的78.9%,差异有统计学意义（P〈0.05）。结论 尺骨远端HME致前臂畸形患者采用骨痂延长术治疗的效果理想,值得推广应用。

一家系遗传性多发性骨软骨瘤的致病突变基因鉴定

目的鉴定一家系遗传性多发性骨软骨瘤(HME)的致病突变基因。方法抽取该家系先证者及家系成员外周血,进行血液常规及生化项目检查,提取基因组DNA,应用全外显子组测序技术进行检测,通过生物信息学分析筛选致病变异,确定突变位点,用PCR-Sanger测序法进行突变验证。结果该家系5例患者均存在EXT1基因第6外显子c.1468dupC(p.Leu490Profs*31)杂合移码突变,表型正常家系成员未检测到该突变,符合家系基因型—表型共分离。结论导致该家系患者发病的致病突变为EXT1基因c.1468dupC(p.Leu490Profs*31)杂合移码变异,该结果进一步扩展了EXT1基因的突变谱,同时也为家系中患者的遗传咨询和产前基因诊断奠定了分子基础。

4个遗传性多发性外生性骨疣病家系的基因定位

运用分别定位于人８号、１１号和１９号染色体上的８个二核苷酸（ＣＡ）ｎ重复多态位点，用连锁分析的方法对１１个遗传性多发性外生性骨疣病（ＥＸＴ）家系进行了基因定位分析。结果提示，其中４个家系致病基因位于１１号染色体近着丝粒区域。

土家族遗传性多发性骨软骨瘤的临床特征观察与分析

目的观察湖南湘西少数民族聚集地区土家族一家系遗传性多发性骨软骨瘤(herecttitarymultipleex-ostosis,HME)的临床特征,以探讨其发病部位及规律。方法将经过临床检查及手术病理检查证实的1个HME土家族家系进行分析。结果肿瘤好发于四肢长骨的干骺端,未侵犯颅面骨、下颌骨及锁骨;临床表现有随遗传代次增加而加重的现象;发病率为男性占67.65%(23/34),女性占32.35%(11/34)。结论HME的发病无明显民族差异,但男性多于女性,发病部位有选择性,临床表现有遗传递增性。该研究有利于进一步探索其发病机制,基因型与表现型的关系,以及土家族病人的异同。

遗传性多发性骨软骨瘤的分子生物学特征

背景:遗传性多发性骨软骨瘤因较低发病率导致少有能作为临床研究的庞大家系,细胞模型、动物模型复制困难等客观因素存在对研究该疾病的发生发展机制造成了一定困扰。目的:就遗传性多发性骨软骨瘤病理改变、分子机制、信号通路等研究进展做出较为详尽的论述。方法:通过查阅往年国内外相关研究文献,研究基因网站,对相关内容及观点进行整合整理。结果与结论:①遗传性多发性骨软骨瘤是一种常染色体显性遗传性骨骼疾病,特征为多个从长管状骨的干骺端向外生长的覆盖软骨的骨肿瘤,临床症状多变,与肿瘤所在位置、大小及形状等因素有关;②该疾病具有遗传异质性,主要与EXT基因家族的肿瘤抑制基因Exostosin-1(EXT1)或Exostosin-2(EXT2)的突变相关,在分子信号通路上与硫酸乙酰肝素及其下游信号传导通路有关;③综述总结了进几十年对遗传性多发性骨软骨瘤的相关研究,希望为后续研究做出铺垫。

一个遗传性多发性骨软骨瘤家系EXT2基因的突变分析

目的对1个遗传性多发性骨软骨瘤（hereditary multiple exostosis, HME）家系候选致病基因EXTj和EXT2的编码序列进行突变分析，寻找该HEM家系的致病突变，为HME疾病的研究提供分子遗传学证据。方法对山东临沂1个HEM家系进行调查，并进行临床体格检查及影像学检查。提取家系成员外周血DNA，应用PCR技术扩增EXTl、EXT2的全部编码序列并进行直接测序分析。结果该HME家系呈常染色体显性遗传。EXTl、EXT2外显子测序结果显示，该家系中6例患者EXT2基因第2外显子均存在e．244delG杂合缺失突变，导致移码突变从而产生一个只有110个氨基酸的EXT2截短蛋白（P．Asp81 IlefsX30），而正常个体未出现该突变，即家系中该突变与疾病共分离。结论EXT2基因e．244delG突变是导致该家系的致病原因。

两个遗传性多发性软骨瘤家系EXT1及EXT2基因的突变检测

目的 对两个遗传性多发性软骨瘤(hereditary multiple exostosis,HME)家系致病基因EXT1和EXT2的编码区进行突变分析.方法 应用二代测序(next-generation sequencing,NGS)对两名先证者进行检测,对疑似突变采用Sanger双向测序对其家系成员和200例健康对照进行验证,并应用qPCR定量或多重连接探针扩增(multiple ligation-dependent probe amplification,MLPA)技术在其家系成员中进行缺失或重复验证.结果 在两个家系中分别发现了EXT1和EXT2基因的突变.家系1先证者及父亲均携带EXT2基因c.337 338insG突变,既往未见报道.在该家系的健康成员和200例健康对照中均未检测到上述突变.家系2先证者及母亲均携带EXT1基因的缺失,其父亲未携带相同的缺失.结论 EXT1、EXT2基因的突变是两个家系的致病原因.NGS结合Sanger测序、qPCR定量分析以及MLPA可以快速准确地对HME进行基因诊断.

1例遗传性多发性骨软骨瘤家系EXT1基因分析

目的遗传性多发性骨软骨瘤(HME)是一种常染色体单基因显性遗传骨发育异常疾病,超过70%为EXT1、EXT2突变所致。该文目的是分析一HME家系(3代24名成员,6名HME患者)临床特征及致病基因与突变;并通过文献复习统计分析中国人种基因突变情况。方法收集、整理、分析该家系临床资料;应用PCR及直接测序进行EXT1基因分析;应用Pubmed及万方数据库检索中国人种HME基因突变文献。结果 (1)该家系起病年龄逐代变早,骨软骨瘤发作部位及数量逐代增多,身体变形逐代严重。(2)患者均发现EXT1基因杂合剪切突变IVS5+1G>A,该突变在中国人中首次发现。(3)至今中国HME家庭(含该家系)基因突变构成比为EXT1为29%(26/90),EXT2为43%(39/90)。结论 (1)该HME家系呈现病情逐代加重情况。(2)该家系由EXT1基因剪切突变IVS5+1G>A导致发病。(3)中国人种EXT1、EXT2突变构成比与西方人不一致。

一个遗传性多发性骨软骨瘤家系EXT1基因的突变分析

目的对1个遗传性多发性骨软骨瘤（hereditary multiple exostosis, HME）家系的先证者进行候选致病基因EXTI和EXT2的所有外显子检测，以寻找该HEM家系的致病性突变。方法应用PCR技术扩增EXT1、EXT2的全部外显子并进行直接Sanger测序分析。结果测序结果显示先证者EXT1基因第4外显子存在e．1202de1T（P．1401Tfs＊2）杂合缺失突变，该突变导致401位后的编码氨基酸发生移码，并在第402位引入终止密码，使EXTl编码的全长746氨基酸组成的蛋白质缩减至由402个氨基酸组成的截短型蛋白。该家系的其他6例患者均存在EXTle．1202delT的杂合移码突变，而表型正常家系成员未检测到该突变，符合基因型一表型共分离。未检测到EXT2基因的可疑突变。结论EXT1c．1202delT杂合移码突变是导致这个HME家系患者发病的分子机制。

应用变性高效液相色谱技术检测三个遗传性多发性外生骨疣家系的EXT1与EXT2基因突变

目的建立一种应用变性高效液相色谱（denaturing high performance liquid chromatograph,DHPLC）技术检测遗传性多发性外生骨疣（hereditary multiple exostosis,EXT）基因突变的新方法,并研究3个EXT家系的基因突变情况。方法扩增EXT致病基因的所有外显子区及部分内含子与外显子交界区,联合连锁分析、DHPLC筛查及测序的方法进行分析。结果3个EXT家系中,共检测到两处已知EXT2基因的剪接位点突变IVS2＋1G〉A、IVS7＋1G〉T,一处28C〉A变异和一处EXT1基因的IVS4＋66G〉A变异。结论EXT2基因的2个剪接位点突变分别是引起相应EXT家系的致病原因,应用DHPLC技术检测遗传性疾病基因变突是一种自动化、高通量、灵敏、快速且简便经济的好方法。

两个遗传性多发性骨软骨瘤家系的致病变异鉴定

目的在两个遗传性多发性骨软骨瘤(hereditary multiple exostosis,HME)家系中进行致病候选基因EXT1和EXT2的变异鉴定,以明确其遗传学病因。方法用酚氯仿法提取先证者及其他家系成员的外周血白细胞基因组DNA,通过PCR-Sanger测序对2个家系先证者的EXT1基因外显子及外显子/内含子衔接区进行序列分析,并在患者家系中进行变异验证。结果测序结果显示家系1先证者存在EXT1基因第1外显子c.812A>G(p.Tyr271Cys)杂合错义变异;家系2先证者存在EXT1基因第6外显子c.1431dup(p.Ser478Leufs*43)杂合移码变异。两种变异均为已知致病变异。家系变异验证存在基因型和表现型共分离。结论EXT1基因第1外显子c.812A>G(p.Tyr271Cys)错义变异和第6外显子c.1431dup(p.Ser478Leufs*43)移码变异分别为这2个家系的致病原因,致病变异的检出为家系的遗传咨询和产前基因诊断提供了依据。