McCune-Albright综合征

McCune-Albright综合征是一种少见的G蛋白病,临床以性早熟、多发性骨纤维异常增殖症及皮肤斑片状色素沉着为最常见的症状,病因是在胚胎形成过程中的鸟嘌呤核苷酸结合蛋白(G蛋白)α亚基(Gsα)基因的突变,导致刺激cAMP产生可激活许多内分泌激素的受体。治疗主要是对症治疗,尚无有效根治方法。该文报道3例该病病例,并复习了相关文献。这3例病例均出现多发性骨纤维异常增殖症、性早熟及咖啡色色素斑典型的三联征而确诊。

McCune-Albright综合征1例报告并文献复习

目的:探讨并提高对McCune-Albright综合征的认识。方法:通过1例McCune-Albright综合征患者的临床资料和文献复习,详细分析McCune-Albright综合征的病因、临床表现、诊断、治疗及预后。结果:目前遵循的MAS诊断标准为:具有多发性骨纤维发育不良、加上至少一种典型的内分泌功能亢进,和(或)特异性皮肤色素沉着。基因诊断,可通过从超声引导下穿刺卵巢滤泡得到的囊内液、异常骨组织等病灶中取材行基因分析,发现Gsα基因的突变而确定。结论:McCune-Albright综合征在临床上十分少见且尚未被国内多数临床医生所认识,易被误诊或漏诊。治疗主要是对症治疗,尚无有效根治方法。对于性早熟的患者以及皮肤的咖啡色色素沉着的患者应考虑到该病,早发现有助于治疗。

McCune-Albright综合征合并低血磷性佝偻病4例并文献复习

目的：总结4例McCune-Albright综合征合并低血磷性佝偻病患者的临床资料，以提高临床医师对该病的认识。方法回顾性分析北京协和医院确诊的4例McCune-Albright综合征合并低血磷性佝偻病患者的临床表现、实验室检查、影像学特点、治疗及转归，并进行文献复习。结果临床特点：4例McCune-Albright综合征合并低血磷性佝偻病患者均为女性，10岁前起病，均为多骨型骨纤维异样增殖症，主要临床表现为骨痛、骨骼畸形和脆性骨折。其中2例合并甲状腺功能亢进，2例合并周围性性早熟。实验室检查：4例患者均显示低磷血症（0.53～1.03mmol/L）和高碱性磷酸酶水平（464～1930U/L），3例患者血β-1型胶原交联羧基末端肽（β-CTX）水平升高，2例患者血全长成纤维细胞生长因子23（intactFGF23）水平升高。影像学特点：4例患者影像学检查结果均符合骨纤维异常增殖症。其中3例患者有典型的佝偻病表现。4例患者均接受全身骨扫描显像，3例患者全身骨骼多发放射性浓聚区。治疗及转归：经给予活性维生素D、中性磷合剂和双膦酸盐，患者的临床症状和生化异常均显著改善。复习文献发现，患者起病越早，骨骼病变相对越重、血磷越低、骨转换指标升高越明显、血FGF23水平越高。结论McCune-Albright综合征合并低血磷性佝偻病是罕见病。对McCune-Albright综合征患者需注意筛查是否合并低血磷性佝偻病，以避免漏诊，改善预后。

McCune-Albright综合征患儿超说明书用药并文献复习

探讨甲羟孕酮、来曲唑和唑来膦酸超说明书用药的合理性。方法:1例6岁8个月男性患儿,出生时发现左臀部咖啡样色斑,4岁颅面部畸形,5岁时出现第二性征发育,同时出现骨龄超前,诊断为"Mc Cune-Albright综合征"。入院后,相继给予甲羟孕酮片(4 mg bid po)+来曲唑片(1.25 mg qd po)+唑来膦酸注射液(3 mg once iv gtt)+碳酸钙片(250 mg qd po)和维生素AD滴剂(胶囊型)(1粒qd po)治疗。结果:经过23 d的对症治疗后,患者一般情况及症状稳定,要求出院。结论:临床药师参与患者的药物治疗过程,对唑来膦酸和甲羟孕酮、来曲唑的超说明书用药有了进一步的认识,提高了药物的治疗水平。临床药师通过参与临床实践,协助医师参与患者的用药监护,提高药物治疗的安全性。

McCune-Albright综合征伴牙源性角化囊肿及成釉细胞瘤1例报道

McCune-Albright综合征（McCune-Albright Syndrome）是一种罕见的鸟嘌呤核苷酸结合蛋白（G蛋白）病,临床以多发性骨纤维异常增殖症、皮肤斑片状色素沉着及性早熟为最常见症状。口腔颌面部常可表现为硬组织的病变和面部畸形。有些患者唇颊黏膜有色素沉着，牙齿提前萌出等症状。我院收治1例，报告如下。

McCune-Albright综合征2例报道并文献复习

目的:探讨McCune-Albright综合征患儿的临床特点及基因突变,并复习相关文献。方法:分析本院收治的2例McCune-Albright综合征患儿的临床资料,并收集其新鲜组织、外周血进行基因检测。结果:患儿主要表现为外周性性早熟(乳房发育、月经初潮、卵巢囊肿)、皮肤牛奶咖啡斑(皮肤不对称性咖啡色色素沉着,边缘不规则)、骨纤维结构不良(桡骨和/或胫腓骨远端骨质改变),基因分子遗传学分析结果显示均存在GNAS基因突变[c.602G>A杂合突变(p.R201H)、c.46C>T(p.R16C)]。结论:McCune-Albright综合征临床罕见,容易漏诊及误诊,基因检测分析有助于McCune-Albright综合征患儿的临床诊断。

成年McCune-Albright综合征并发高性激素、低磷血症一例

报告1例McCune-Albright综合征(MAS)患者的临床资料,并文献复习国内外MAS合并低磷血症及性激素水平变化。MAS合并低磷血症者骨骼病变更重,部分MAS青年女性患者卵巢囊肿和雌激素过多的卵巢功能亢进持续存在,导致雌激素及雄激素水平升高。成年McCune-Albright综合征患者合并高性激素血症国内尚未见报道,合并低磷血症少见,提醒医务人员对于MAS患者成年后仍需密切关注性激素及血磷水平。

McCune-Albright综合征(附本病伴甲状旁腺增生一例)

McCune-Albright综合征是骨纤维异常增殖症的一种类型,是一种少见的G蛋白病。其典型的临床特点是：多发性骨纤维发育不良;皮肤色素沉着;一个或多个内分泌腺增生或腺瘤引起的自主性功能亢进。笔者从发病机理、临床表现、辅助诊断、治疗讲述该病,并附病例一例,加强对该病的认识。

McCune-Albright综合征SPECT/CT骨显像1例

1临床资料患者女,42岁,多处皮肤片状色素沉着42年,左下肢疼痛1月余入院。患者于出生时无明显诱因出现颜面部、胸前区、右上肢等多处皮肤色素沉着,未予重视及治疗,2016年因下颌骨疼痛于外院诊断下颌骨骨纤维结构增生异常综合征,予保守治疗。近1月来无诱因出现左下肢肿胀疼痛,休息后缓解,在当地医院给予消炎止痛处理,效果不佳,2019-12-06外院胫腓骨正侧位平片考虑慢性骨髓炎改变,为进一步确诊,特来我院就医。患者一般情况良好。既往2015年乳腺囊肿切除术,无家族史,月经规则。入院后查体:营养良好,颜面部、胸前区、右上肢等多处皮肤可见咖啡牛奶斑(图1),心肺查体无异常,左下肢局部皮肤肿胀,有压痛,四肢活动正常。

McCune-Albright综合征合并外耳道胆脂瘤1例

McCune-Albright综合征(McCune-Albright syndrome,MAS)是骨纤维异常增殖症的一种,是指多骨型骨纤维异常增殖症合并皮肤咖啡样色素沉着和内分泌腺功能亢进(如性早熟、甲状腺功能亢进、Cushing综合征、生长激素异常分泌等)。本病呈散发性,比较罕见,发病率大概为1/1000,000-1/10000[1]。我科收治1例患者报告如下。

McCune-Albright综合征诊治现状

McCune-Albright综合征(MAS)是一种罕见病,可导致全身多个系统出现病变,如多发性骨纤维结构不良、内分泌异常等。迄今为止,发表的相关文献大多为病例报道。MAS的发病机制尚不十分明确,随着临床检测技术的不断发展,其主要病因是基因突变,确诊依据为基因诊断。该病目前亦无有效根治方法,主要治疗方案为对症治疗,治疗效果也有待进一步研究。

McCune-Albright综合征伴甲状腺功能亢进1例报告及文献复习

Mc Cune-Albright综合征(MAS)是一种临床罕见的疾病,其典型三联征包括多骨性骨纤维异常增殖症、牛奶咖啡色斑及性早熟。本文报告1例伴有甲状腺功能亢进的Mc Cune-Albright综合征患者,并通过相关文献复习,阐述MAS的病因、临床表现、诊断及治疗等。

Long term treatment of recurring pathological fractures due to Mccune Albright Syndrome: Case report and literature review

McCune Albright syndrome is a rare genetic disorder which is characterized by café au lait skin pigmentation, precocious puberty and polyostotic fibrous dysplasia. Treating recurring pathological fractures due to Albright syndrome is a very challenging endeavor, and more so when it is accompanied by poor bone quality and deformity. We hereby present the case of a 23-year-old male patient who is treated several times for recurrent pathological fractures of the femur at our center. We analyze the difficulties associated with treating a patient with poor bone quality over several years, discuss our treatment options, review the literature for similar cases and look at what we could have done differently. We weigh in on the difficulties in treating a severely deformed shepherd’s crook, the ways of achieving proper internal fixation and the dangers of using plating instead of an IM nail as suggested in the literature. Our main goal in reporting this case is to bring forth the unusual challenges encountered when treating patients with Albright syndrome and discussing the options of the orthopedic surgeons when treating these types of patients.

Neonatal cholestasis can be the first symptom of McCune–Albright syndrome:A case report

BACKGROUND McCune–Albright syndrome(MAS)is caused by postzygotic somatic mutations of the GNAS gene.It is characterized by the clinical triad of fibrous dysplasia,caféau-lait skin spots,and endocrinological dysfunction.Myriad complications in MAS,including hepatobiliary manifestations,are also reported.CASE SUMMARY This is a case of a 4-year-old boy who presented with MAS with neonatal cholestasis.He was suspected to have Alagille syndrome due to neonatal cholestasis with intrahepatic bile duct paucity in liver biopsy,peripheral pulmonary artery stenosis,and renal tubular dysfunction.By the age of 2 years,his cholestatic liver injury gradually improved,but he had repeated left femoral fractures.He did not exhibit endocrinological abnormality or café-au-lait skin spots.However,MAS was suspected due to fibrous dysplasia at the age of 4 years.No mutation was identified in the GNAS gene in the DNA isolated from the peripheral blood,but an activating point mutation(c.601C>T,p.Arg201Cys)was observed in the DNA extracted from the affected bone tissue and that extracted from the formalin-fixed paraffin-embedded liver tissue,which was obtained at the age of 1 mo.CONCLUSION MAS should be considered as a differential diagnosis for transient cholestasis in infancy.

Anesthetic Consideration of a Patient with McCune-Albright Syndrome: A Case Report

The McCune-Albright syndrome is rare disease diagnosed by the clinical triad, fibrous dysplasia, café-au lait skin pigmentations and endocrine hyperfunction. Those patients with bone issues could have various surgeries under general anesthesia. Airway abnormality and various endocrine abnormalities should be considered during general anesthesia for McCune-Albright syndrome patients. A 15-year-old male with McCune-Albright syndrome was admitted with complaint of right nasal obstruction originated from fibrous dysplasia. Endoscopic resection of nasal cavity lesion was scheduled under navigation system guidance. Difficult airway could be anticipated due to protrusion of maxilla and right nostril. Awake fiberoptic intubation was performed by spray-as-you-go technique. When an anesthesiologist expects to take care of the patient with the McCune-Albright syndrome, the most appropriate anesthetic induction and tracheal intubation technique should be selected, and multiple backup instruments such as supraglottic device, video laryngoscope and fiberoptic bronchoscopy should be prepared.

McCune-Albright综合征的致病机制及诊治研究进展

McCune-Albright综合征是一种由于合子后GNAS基因突变导致的罕见嵌合体性疾病,属于鸟核苷酸结合蛋白病,影响范围广泛,以骨纤维发育不良、咖啡牛奶斑及性早熟为特征,并伴有其他可变的临床表现。目前针对McCune-Albright综合征,分子诊断存在困难,临床上缺乏有效的治疗方法来阻止或逆转病程及转归。本文分析归纳了McCune-Albright综合征的临床表现、诊断、致病分子机制、治疗现状以及相关的生育指导,以期为McCune-Albright综合征的进一步研究和治疗提供借鉴。

McCune-Albright综合征患儿生活质量及其影响因素分析

目的调查McCune-Albright综合征(MAS)患儿的生活质量及影响因素, 为提高患儿生活质量提供科学依据。方法回顾性分析2015年6月至2021年12月在河南省儿童医院诊断及随访的31例MAS儿童(MAS组)的临床资料, 同时按照1∶1匹配同年龄、同性别健康儿童37例(健康对照组), 应用儿童生活质量普适性核心量表(PedsQL?4.0)进行调查及对比分析, 统计学方法采用独立样本t检验、χ^(2)检验及多元回归分析。结果与健康对照组比较, MAS组患儿生理功能(t=2.092, P<0.05)、情感功能(t=2.373, P<0.05)、总分(t=2.360, P<0.05)均明显降低, 差异均有统计学意义。多元回归分析显示, 生理功能与每年阴道出血次数(t=-2.367, P<0.05)、首次骨折年龄呈负相关(t=-2.606, P<0.05)。社交功能与骨折次数呈负相关(t=-2.481, P<0.05)。结论 MAS儿童总体生活质量低, 以生理功能、情感功能较明显, 每年阴道出血次数、首次骨折年龄、骨折次数可能是患儿生活质量降低的影响因素。

McCune-Albright综合征患者3例的致病变异鉴定

目的对3例McCune-Albright综合征(MAS)患者进行候选基因GNAS的变异鉴定,以明确其遗传学病因。方法选取2019年4月于山东省立医院就诊和2020年8月、2021年5月于北京协和医院就诊的共3例患者为研究对象。采用酚-氯仿法提取患者及其家系成员的外周血样基因组DNA,通过全外显子组测序(WES)对候选致病变异进行筛查,通过Sanger测序对候选变异进行家系验证。结果测序显示家系1患者存在GNAS基因第8外显子的c.601C>T(p.Arg201Cys)杂合错义变异;家系2和家系3患者均存在GNAS基因第8外显子的c.602G>A(p.Arg201His)杂合错义变异。两种变异均为已知致病变异,患者均为相应致病变异的嵌合体,但比例有所不同。结论WES是鉴定MAS等体细胞遗传病的有效方法。本研究联合应用WES和Sanger测序鉴定了MAS患者致病变异及其嵌合程度,并证实其与患者的表型无明显相关性,为遗传咨询和产前诊断提供了依据。

41例McCune-Albright综合征女童临床及基因分析

目的探讨McCune-Albright综合征（MAS）的临床特点及分子病理机制，以期为MAS精准医疗提供指导。方法回顾性分析41例MAS女童的临床资料及基因检测结果。结果（1）MAS女童具有提前出现的性征发育及高雌二醇、低LH和FSH、子宫、卵巢容积明显增大的外周性性早熟表型。（2）41例MAS女童中17例存在GNAS1基因突变，总阳性率41.5%，其中三联症组为66.7%，二联症组为56.3%，一联症组为12.5%。在具有骨纤维结构不良患儿中可见78.6%存在突变阳性，而伴皮肤咖啡牛奶斑仅见55.0%阳性。儿童性早熟伴骨纤维结构不良是临床诊断MAS的重要依据，而皮肤牛奶咖啡斑似乎并不是MAS特异性的重要表现。结论MAS女童临床以不典型者居多，性早熟伴骨纤维结构不良是临床诊断MAS的重要权重因素。GNAS1基因筛查可有助于MAS临床精准诊断。

McCune-Albright综合征多病变部位基因诊断

目的研究1例McCune-Albright综合征(MAS)患者不同病变组织的G蛋白α亚单位(Gsα)基因突变情况。方法收集1例MAS患者的外周血、病变骨组织、皮肤及胸膜组织样本,分别提取基因组DNA并对目的片段进行PCR扩增和直接测序。结果该患者外周血和骨组织中存在Gsα基因R201C突变,而其皮肤和胸膜组织中未检出突变。结论经基因诊断证实该例临床确诊的MAS患者的Gsα基因存在经典的R201C突变,且累及多种组织。突变发生在胚胎形成早期,临床表现可呈现多样性。