Tumor-induced osteomalacia with elevated fibroblast growth factor 23: a case of phosphaturic mesenchymal tumor mixed with connective tissue variants and review of the literature

Tumor-induced osteomalacia (TIO), or oncogenic osteomalacia (OOM), is a rare acquired paraneoplastic disease characterized by renal phosphate wasting and hypophosphatemia. Recent evidence shows that tumor-overexpressed fibroblast growth factor 23 (FGF23) is responsible for the hypophosphatemia and osteomalacia. The tumors associated with TIO are usually phosphaturic mesenchymal tumor mixed connective tissue variants (PMTMCT). Surgical removal of the responsible tumors is clinically essential for the treatment of TIO. However, identifying the responsible tumors is often difficult. Here, we report a case of a TIO patient with elevated serum FGF23 levels suffering from bone pain and hypophosphatemia for more than three years. A tumor was finally located in first metacarpal bone by octreotide scintigraphy and she was cured by surgery. After complete excision of the tumor, serum FGF23 levels rapidly decreased, dropping to 54.7% of the preoperative level one hour after surgery and eventually to a little below normal. The patient's serum phosphate level rapidly improved and returned to normal level in four days. Accordingly, her clinical symptoms were greatly improved within one month after surgery. There was no sign of tumor recurrence during an 18-month period of follow-up. According to pathology, the tumor was originally diagnosed as "glomangioma" based upon a biopsy sample, "proliferative giant cell tumor of tendon sheath" based upon sections of tumor, and finally diagnosed as PMTMCT by consultation one year after surgery. In conclusion, although an extremely rare disease, clinicians and pathologists should be aware of the existence of TIO and PMTMCT, respectively.

Oncogenic osteomalacia caused by a phosphaturic mesenchymal tumor of the femur: A case report

BACKGROUND Oncogenic osteomalacia caused by phosphaturic mesenchymal tumors is very difficult to detect.We report a case of tumor-induced osteomalacia caused by a phosphaturic mesenchymal tumor of the left femur in a middle-aged woman after medical imaging and biopsy.CASE SUMMARY A 57-year-old woman presented with progressive bone pain for five years.She was diagnosed with hypophosphatemic osteomalacia,as her laboratory data showed low serum phosphorus and low serum calcium.Her knee joint radiography revealed an osteolytic lesion of the left femur.A computed tomography scan showed mixed density shadows in the left femur.Magnetic resonance imaging of the left femur showed the presence of an oval area with a hypointense signal in T1-weighted magnetic resonance imaging(MRI)and highlow mixed signal in T2-weighted MRI.Biopsy samples revealed the presence of short spindle cells,vascularization,and characteristics of phosphaturic mesenchymal tumors.Tumor resection was performed,and the clinical presentations and laboratory abnormalities were reversed.CONCLUSION Diagnosis of oncogenic osteomalacia is difficult due to the varieties and localization of source tumors and absence of pathognomonic biomedical signs.Our case highlights the importance of a combination of medical imaging and biopsy in the diagnosis of oncogenic osteomalacia caused by a phosphaturic mesenchymal tumor.

Oncogenic Osteomalacia Associated with Phosphaturic Mesenchymal Tumor of the Knee: Case Presentation and Review of the Literature

Oncogenic osteomalacia (OOM) is an uncommon metabolic and bone disease caused by fibroblast growth factor 23 (FGF23), a phosphaturic factor produced by phosphaturic mesenchymal tumors (mixed connective tissue variant, PMTMCTV) characterized by phosphate leakage from kidneys and subsequent hypophosphatemia. In this paper, we present the case of a patient, 42-year-old woman affected by left side limp and pain involving lumbar spine, pelvis and hip joints, referred to the Rheumatology Department of our Hospital for the treatment of a suspected sero-negative spondilo-arthritis. During hospitalization patient began an immuno-suppressive therapy with TNF-alpha inhibitors associated with Pamidornate, Indometacin, Esomeprazole and vitamin D3. Nevertheless pain did not decrease and a new examination found a worst hypophosphatemia (1 mg/dl) with normal Ca and PTH’s plasma values. During the same check-up a painful bulge on the anterior part of the right knee was observed and the Magnetic Resonance Imaging scan revealed an ovular solid lesion in the soft tissue closed to the upper part of the patella. Histological analysis identified the lesion as a PMTMCTV. After surgical removal patient got complete recovery. We will discuss about diagnostic evaluation, differential diagnosis and treatment.

Adult-onset hypophosphatemic osteomalacia as a cause of widespread musculoskeletal pain:A retrospective case series of single center experience

BACKGROUND Osteomalacia(OM)is frequently confused with various musculoskeletal or other rheumatic diseases,especially in patients with adult-onset widespread musculoskeletal pain because of its low prevalence and non-specific manifestations.AIM To facilitate the early diagnosis and etiology-specific treatment of adult-onset hypophosphatemic OM.METHODS A retrospective review of medical records was performed to screen adult patients who visited a physiatry locomotive medicine clinic(spine and musculoskeletal pain clinic)primarily presenting with widespread musculoskeletal pain at a single tertiary hospital between January 2011 and December 2019.We enrolled patients with hypophosphatemia,high serum bone-specific alkaline phosphatase levels,and at least one imaging finding suggestive of OM.RESULTS Eight patients with adult-onset hypophosphatemic OM were included.The back was the most common site of pain.Proximal dominant symmetric muscle weakness was observed in more than half of the patients.Bone scintigraphy was the most useful imaging modality for diagnosing OM because radiotracer uptake in OM showed characteristic patterns.Six patients were diagnosed with adefovir(ADV)-induced Fanconi syndrome,and the other two patients were diagnosed with tumor-induced OM and light-chain nephropathy,respectively.After phosphorus and vitamin D supplementation and treatment for the underlying etiologies,improvements in pain,muscle strength,and gait were observed in all patients.CONCLUSION Mechanical pain characteristics,hypophosphatemia,and distinctive bone scintigraphy patterns are the initial diagnostic indicators of adult-onset hypophosphatemic OM.ADV-induced Fanconi syndrome is the most common etiology of hypophosphatemic OM in hepatitis B virus-endemic countries.

庄礼兴教授针药结合治疗磷酸盐尿性间叶性肿瘤术后疼痛

总结庄礼兴教授针药结合治疗磷酸盐尿性间叶性肿瘤术后疼痛经验。庄礼兴教授认为本病病机为脾肾阳虚、寒湿阻络,岭南火针治疗以温阳祛寒、调神止痛为主,取阿是穴、神门、内关、三阴交、足三里、申脉、照海、章门和京门频频浅刺,督脉、膀胱经循经散刺,配合中药内服以附子汤为主方温阳除湿。针药结合,标本兼顾,疗效显著。

磷酸盐尿性间叶肿瘤误诊分析(附7例)

目的:分析磷酸盐尿性间叶肿瘤(PMT)误诊原因,明确影像学检查路径。方法:回顾性分析我院2017年7月至2022年3月经病理证实PMT患者临床、影像、病理资料。结合文献复习,总结误诊原因,提出影像学检查路径。结果:7例患者3例男性,4例女性,平均年龄为(50.29±15.66)岁(范围17~69岁)。患者表现为不同程度乏力、骨痛等,均伴随骨折,病程平均(5.00±3.25)年(范围1~12年)。患者术前血磷均减低,术后血磷均升高,6例患者血磷在术后7~15天恢复正常,1例失访。6例患者术前碱性磷酸酶升高,1例正常。肿瘤最大径(2.01±1.32)cm(范围0.8~2.5 cm),2例位于软组织,5例位于骨组织。6例行X线检查,显示全身或局部骨质不同程度骨软化和伴随骨折,3例病灶无法显示。6例CT检查中5例骨组织病灶显示为高密度,1例为软组织密度结节。6例MRI平扫T1WI为低、等信号为主,偶尔见高信号,T2WI混杂高信号,内部或边缘可见低信号区。4例MRI增强检查显示病灶中度至明显强化,强化不均匀。结论:PMT影像表现缺乏特异性,容易被误诊。骨质软化、骨痛、骨折以及低血磷、高碱性磷酸酶患者,需考虑此病。可先行OCT检查发现可疑病灶,再行解剖学检查(X线、CT,MRI)对可疑致病肿瘤进一步诊断和术前定位、评估切缘和治疗随访。

多灶性肿瘤性骨软化症一例报告

肿瘤性骨软化症是一种副肿瘤综合征,以低血磷、高尿磷、血钙及甲状旁腺素正常、1,25-二羟维生素D 3[1,25-dihydroxyvitamin D 3,1,25(OH)2D 3]正常或偏低、成纤维细胞生长因子23(fibroblast growth factor 23,FGF-23)升高为主要特征,经过手术治疗可获得根治。其多灶病例非常罕见。现报道多灶性肿瘤骨软化1例并文献复习,探讨该特殊情况下的处理策略。

软组织磷酸盐尿性间叶肿瘤的临床病理分析

目的研究磷酸盐尿性间叶肿瘤(混合结缔组织亚型)的临床与病理学特点。方法对1例骨软化症患者的肿块切除标本进行光镜、电镜和免疫组化SP法检测。结合临床资料,并复习相关文献。结果患者表现为顽固性骨软化症、低磷酸盐血症,高磷酸盐尿,高血清碱性磷酸酶,外周血单核细胞增多,血钙浓度正常。经99mTc-OCT(奥曲肽)检查指导临床发现左腘窝区小肿块并切除之。术后3天,血磷恢复正常。光镜下肿瘤主要由肥胖的梭形细胞和破骨细胞样多核巨细胞构成,具有丰富的血管,可见血管外皮瘤样血管、散在脂肪岛、明显的出血及含铁血黄素沉积,肿瘤边缘有不完整的膜状骨样或软骨样组织。电镜下见梭形细胞内含数量不等的细颗粒状电子致密物,其中部分为结晶样高电子致密度颗粒。免疫组化显示多核细胞和单核间质细胞CD68阳性。结论该例为肿瘤源性骨软化症,其病理类型为磷酸盐尿性间叶肿瘤,混合结缔组织亚型。外科切除后治愈,99mTc-OCT对于指导临床发现小的隐蔽病灶很有价值。

肿瘤源性骨软化症的临床特征

目的分析肿瘤源性骨软化症(tumor-induced osteomalacia,TIO)患者的临床特点、诊断、病理及手术后情况,以提高临床对TIO的认识.方法收集并整理2008年1月至12月于解放军总医院就诊的14例肿瘤源性骨软化症患者的病史、一般情况、临床表现、辅助检查、病理及术后情况.结果患者平均病程为(3.0±3.8)年,临床症状以骨痛(14/14,100%)和乏力(6/14,42.9%)最常见,部分患者有病理性骨折,在确诊前均有误诊病史.生化特点以低血磷(0.43±0.12)mmol/L、高尿磷(13.71±5.32)mmol/L 24 h、血碱性磷酸酶升高(309.30±146.41)U/L和正常血钙(2.19±0.13 mmol/L)为主.定位诊断中,99Tcm-奥曲肽SPECT/CT扫描和68 Ga-DOTA-TATE PET/CT阳性率均较高(100%),并经相应部位的CT、MRI或超声检查证实.肿瘤分布在全身不同部位的软组织(4/14,28.6%)或骨组织(10/14,71.4%)中.手术切除肿瘤后,血磷平均恢复时间为(6.4±2.3)d.1例因病灶难以完全切除,术后未缓解.2例患者术后出现复发.结论TIO起病隐匿,症状不具有特异性,容易被误诊.99 Tcm-奥曲肽SPECT/CT扫描或68 Ga-DOTATATE PET/CT检查对定位诊断效率较高.手术治疗可以治愈TIO,但远期仍可能复发,需要定期随访.

颅内磷酸盐尿性间叶肿瘤

目的报告1例颅内磷酸盐尿性间叶肿瘤病例,并总结磷酸盐尿性间叶肿瘤病理学、影像学以及诊断与治疗特点。方法与结果男性患者,53岁。以全身多发性骨痛7年、加重1个月入院。临床表现为血清磷明显降低;99Tcm-奥曲肽显像以左侧枕部生长抑素受体高表达灶为特征性改变;MRI显示左侧枕骨和硬脑膜病变。拟诊肿瘤诱发骨软化症,手术全切除病变。术后组织学形态观察,肿瘤呈弥漫浸润生长,累及硬脑膜和颅骨骨质,肿瘤细胞呈卵圆形和短梭形,可见畸形厚壁血管、扩张的窦样血管、成熟脂肪组织和间质黏液变性,核分裂象罕见,未见坏死。免疫组织化学染色,肿瘤细胞胞质高表达纤维母细胞生长因子-23、波形蛋白、生长抑素受体2、CD56和神经元特异性烯醇化酶,灶性表达Bcl-2和D2-40,Ki-67抗原标记指数为5%。病理诊断:磷酸盐尿性间叶肿瘤。术后血清磷恢复正常,随访22个月肿瘤无复发、无转移。结论颅内磷酸盐尿性间叶肿瘤极其罕见,病变隐匿而不易早期发现,常被误诊为脑膜瘤和血管外皮瘤,准确定位并全切除肿瘤是有效治疗方法。综合临床表现、血液生化、影像学和病理学特点有助于准确诊断并与脑膜瘤等梭形细胞肿瘤相鉴别。

肿瘤性骨软化症特征及诊治

目的通过对肿瘤性骨软化症(tumor-induced osteomalacia,TIO)患者临床特点、诊断过程及术后疗效随访的分析,提高对TIO的认识及临床诊治水平。方法回顾性分析15例TIO确诊患者的临床特点及手术前后临床及生化指标变化。结果 15例年龄(42.8±10.7)岁,病程为(3.5±2.8)年;其中2例复发(13.3%),1例复发后恶变(6.7%)。血磷(0.41±0.10)mmol/L、肾磷酸根阈值(RTPC)(0.33±0.10)mmol/L,均低于正常值。15例共住院手术19人次,肿瘤位于骨组织10人次,软组织9人次,13例手术一次性治愈(86.7%)。19次术后病理结果均为磷酸盐尿性间叶细胞瘤混合结缔组织型(PMTMCT)。分析显示:肿瘤位于软组织患者较肿瘤位于骨组织患者血磷及RTPC均更低(t=2.264,P=0.041);血磷主要受RTPC影响(标准系数0.836,t=3.862,P=0.005);RTPC受肿瘤体积、肿瘤组织来源相关影响(标准系数0.405、0.546,t=-2.635、3.925,P=0.030、0.004)。结论对于TIO的患者应警惕恶性及复发的可能;RTPC能较24 h尿磷更好地反映肾小管重吸收磷的受损情况;肿瘤位于软组织患者较肿瘤位于骨组织病情更为严重。

磷酸盐尿性间叶肿瘤12例临床病理分析

目的探讨磷酸盐尿性间叶肿瘤的临床病理学特征。方法回顾性分析12例磷酸盐尿性间叶肿瘤的临床资料、组织学及免疫表型，并复习相关文献。结果12例中男性8例，女性4例，年龄23-63岁，平均40．5岁；病程1-14年，平均5．6年；患者均有不同程度的骨痛、关节痛和活动受限伴低血磷、高尿磷；肿瘤最大径1-7．5cm，平均2．7cm；肿瘤主要由梭形细胞构成，部分病例伴有破骨样多核巨细胞，血管丰富，可见簇状厚壁畸形血管、薄壁血管、散在脂肪岛及软骨样细胞；7例伴有不规则钙盐沉积，2例伴条索状上皮，其中CK（AE1／AE3）阳性；10例核分裂象少见，2例核分裂象多见，其中1例肿瘤细胞异性明显；瘤细胞均表达vimentin、、CD56（其中2例分别为弱阳性和灶阳性），11例NSE阳性，8例CD99阳性，7例BCL-2阳性，4例CD34和6例SMA呈不同程度阳性，10例Ki-67增殖指数≤5％，2例分别为10％、25％。随访时间2—108个月，其中2例分别于术后72、84个月复发，其余病例均未见复发。结论磷酸盐尿性间叶肿瘤多表现为良性或低度恶性，其组织学形态多变且缺乏特异性，掌握其共性特征并紧密结合临床才能正确诊断。

磷酸盐尿性间叶瘤临床病理观察

目的通过对磷酸盐尿性间叶瘤(PMT)的临床与病理观察及复习文献,探讨其病变机制与病理特点。方法对1例骨病患者的右大腿肿块切除标本进行光镜、电镜观察和免疫组化检测,结合临床资料,并复习相关文献。结果患者表现为持续性全身多处骨痛、低磷酸血症、高磷酸盐尿和高血清碱性磷酸酶,血钙正常。临床行右大腿肿块切除,术后5天,血磷恢复正常。大体见灰黄、灰红色肿物,大小3 cm×2.5 cm×2 cm,质中,与周围界限不清。瘤组织主要由片状分布的圆形细胞和短梭形细胞构成,胞质丰富红染,境界不清,局部可见黏液变。间质见血管外皮瘤样细小血管、厚壁静脉血管,散在脂肪岛,局部灶性出血及多核巨细胞浸润,肿瘤边缘近乎完整的薄层纤维包膜。免疫组化显示肿瘤细胞vimentin、CD68、HMB-45、CD63和FGF23强(+)。电镜见瘤细胞胞质内含数量不等的高电子密度的致密物质,部分颗粒与初级溶酶体关系密切。结论 PMT有特征性的临床表现,但缺乏特异的形态学改变,一般应结合临床检查作出最后诊断。本例形态学主要呈血管平滑肌脂肪瘤样病理改变,HMB-45(+),是该瘤一个新的病理学特点,结合瘤细胞对FGF23高表达及电镜见斑片状致密物,对诊断有重要意义。

9例肿瘤源性骨软化症诊治分析

目的：分析肿瘤源性骨软化症（tumor-induced osteomalacia，TIO）的临床特点、诊断和治疗方法，以提高对本病的认识。方法收集并整理9例TIO患者的临床表现、实验室检查、影像学特点及治疗方法等资料，分析和比较患者手术前后的血生化指标的改变。结果患者均有骨痛、无力及活动受限的表现，实验室检查提示低磷血症，骨扫描提示骨质疏松、骨软化症。9例患者均进行奥曲肽显像（99mTc-OCT），其中8例诊断部位准确，另1例显像定位不准确，后经68Ga-TATE及其他影像学检查确诊病灶部位。8例患者病理诊断为磷酸盐尿性间叶组织肿瘤，1例为胸膜外脂肪瘤样型孤立性纤维性肿瘤。7例患者在明确肿瘤定位后立即接受手术切除治疗，术后血磷恢复正常，并在术后6～12个月保持在正常水平。结论 TIO多见于成人起病、无家族史的低磷骨软化症患者。99mTc-OCT对诊断本病有重要意义，B超、CT、MRI及骨扫描等对辅助定位和诊断病灶有帮助，必要时可进行68Ga-TATE检查。确定肿瘤病灶之后及时进行手术切除，是目前最有效的治疗方法。

腹股沟区肿瘤性骨软化症12例临床特征及手术治疗效果

背景:腹股沟区肿瘤性骨软化症(TIO)的致病瘤体位置隐匿,定位及定性诊断困难,且临床医师常缺乏对该病的认识,故临床上极易造成漏诊和误诊。目的:探讨腹股沟区TIO的临床特征,以提高临床医师对该病的认识及手术治疗水平。方法:回顾性分析2015年1月至2019年1月行手术治疗的12例腹股沟区TIO患者的临床资料,研究其临床特点及手术治疗效果,总结临床实践经验。结果:术后病理学证实12例均符合TIO的临床诊断标准,12例均出现不同程度的骨痛、乏力及活动受限,4例病程中身高明显短缩。12例均出现低磷血症,11例出现血清碱性磷酸酶水平升高,12例出现24 h尿磷水平相对升高,12例患者的血钙水平基本正常或轻度降低,3例出现甲状旁腺激素水平升高。12例患者均接受腹股沟区手术治疗,病理诊断均证实为磷酸盐尿性间叶组织肿瘤。12例患者经手术治疗后,骨痛及乏力症状均有所改善。12例患者术后血磷水平逐渐升高,随访2个月至4年,血磷水平均处于正常范围。结论:腹股沟区TIO的致病瘤体位置隐匿,临床上极易造成漏诊和误诊,应增强临床医师对该病的认识,术中需注意避免神经、血管等副损伤发生,提高外科医师对该类病例的临床诊治水平。

头颈部普通型磷酸盐尿性间叶肿瘤与混合性上皮-结缔组织亚型的病理学对比研究

目的观察普通型磷酸盐尿性间叶肿瘤(PMT)与混合性上皮-结缔组织亚型(PMTMECT)的组织学形态,比较PMTMECT与普通型PMT临床病理特征和免疫表型的差异。方法选取25例PMTMECT,同时选取同部位(头颈部)普通型PMT 50例做为对照,分析组织学形态并比较免疫表型差异。结果 PMTMECT多见于男性,男∶女为2.57∶1;普通型PMT多见于女性,男∶女为0.56∶1。PMTMECT中位年龄34岁,普通型PMT中位年龄42.5岁;PMTMECT发病部位为上颌骨(11/25)和下颌骨(14/25),普通型PMT发病部位以鼻腔为主(29/50)。组织学上,PMTMECT由上皮和间叶成分混合构成;普通型PMT由间叶成分构成。免疫组化结果显示,PMTMECT中AE1/AE3呈强(+),FGF23、SSTR2A、FGFR1、NSE、 vimentin、CD99、CD56、bcl-2、D2-40、CD68、SMA和CD34的表达与普通型PMT一致。PMTMECT中Ki-67≤5%者占80%(20/25);普通型PMT中Ki-67≤5%者占85.4%(35/41)。结论 PMTMECT常见于年轻男性,病变均定位于牙槽骨,肿瘤由上皮和间叶成分混合构成,可表达多种免疫组化标记物,提示具有多向分化潜能,与普通型PMT相比具有AE1/AE3特异阳性,为一罕见的PMT亚型。

^(68)Ga-DOTA-TATE正电子发射断层显像/计算机断层显像对^(99m)Tc-HYNIC-TOC单光子发射断层显像阴性瘤源性骨软化症致病肿瘤的定位价值

目的分析^(99m)Tc-HYNIC-TOC单光子发射计算机断层显像(SPECT)结果阴性的瘤源性骨软化症(TIO)致病肿瘤的^(68)Ga-DOTA-TATE正电子发射断层显像/计算机断层显像(PET/CT)的图像特征,探讨其对致病肿瘤准确定位的指导价值。方法纳入37例经临床及病理确诊的^(99m)Tc-HYNIC-TOC SPECT显像结果阴性的TIO患者,回顾性分析致病肿瘤的^(68)Ga-DOTA-TATE PET/CT图像特点。结果 37例TIO患者致病肿瘤均为单发,术后病理包括35例磷酸盐尿性间叶组织肿瘤和2例梭形细胞瘤。所有TIO致病肿瘤^(68)Ga-DOTA-TATE PET/CT上均表现为放射性浓聚灶,标准化摄取最大值和标准化摄取平均值分别为7. 2±4. 3和4. 3±2. 4,平均最大径为(1. 9±0. 7) cm。37例TIO致病肿瘤,最常见发病部位为下肢(19/37),其次为躯干(11/37)、上/下颌骨(5/37)及上肢(2/37)。24例位于骨组织病灶,最常位于下肢长骨(13/24),多呈偏心性生长(8/13),3例累及骨皮质,同机CT以局限性溶骨性骨质破坏多见(14/24),部分呈骨质硬化型改变(9/24),较少累及周围软组织。13例位于软组织病灶,多呈边界清楚等或低密度结节(10/13),1例位于胸膜病灶伴钙化。结论 ^(68)Ga-DOTA-TATE PET/CT能够检出^(99m)Tc-HYNIC-TOC SPECT漏诊的TIO病例。若生长抑素受体高度表达病灶局部见溶骨性或硬化型骨质改变、软组织内等或低密度结节,更倾向于TIO的诊断。

3例不同部位磷酸盐尿性间叶性肿瘤临床病理特征分析

目的:分析磷酸盐尿性间叶性肿瘤(PMT)的临床特点及病理学特征。方法:回顾性分析温州医科大学附属第一医院原发于不同部位的3例PMT的临床资料、组织病理学形态和免疫组化特点。结果:3例患者术前血磷均明显降低,术后血磷均恢复正常,其中1例伴成人软骨症。肿瘤细胞排列成束状或编织状,细胞呈梭形或卵圆形,无明显异型性及核分裂,血管丰富,间质内可见烟熏样基质,部分病例可见成熟脂肪组织、黏液样、骨样基质。瘤细胞一致表达Bcl-2、CD56、CD99、SATB2。结论:PMT非常罕见,需结合临床资料、组织病理学形态和免疫组化表达特点明确诊断。

中枢神经系统原发性磷酸盐尿性间叶性肿瘤

目的探讨中枢神经系统原发性磷酸盐尿性间叶性肿瘤(PMT)的临床病理特点。方法报道北京协和医院诊断的中枢神经系统原发性PMT 2例,回顾临床病史并做免疫组化染色。结果 2例中枢神经系统PMT均为女性,年龄分别为68岁和56岁,部位于右侧嗅沟及胸11椎管内,均手术切除。镜下,肿瘤细胞呈梭形或星芒状,散在小灶成熟脂肪细胞,可见云雾状钙化及骨化,富于小血管,可见厚壁血管,间质黏液样变性,核分裂象罕见。免疫组化肿瘤细胞FGF23、vimentin、CD56和NSE均(+),CD99和Bcl-2灶状(+),EMA、GFAP和CD34(-),Ki-67增殖指数<5%。结论中枢神经系统原发性PMT非常罕见,具有临床及病理特点,影像及病理易被诊断为脑膜瘤。手术切除为主要治疗手段,手术切除不净可复发,放疗有效。

磷酸盐尿性间叶组织肿瘤临床与影像学特点及文献复习

目的:总结磷酸盐尿性间叶组织肿瘤(PMT)的临床与影像学特点并进行文献复习。方法:回顾分析2014年1月~2019年1月中日友好医院病理科诊断为PMT患者的临床、病理及影像学资料,进行相关文献的复习。结果:4例患者中男3例、女1例,平均年龄为47.2岁。患者均具有不同程度的乏力、骨痛、关节痛等临床表现,血磷减低,平均值为0.5mmol/L(正常值为0.81~1.78mmol/L)。病变部位:1例位于上肢,1例位于下肢,2例位于头颈部。影像学表现:CT表现为软组织密度结节或肿块,平均CT值为47Hu,病变较小时边界清楚,病变较大时可合并骨质破坏;MRI表现为T1WI等及低信号,T2WI脂肪抑制图像不均匀高信号,内部可见低信号区,增强扫描病变中度到明显强化,较大病变内部强化欠均匀。结论:PMT发病率低,其临床及影像学具有一定的特点,掌握这些特点有助于临床早期诊断和治疗。