下颌骨纤维骨性病变致种植失败一例及文献回顾

本文报道一例同期于患者双侧下颌后牙区各植入一颗种植体,6个月后右侧种植体骨结合失败、松动取出,左侧种植体骨结合良好,常规修复并负荷。术后回顾分析发现该病例右侧下颌后牙区骨内存在影像学表现不明显的纤维骨性病变,并最终通过组织病理学检查确诊。颌骨纤维骨性病变主要是指一类在组织形态学上表现为纤维和骨化的混合性病变,这类病变临床及影像学表现往往不明显,难以发现;或者与其他疾病表现相似,鉴别困难。本文通过对该病例失败原因进行分析,对颌骨纤维骨性病变临床、影像学及组织病理学的特征等进行相关文献回顾和讨论,以期为临床提供纤维骨性病变种植风险评估预警。

鼻窦及颌面部273例良性纤维骨性病变的回顾性分析

目的:骨瘤、骨化纤维瘤(OF)、骨纤维异常增生症(FD)三种鼻窦及颌面部良性纤维骨性病变(FOLS)的分析比较。方法:回顾分析2012-2017年间来我科就诊的共273例鼻窦及颌面部FOLS患者(骨瘤153例,OF 44例,FD 76例)的病例资料,并对患者进行6个月~5年的随访,分析比较三种病变在发病率、性别、年龄、病变部位、术前血清ALP的含量及复发率的差异。结果:骨瘤多发于鼻窦(72.5%),其中筛窦(50.3%)最常见,额窦(22.1%)次之,17.7%的骨瘤患者合并鼻窦炎,女性发病率约为男性患者的2倍,未见术后复发病例。OF多发于颌面骨(65.9%),以单骨型病变(75.0%)为主,其中发于鼻窦(34.1%)者以筛窦(27.3%)多见,27.3%的患者合并鼻窦炎;男女发病率未见明显差异;复发率为13.6%。FD多发于颌面骨(64.5%),多为单骨型病变(64.5%),其中以上颌骨(50.0%)最为常见;病变位于鼻窦者多为多骨型病变,其中以蝶窦(34.2%)最为多见,FD男女发病率未见明显差异;13.2%的患者合并鼻窦炎,术后复发率为14.5%,其中9例(75.0%)患者首次手术年龄小于20岁。骨瘤、OF、FD的平均发病年龄分别为(40.7±14.55)岁、(28.0±17.9)岁和(20.32±15.2)岁,差异有统计学意义(P<0.01);3种病变患者术前血清ALP含量分别为(68.3±24.1)U/L、(130.1±107.0)U/L和(127.7±78.7)U/L,差异有统计学意义(P<0.01)。OF单骨型与多骨型病变患者术前血清ALP分别为(117.2±92.6)U/L和(168.7±140.1)U/L,差异无统计学意义(P>0.01);FD单骨型与多骨型病变患者术前血清ALP分别为(122.2±82.9)U/L和(137.7±70.7)U/L,差异无统计学意义(P>0.01)。结论:骨瘤、OF、FD三种鼻窦及颌面部良性纤维骨性病变的发病年龄、病变部位、术前血清ALP含量及复发率存在差异。手术治疗是目前最有效的治疗方法。

颅面骨纤维异常增殖症25例CT和MRI影像学表现分析

目的对颅面骨纤维异常增殖症CT和MRI表现特征进行分析,提高诊断和鉴别诊断水平。方法对我院2007年3月～2010年12月收治的25例颅面骨纤维异常增殖症CT和MRI表现进行回顾性分析。结果本组单骨型5例,多骨型20例,其中15例跨越中线累及双侧颅面骨。CT表现为囊状膨胀样、磨玻璃样及硬化改变;MRI表现以膨胀样改变为主,自然孔道明显变形,组织成分不同MRI表现亦不同。结论 CT能够对病变进行定性诊断,MRI能够判断病变的病理学基础,两者对该病的早期诊断、治疗方法选择及术后评价具有重要意义。

Progress in non-invasive detection of liver fibrosis

Liver fibrosis is an important pathological precondition for hepatocellular carcinoma.The degree of hepatic fibrosis is positively correlated with liver cancer.Liver fibrosis is a series of pathological and physiological process related to liver cell necrosis and degeneration after chronic liver injury,which finally leads to extracellular matrix and collagen deposition.The early detection and precise staging of fibrosis and cirrhosis are very important for early diagnosis and timely initiation of appropriate therapeutic regimens.The risk of severe liver fibrosis finally progressing to liver carcinoma is＆gt;50%.It is known that biopsy is the gold standard for the diagnosis and staging of liver fibrosis.However,this method has some limitations,such as the potential for pain,sampling variability,and low patient acceptance.Furthermore,the necessity of obtaining a tissue diagnosis of liver fibrosis still remains controversial.An increasing number of reliable non-invasive approaches are now available that are widely applied in clinical practice,mostly in cases of viral hepatitis,resulting in a significantly decreased need for liver biopsy.In fact,the noninvasive detection and evaluation of liver cirrhosis now has good accuracy due to current serum markers,ultrasound imaging,and magnetic resonance imaging quantification techniques.A prominent advantage of the non-invasive detection and assessment of liver fibrosis is that liver fibrosis can be monitored repeatedly and easily in the same patient.Serum biomarkers have the advantages of high applicability（〉95%）and good reproducibility.However,their results can be influenced by different patient conditions because none of these markers are liver-specific.The most promising techniques appear to be transient elastography and magnetic resonance elastography because they provide reliable results for the detection of fibrosis in the advanced stages,and future developments promise to increase the reliability and accuracy of the staging of hepatic fibrosis.This article aims to describe the recent progress in the development of non-invasive assessment methods for the staging of liver fibrosis,with a special emphasize on computer-aided quantitative and deep learning methods.