Changes of Tumor Necrosis Factor-α and the Effects of Ulinastatin Injection during Cardiopulmonary Cerebral Resuscitation

Summary: The changes of tumor necrosis factor-α (TNF-α) and brain ultrastructure during cardiopulmonary resuscitation and the effects of ulinastation injection were observed, and the mechanism was investigated. Twenty-four adult healthy Sprague-Dawley rats were randomly divided into control group (8 rats), resuscitation group (8 rats) and ulinastatin (UTI) group (8 rats). Rats in control group underwent tracheotomy without clipping the trachea to induce circulatory and respiratory standstill. Rats in resuscitation and ulinastatin group were subjected to the procedure of establishing the model of cardiopulmonary cerebral resuscitation (CPCR). Rats in ulinastatin group were given with UTI 104 U/kg once after CPCR. In the control group, the plasma was collected immediate, 30 min, 2 h, 4 h, and 6 h after tracheotomy. In resuscitation group and UTI group, plasma was collected immediate after tracheotomy, 30 min, 2 h, 4 h and 6 h after successful resuscitation. The plasma levels of TNF-α were determined by radioimmunoassay (RIA). At the end of the experiment, 2 rats were randomly selected from each group and were decapitated. The cortex of the brain was taken out immediately to observe the ultrastructure changes. In control group, there were no significant differences in the level of TNF-α among different time points (P>0.05). In resuscitation group, the level of TNF-α was increased obviously after resuscitation (P<0.01) and reached its peak 2 h later after resuscitation. An increasing trend of TNF-α showed in UTI group. There were no differences in TNF-α among each sample taken after successful resuscitation and that after tracheotomy. The utrastructure of brains showed the injury in UTI group was ameliorated as compared with that in resuscitation group. In early period of CPCR, TNF-α was expressed rapidly and kept increasing. It indicated that TNF-α might take part in the tissue injury after CPCR. The administration of UTI during CACR could depress TNF-α and ameliorate brain injury. By regulating the expression of damaging mediator, UTI might provide a protective effect on the tissue injury after CPCR.

Desmoplastic small round cell tumor with atypical immunohistochemical profile and rhabdoid-like differentiation

Desmoplastic small round cell tumor(DSRCT) is a rare,aggressive malignant neoplasm of unknown origin, and is comprised of small round cells with a characteristic desmoplastic stroma. DSRCT typically expresses epithelial, mesenchymal and neural markers simultaneously. We describe a case of DSRCT with an atypical immunohistochemical profile and rhabdoid-like tumor cells on electron microscopy. In the present case, the neoplastic cells were positive only for vimentin, desmin(cytoplasmic membranous pattern) and CD56,and negative for smooth muscle actin, synaptophysin,CD117, CD45, myogenin, CAM5.2, pancytokeratin,WT1, EMA, CD99, neurofilament, CD34 and p53. Ki67 showed a low proliferative activity. Electron microscopy showed focal rhabdoid differentiation. However, INI-1(SNF-5/BAF47) demonstrated preservation of nuclear positivity in the neoplastic cells. Cytogenetic studies showed translocation t(11;22)(p13;q12) confirming an EWSR1-WT1 translocation characteristic for DSRCT, and t(1;15)(q11;p11.2) of unknown significance. This case is a diagnostic challenge because of atypical immunohistochemical profile and cytogenetic study is crucial in rendering the correct diagnosis.

ULTRASTRUCTURAL STUDY ON THE INVASION OF RETINAL INNER LIMITING MEMBRANE BY THE MALIGNANT TUMOR CELLS

To observe the process of invasion, retina of rat was used as a model to substitute the inner limiting membrane of retina for the basement membrane. Retina invaded by esophageal carcinoma cells and B16 melanoma cells upon the inner limiting membrane was studied by scanning and transmission electron microscopy. The results showed that the inner limiting membrane was destroyed by both kinds of tumor cells. The process of destruction was followed by a series of transformations in the inner limiting membrane, i.e. folding, swelling, thickening, and granular change. The inner limiting membrane was dissolved focally as a result of transformation, and then tumor cells invaded the retina through these dissolved regions. It seems that, as a barrier, the inner limiting membrane plays a similar role as the basement membrane.

骨骼肌钝挫伤大鼠模型的构建与评价

目的:建立可靠、稳定、符合临床实际的大鼠骨骼肌钝挫伤模型。方法:通过170g重物,70cm高度,用底部直径0.5cm弹簧缓冲聚合式打击部,以引导下落的撞击方法,连打5次,建立大鼠腓肠肌钝挫伤模型。分别于造模后0h、12h、24h、3d、7d、14d,采用Cat Walk分析系统评估大鼠步态改变;HE染色观察大鼠局部组织病理学改变,透射电子显微镜观察局部组织超微结构的改变。酶联免疫吸附试验(enzyme linked immunosorbent assay,ELISA)检测局部组织肿瘤坏死因子(tumor necrosis factor-α,TNF-α)含量变化。结果:(1)Cat Walk步态参数:与空白组相比,模型组的平均速度与最大速度变化率均明显下降,差异具有显著性意义(P<0.001);与健康侧肢体组相比:受伤侧肢体组肢体的最大接触面积、足印面积和站立相持续时间均明显减少,差异具有显著性意义(P<0.05)。(2)HE染色:观察到3d后大量炎症细胞浸润,肌纤维大量溶解坏死,14d尽管瘢痕组织仍然存在,但HE染色上的组织修复与空白组几乎没有区别。(3)超微结构:打击后0h部分肌浆网出现空泡现象,3d肌纤维和部分肌浆网溶解,炎症反应加重,到14d基本恢复正常。(4)TNF-α表达水平:0h开始至12h这段时间内,TNF-α含量即开始逐渐升高达到高峰,并在损伤后12—72h一直保持较高水平,与空白组相比差异具有显著性意义(P<0.05),到14d基本恢复正常水平。结论:以锤重170g、70cm高度、底部带弹簧缓冲装置的直径0.5cm圆钝型打击头,连打5次,可对大鼠骨骼肌造成中度损伤,其自然恢复时间至少14d,适用于大鼠骨骼肌钝挫伤模型的建立,可为今后大鼠骨骼肌钝挫伤模型提供参考依据。

Effect of Phosphorus-32 Glass Microspheres on the Human Hepatocellular Carcinoma in Nude Mice

Objective To study anticancer effect and ultrastructural influence of phosphorus 32 glass microspheres( 32 P GMS) injected in the hepatocellular carcinoma in nude mice. MethodsThe ultrastructural changes of tumor in both the treatment group and control group were examined by transmission electron microscope. ResultsIn the treatment group,a large number of tumor cells were killed and the death rate of tumor cells was much higher(35%-70%). Ultrastructurally, severe nuclear damage was observed in the dead cells. The early characteristics of necrosis such as margination of heterochromatin were also found in some tumor cells. Besides,well differentiated tumor cells, degenerative tumor cells and some lymphocytes were seen. The skin and muscle close to the tumor were normal. In the control group,the tumor consisted of poor differentiated tumor cells,in which there were only a few appototic cells(5%). ConclusionThe results suggest that the local administration of 32 P GMS produces obviously the anticancer effect.

原始神经外胚层肿瘤(PNET)1例光镜、免疫组化和电镜观察及文献复习

目的：研究原始性神经外胚层肿瘤（ＰＮＥＴ）的特征。方法：采用光镜、电镜和免疫组化对１例颈部原始性神经外胚层肿瘤（ＰＮＥＴ）进行观察。结果：肿瘤组织由小圆形细胞构成，肿瘤细胞胞膜示ＭＩＣ２强阳性，肿瘤细胞胞浆内含有微管及神经内分泌颗粒。结论：ＰＮＥＴ是一种极度恶性的软组织小圆形细胞肿瘤，它的诊断必须依靠免疫组化及电镜。

脑脊膜血管外皮瘤的临床病理研究

背景与目的:原发于脑脊膜的血管外皮瘤临床少见。本文回顾分析我院收治的20例,探讨其临床病理特征、组织学发生及生物学行为。方法:结合临床资料、运用组织病理学和免疫组化方法观察20例原发于脑脊膜的血管外皮瘤,并对其中4例进行透射电镜观察。结果:本病中位年龄42.4岁,男女之比1.2∶1。临床上多以头痛等症状就诊。肿瘤可发生在颅内脑脊髓表面的任何部位。大体上:肿瘤多似有包膜,质地韧,部分呈鱼肉样。组织学:肿瘤组织内血管丰富,可见典型的“鹿角样”血管,血管周围为短梭形的肿瘤性外皮细胞,沿血管呈放射状分布,瘤细胞异形,见核分裂像。网状纤维染色:嗜银纤维围绕单个瘤细胞、并沿血管呈放射状分布。免疫组化标记:瘤细胞除Vim阳性外,其余S-100蛋白、FⅧ、EMA、GFAP和CD34均阴性。电镜:瘤细胞中见丰富的10nm的中丝,细胞外基膜明显,并围绕单个瘤细胞分布。随访:获随访的17例病人中8例复发(占47.1%)。结论:脑脊膜的血管外皮瘤为起源于脑脊膜间叶组织、低度恶性的肿瘤,组织学形态、免疫表型和超微结构类似于软组织的血管外皮瘤。

脑胶质瘤的血瘤屏障超微结构观察

目的 :探讨脑部胶质瘤中血瘤屏障的超微结构改变与胶质瘤细胞生物学特性之间的关系。方法 :应用电镜观察 1 3例胶质瘤患者瘤组织中血瘤屏障的超微结构改变。结果 :脑胶质瘤组织中的血瘤屏障发生的一系列改造和重建 :1、多数血瘤屏障中毛细血管基膜呈限局性或广泛性增厚 ,基板多层化 ,胶原纤维增生 ;2、多数毛细血管基膜的胶质膜侧常见大小不等 ,多少不一的虫蚀状空洞或血管外间隙扩大 ;3、毛细血管胶质膜侧脚板外侧基板常不完整 ;4、内皮细胞间紧密连接延长 ,偶见内皮细胞出现窗孔 ,内皮细胞增生出芽。结论 :脑胶质瘤组织中的血瘤屏障发生的一系列改造和重建的超微结构改变 。

恶性颗粒细胞瘤临床病理、免疫组化和超微结构观察

目的：探讨恶性颗粒细胞瘤的病理学诊断和鉴别诊断要点及组织学起源。方法：对３例恶性颗粒细胞瘤进行临床病理、免疫组化及超微结构观察研究。结果：男性２例，女性１例，平均年龄为４９岁。部位分别为颈部１例，右大腿２例。其中２例分别于术后２年半及７年复发，并伴有区域淋巴结转移。组织学上３例与良性颗粒细胞瘤十分相似，局部区域出现梭形瘤细胞，空泡状核及明显的核仁，其中１例在肿瘤的周边部可见到瘤细胞与外周神经束支之间有直接移行关系。免疫酶标结果显示瘤细胞强阳性表达Ｓ－１００蛋白和神经特异性烯醇化酶（ＮＳＥ），１例电镜检测显示胞浆内充满膜包被复合性溶酶体。结论：对临床明显恶性而组织学上却极似良性的恶性颗粒细胞瘤，以下几点能提示恶性诊断：（１）肿瘤超过４ｃｍ；（２）核分裂象超过２个／１０ＨＰＦ；（３）核呈空泡状并有明显的核仁；（４）出现梭形瘤细胞；（５）有肿瘤性坏死。此外，免疫组化标记及超微结构观察有助于鉴别诊断及揭示组织学起源。

双歧杆菌诱发实验性大肠癌凋亡的电镜观察

本文以大肠癌裸鼠移植瘤为动物模型，用透射电镜观察了青春型双歧杆菌对移植瘤超微结构的影响。结果表明：双歧杆菌经荷瘤鼠腹腔注射后能诱导多量大肠癌细胞凋亡，凋亡早期的细胞主要表现为核染色质浓缩边聚；中期为核膜破裂，胞核崩解，凋亡小体形成；晚期主要为邻近活细胞吞噬凋亡小体。提示双歧杆菌诱导大肠癌细胞程序化死亡可能是其抑瘤机制之一。

胰腺实性-假乳头状肿瘤的超微结构研究

目的探讨胰腺实性-假乳头状肿瘤(SPTP)的超微病理特征、鉴别诊断及组织起源。方法对3例SPTP进行了电镜观察。结果电镜观察见肿瘤细胞大小形态较一致,核圆形或卵圆形,异型不明显,可见核沟,核分裂象罕见.瘤细胞有丰富的线粒体及粗面内质网,可见到神经分泌颗粒,酶原样颗粒及特征性的环状板层体。结论SPTP可能起源于胰腺原始多潜能干细胞,诊断上须与胰腺其它良恶性肿瘤相鉴别.

妊娠滋养细胞肿瘤(疾病)的超微结构观察

本文报道了对１１４例葡萄胎、恶性葡萄胎、绒毛膜上皮癌的滋养细胞超微结构形态及其变化规律，试对滋养细胞肿瘤（疾病）本质的探讨。

18例良、恶性造釉细胞瘤的超微结构观察

通过18例牙源性良、恶性造釉细胞瘤的超微结构观察,发现肿瘤细胞岛的中心部细胞分化程度不一,呈现2种形态特征,据此将其分为二型。本文着重观察二型细胞在良、恶性造釉细胞瘤中的分布特点,并结合生物学行为进行了讨论。

伽玛刀治疗颅内肿瘤的光镜及电镜观察

目的探讨伽玛刀（γ-刀）治疗颅内肿瘤的形态学变化及其与临床的关系。方法应用光镜、电镜观察16例γ-刀照射后颅内肿瘤手术切除标本的病理形态学变化，其中星形细胞瘤7例，少突胶质细胞瘤2例；脑膜瘤2例；颅咽管瘤1例；血管母细胞瘤1例；垂体腺瘤1例和转移性腺癌2例。结果γ-刀照射后肿瘤中心和肿瘤边缘的瘤细胞及血管均出现不同程度的凝固性坏死，恶性肿瘤呈急性坏死，良性肿瘤呈延迟性坏死；边缘部位残留的瘤细胞较中心部位多，肿瘤旁脑组织中神经元、胶质细胞及血管均出现不同程度的损伤，但主要以胶质细胞损伤为显著。结论残留的瘤细胞是肿瘤复发的形态学依据，γ-刀对肿瘤旁脑组织的损伤与脑水肿的产生有密切关系。提示临床应注意选择适当的照射剂量及肿瘤大小，以防止肿瘤复发和预防脑水肿的发生。

多种肿瘤细胞表面超微结构的原子力显微镜观察及药物对细胞膜表面超微结构影响的初步研究

本文应用原子力显微镜对人胃癌SGC790 1、人肝癌HepG2、人肺癌AFTC A 1、人乳腺癌MCF_7_R和人肺腺癌A5 49等肿瘤细胞膜表面进行了超微结构的形态学观察和比较。并研究了Nm2 3 H1 NDPK A蛋白对人肺腺癌A5 49等细胞膜表面超微结构的影响。发现不同肿瘤细胞膜表面超微结构存在较大的差异 ,药物处理和对照组A5 49细胞膜的表面超微结构也存在较大差异 ,药物处理的A5 49细胞膜表面出现大量的疤痕状集聚物 ,而药物处理的其它几种肿瘤细胞膜表面未发现明显的变化。说明原子力显微镜具有发展为一种观察和鉴别某些细胞的有力工具的潜力 ,并有可能应用于病理学或药理学研究 ,但在这些研究中这种技术只能作为一种辅助手段。

子宫颈神经内分泌肿瘤临床病理学研究

目的探讨宫颈神经内分泌肿瘤(NTC)的临床病理特征、诊断鉴别诊断及其生物学行为。方法对5例NTC进行光镜、电镜、免疫组化观察分析、随访及文献复习。结果瘤组织呈弥漫性或片团状浸润,瘤细胞体积小,圆形、卵圆形或短梭形,胞质少,核深染,分裂象多见,每例均有坏死。2例可见菊形团样结构。免疫组化瘤细胞表达CK、低分子量CK(35βH11),5例瘤细胞均表达CgA、Syn及NSE。电镜观察到菊形团样结构及神经内分泌颗粒。5例NTC中2例为非典型类癌,3例为小细胞癌,2例伴鳞癌分化,1例伴腺癌分化。结论宫颈NTC的组织形态类似于肺的NTC,除典型类癌外,其恶性程度高,预后差。诊断宫颈神经内分泌癌必须两项以上神经内分泌标记物阳性或电镜观察到神经内分泌颗粒。病理诊断应与子宫颈内膜间质肉瘤、非霍奇金淋巴瘤及小细胞型低分化鳞癌等鉴别。免疫组化及电镜对这些肿瘤的鉴别诊断很有帮助。

肾脏原发性神经内分泌肿瘤4例临床病理学观察

目的 探讨肾脏原发性神经内分泌肿瘤（primary renal neuroendocrine tumors,PRNET）的临床病理学特征。方法 对4例PRNET切除标本行HE染色、免疫组化染色,电镜下观察其形态结构、免疫表型及超微结构特点,并复习相关文献。结果 4例PRNET中3例男性,1例女性;年龄39-73岁,平均50岁。2例PRNET因腰背部疼痛就诊,2例PRNET患者体检发现入院。4例PRNET镜下结构相似,肿瘤细胞呈管状、条带状紧密排列生长,部分呈巢、团状;肿瘤细胞规则一致,核深染,染色质细腻,核仁不易见,核分裂象均3个/10HPF。免疫表型：4例Syn均呈强阳性,2例CgA呈阳性,2例CKpan呈局灶阳性,1例P504S呈阳性;CD10、CD117、PAX2、PAX8、PLAP、Ksp-cadherin均阴性;Ki-67增殖指数1%-5%。1例PRNET于电镜下见胞质内有大量神经内分泌颗粒,细胞间有桥粒连接。结论 PRNET是一种罕见的肾脏肿瘤,可发生于肾脏任何部位,无明显性别差异。诊断多依靠病理学检查,并结合免疫表型,必要时辅助电镜技术以明确诊断。

卵巢硬化性间质瘤临床病理及电镜和免疫组化分析

目的探讨卵巢硬化性间质瘤(sclerosing stromaltumer of ovarg,SST)的临床病理、电镜及免疫组化特点。方法通过11例SST的临床、形态学特征、免疫组化及其中的5例电镜观察和10例随访。结果 11例中30岁以下8例,10例有月经紊乱,1例早熟,5例伴有腹水。光镜显示假小叶结构及小叶间疏松水肿的结缔组织和致密的胶原纤维,瘤细胞形态多样,可见印戒样细胞,血管丰富。电镜见有三类瘤细胞:分别为类似储脂细胞,纤维母细胞及原始未分化间叶细胞,瘤细胞间或周围有大量的毛细血管。组织化学:PAS全部(-);免疫组化:α-inhibin7例(+),4例(-);ER4例(+),7例(-);CR3例(+),8例(-);vimentin、SMA、PR均(+);CK、EMA均(-)。随访:术后月经均恢复正常,已婚未育2例术后都怀孕生子,未婚者中术后有2例结婚并已生子。结论 SST是一种具有特殊组织学结构的少见卵巢良性肿瘤,术后不复发,预后好。病理诊断应注意与卵巢印戒细胞间质瘤、卵泡膜细胞瘤、卵巢纤维瘤、Krukenberg瘤等鉴别。

扁桃体滤泡树突细胞肉瘤1例并文献复习

目的探讨扁桃体滤泡树突细胞肉瘤的临床和病理特点,提高对其诊治水平。方法运用组织病理学、免疫组化及电镜观察扁桃体滤泡树突细胞肉瘤的特征,总结临床特点和治疗情况,并复习文献加以分析。结果瘤组织常排列成结节状、旋涡状和席纹状,瘤细胞呈梭形合体状,核椭圆形,染色质点彩状,有小核仁。瘤细胞间常混有小淋巴细胞。瘤细胞CD35、S-100、CD68和Vim(+),CKAEl、CKAE3和LCA(-)。电镜下见瘤细胞胞质有多个长突起彼此相连。结论滤泡树突细胞肉瘤是一种少见的低度恶性肿瘤,发生于扁桃体者更为罕见,诊断依赖组织病理学及免疫组化标记。

胃间质瘤的临床病理改变

目的:了解胃间质瘤的特殊临床病理改变。方法:收集37例胃间质瘤的临床病理资料,常规光镜切片观察,免疫组化SMA,S100,CD34,CD117,CKp标记。2例恶性胃间质瘤新鲜组织常规电镜切片,观察超微结构。结果:胃间质瘤临床症状以上腹痛、肿块和呕血为主。良性间质瘤直径<4.5cm,无出血坏死,瘤细胞以梭形细胞为主,核分裂0-2个/50HPF。多数恶性间质瘤直径>5cm(20/25),有出血坏死,瘤细胞多形性,核分裂6-56个/HPF。免疫组化标记:肿瘤细胞以CD34和CD117阳性为主。电镜观察2例恶性间质瘤的瘤细胞中细胞器稀少,无密体密斑、神经内分泌颗粒和细胞外基板。结论:胃间质瘤临床症状与胃癌相似,良性和恶性胃间质瘤的病理诊断依据组织学改变和免疫组化染色。免疫组化和电镜观察示胃间质瘤以未分化型为主。