Secondary endoscopic submucosal dissection for locally recurrent or incompletely resected gastric neoplasms

AIM To investigate the feasibility and safety of secondary endoscopic submucosal dissection(ESD) for residual or locally recurrent gastric tumors. METHODS Between 2010 and 2017, 1623 consecutive patients underwent ESD for gastric neoplasms at a single tertiary referral center. Among these, 28 patients underwent secondary ESD for a residual or locally recurrent tumor. Our analysis compared clinicopathologic factors between primary ESD and secondary ESD groups. RESULTS The en bloc resection and curative rate of resection of secondary ESD were 92.9% and 89.3%, respectively. The average procedure time of secondary ESD was significantly longer than primary ESD(78.2 min vs 55.1 min, P = 0.004), and the adverse events rate was not significantly different but trended slightly higher in the secondary ESD group compared to the primary ESD group(10.7% vs 3.8%, P = 0.095). Patients who received secondary ESD had favorable outcomes without severe adverse events. During a mean follow-up period, no local recurrence occurred in patients who received secondary ESD. CONCLUSION Secondary ESD of residual or locally recurrent gastric tumors appears to be a feasible and curative treatment though it requires greater technical efficiency and longer procedure time.

Extrapancreatic malignancies and intraductal papillary mucinous neoplasms of the pancreas

Over the last two decades multiple studies have demonstrated an increased incidence of additional malignancies in patients with intraductal papillary mucinous neoplasms(IPMNs).Additional malignancies have been identified in 10%-52% of patients with IPMNs.The majority of these additional cancers occur before or concurrent with the diagnosis of IPMN.The gastrointestinal tract is most commonly involved in secondary malignancies,with benign colon polyps and colon cancer commonly seen in western countries and gastric cancer commonly seen in Asian countries.Other extrapancreatic malignancies associated with IPMNs include benign and malignant esophageal neoplasms,gastrointestinal stromal tumors,carcinoid tumors,hepatobiliary cancers,breast cancers,prostate cancers,and lung cancers.There is no clear etiology for the development of secondary malignancies in patients with IPMN.Although population-based studies have shown different results from single institution studies regarding the exact incidence of additional primary cancers in IPMN patients,both have reached the same conclusion:there is a higher incidence of extrapancreatic malignancies in patients with IPMNs than in the general population.This f inding has signif icant clinical implications for both the initial evaluation and the subsequent long-term followup of patients with IPMNs.If a patient has not had recent colonoscopy,this should be performed during the evaluation of a newly diagnosed IPMN.Upper endoscopy should be performed in patients from Asian countries or for those who present with symptoms suggestive of upper gastrointestinal disease.Routine screening studies(breast and prostate) should be carried out as currently recommended for patient's age both before and after the diagnosis of IPMN.

European vs 2015-World Health Organization clinical molecular and pathological classification of myeloproliferative neoplasms

The BCR/ABL fusion gene or the Ph^1-chromosome in the t(9;22)(q34;q11)exerts a high tyrokinase acticity,which is the cause of chronic myeloid leukemia(CML).The1990 Hannover Bone Marrow Classification separated CML from the myeloproliferative disorders essential thrombocythemia(ET),polycythemia vera(PV)and chronic megakaryocytic granulocytic myeloproliferation(CMGM).The 2006-2008 European Clinical Molecular and Pathological(ECMP)criteria discovered 3variants of thrombocythemia:ET with features of PV(prodromal PV),"true"ET and ET associated with CMGM.The 2008 World Health Organization(WHO)-ECMP and 2014 WHO-CMP classifications defined three phenotypes of JAK2^(V617F)mutated ET:normocellular ET(WHO-ET),hypercelluar ET due to increased erythropoiesis(prodromal PV)and ET with hypercellular megakaryocytic-granulocytic myeloproliferation.The JAK2^(V617F)mutation load in heterozygous WHO-ET is low and associated with normal life expectance.The hetero/homozygous JAK2^(V617F)mutation load in PV and myelofibrosis is related to myeloproliferative neoplasm(MPN)disease burden in terms of symptomaticsplenomegaly,constitutional symptoms,bone marrow hypercellularity and myelofibrosis.JAK2 exon 12mutated MPN presents as idiopathic eryhrocythemia and early stage PV.According to 2014 WHO-CMP criteria JAK2 wild type MPL^(515)mutated ET is the second distinct thrombocythemia featured by clustered giant megakaryocytes with hyperlobulated stag-horn-like nuclei,in a normocellular bone marrow consistent with the diagnosis of"true"ET.JAK2/MPL wild type,calreticulin mutated hypercellular ET appears to be the third distinct thrombocythemia characterized by clustered larged immature dysmorphic megakaryocytes and bulky(bulbous)hyperchromatic nuclei consistent with CMGM or primary megakaryocytic granulocytic myeloproliferation.

PVSG and WHO vs European Clinical,Molecular and Pathological Criteria for prefibrotic myeloproliferative neoplasms

The Polycythemia Vera Study Group(PVSG),World Health Organization(WHO) and European Clinical,Molecular and Pathological(ECMP) classifications agree upon the diagnostic criteria for polycythemia vera(PV) and advanced primary myelofibrosis(MF). Essential thrombocythemia(ET) according to PVSG and 2007/2008 WHO criteria comprises three variants of JAK2V617 F mutated ET when the ECMP criteria are applied. These include normocellular ET,hypercellular ET with features of early PV(prodromal PV),and hypercellular ET due to megakaryocytic,granulocytic myeloprolifera-tion(ET.MGM). Evolution of prodromal PV into overt PV is common. Development of MF is rare in normocellular ET(WHO-ET) but rather common in hypercellular ET.MGM. The JAK2V617 F mutation burden in heterozygous mutated normocellular ET and in heterozygous/homozygous or homozygous mutated PV and ET.MGM is of major prognostic significance. JAK2/MPL wild type ET associated with prefibrotic primary megakaryocytic and granulocytic myeloproliferation(PMGM) is characterized by densely clustered immature dysmorphic megakaryocytes with bulky(bulbous) hyperchromatic nuclei,which are never seen in JAK2V617 F mutated ET,and PV and also not in MPL515 mutated normocellular ET(WHO-ET). JAK2V617 mutation burden,spleen size,LDH,circulating CD34+ cells,and pre-treatment bone marrow histopathology are mandatory to stage the myeloproliferative neoplasms ET,PV,PMGM for proper prognosis assessment and therapeutic implications. MF itself is not a disease because reticulin fibrosis and reticulin/collagen fibrosis are secondary responses of activated polyclonal fibroblasts to cytokines released from the clonal myeloproliferative granulocytic and megakaryocytic progenitor cells in ET.MGM,PV and PMGM.

Epithelioid Angiosarcoma of Bone: A Neoplasm with Potential Pitfalls in Diagnosis

Angiosarcoma of bone is an exceedingly rare primary bone malignancy that can present as an aggressive osteolytic lesion. This subset can radiologically mimic non-vascular neoplasms and impose serious challenges in reaching the correct diagnosis. Meanwhile histological diagnosis can be extremely challenging too, as the pathological features often resemble that of aneurysmal bone cysts. We present an unusual case of a 22-year-old woman who presented with a rapidly growing humeral tumor of 8 months’ duration. The case of intraosseous angiosarcoma presented as a diagnostic dilemma and the relevant radiological and pathologic findings were discussed. We describe the clinical, radiological and pathological features of this unique case, and review the literature concerning Angiosarcoma of bone. Our case highlights the diagnostic difficulties for such very rare tumours and clinico-pathological correlation is of paramount importance to differential diagnosis.

Bone Dysmorphia-Induced Blindness Following a Secondary Hyperparathyroidism: A Case Report

Introduction: Conjunctival-corneal or choroidal calcifications are frequent in SHPT, blindness is however exceptional. We report a case of blindness secondary to compressive ischemic optic neuropathy. Case Report: Mr. B.E.K., 49 years old, has a chronic renal failure secondary to unlabeled glomerular nephropathy for 17 years. He has been on chronic hemodialysis for 12 years and has had SHPT for nine years. He secondarily developed disabling segmental osteoarticular deformities associated with kyphoscoliosis, “drumstick” fingers and facial dysmorphism. Five months before admission he developed eye pain and reduced visual acuity progressing within one month to blindness. Biology noted: serum creatinine at 726 umol/l (60 - 120 umol/L), azotemia at 14.3 mmol/l (2.5 - 7.5 mmol/L), serum calcium at 2.25 (2.25 - 2.55 mmol/L), phosphatemia at 1.13 (0.8 - 1.35 mmol/L), alkaline phosphatases at 2196 (5 - 270 IU/L) and parathyroid hormone level at 2257 (10 - 60 pg/mL). Retinal angiography revealed lesions suggestive of ischemic neuropathy. The orbit CT scan with 3D coronal reconstruction revealed narrowing of the caliber of the optical channels with dystrophic thickening of the skull base and cranial vault. Cranioencephalic and orbital MRI revealed diffuse brown tumors and pre-chiasmatic optic atrophy. Discussion: The most frequent ocular complications of SHPT are conjunctival-corneal or sclero-choroidal calcifications, asymptomatic, associated with hypercalcemia. Compressive manifestations are rarer, represented mainly by an amputation of the visual field, diplopia, ptosis or blindness, as described in our patient. The main cause is osteodystrophy and brown tumors of the skull base (1% - 2%). Conclusion: This case report underlines the importance of early detection of SHPT, in order to avoid its major complications, such as blindness, especially since current preventive and curative measures have proven their effectiveness.

VSD治疗对胫骨骨折术后继发骨感染患者手术指标、炎性因子及功能恢复的影响

目的探讨负压封闭引流技术(VSD)治疗对胫骨骨折术后继发骨感染患者手术指标、炎性因子、功能恢复的影响。方法选取2020年12月至2022年6月河北医科大学第三医院收治的87例胫骨骨折内固定术后继发骨感染患者,均为胫骨干骨折;其中原开放骨折55例,一期均缝合伤口;32例在外伤发生时一期清创后行内固定手术;对患者采用手术清创、去除内固定物,行外固定架固定,经清创后局部均存在创面不能完全闭合,合并骨外露,随机选用VSD覆盖治疗(研究组,n=46)或骨水泥覆盖治疗(对照组,n=41),分析患者病原菌构成分布、比较两组手术指标、炎症因子[肿瘤坏死因子-α(TNF-α)、白介素-6(IL-6)、C反应蛋白(CRP)水平]、功能恢复情况[膝关节、踝关节功能以及肢体功能恢复情况]以及并发症情况。结果87例患者共87株病原菌,其中革兰阳性菌43株(49.42%),革兰阴性菌32株(36.78%),真菌12株(13.80%)。研究组换药次数少于对照组,控制感染时间、创面无菌时长、住院时间、行皮瓣转移手术时间均短于对照组,差异均有统计学意义(P<0.05);治疗后两组TNF-α、IL-6、CRP水平均下降,其中研究组变化最为显著,差异有统计学意义(P<0.05);治疗后两组HSS、Baird-Jackson评分均上升,其中研究组变化最为显著,差异有统计学意义(P<0.05)。研究组优良率为(95.65%)高于对照组优良率(80.49%),差异有统计学意义(P<0.05)。结论在创面不能闭合情况下,VSD治疗胫骨骨折内固定术后继发骨感染患者,可改善患者手术指标、炎性因子水平,促进患者肢体功能恢复,值得临床推广应用。

骨质疏松性椎体压缩骨折二级预防失败患者骨代谢指标及骨密度的变化

目的了解骨质疏松性椎体压缩骨折二级预防失败患者骨代谢指标及骨密度的特点。方法选择2015年1月至2020年1月在我院骨科因骨质疏松性椎体压缩骨折行2次或2次以上手术治疗的患者为观察组研究对象,共65例,同时选择同时期行手术治疗的非多次脊柱压缩骨折患者219例作为配对资料对照组,回顾性分析这284例患者临床资料,记录其术前骨代谢标志物水平及骨密度(bone mineral density,BMD)结果并进行两组患者间比较。结果观察组患者骨代谢标志物中人血清和血浆中的总I型前胶原氨基端肽(tP1NP)、N⁃MID骨钙素(OCN)以及血清25⁃羟维生素D(25⁃hydroxy vitamin D,25OHD)水平与对照组相比差异无统计学意义(P>0.05),骨代谢标志物I型胶原羧基端肽β特殊序列(β⁃CTX)水平明显高于对照组(P<0.05)。两组患者髋部BMD值、股骨颈BMD值差异无统计学意义(P>0.05),观察组腰椎BMD值明显低于对照组(P<0.05)。结论骨质疏松性椎体压缩骨折二级预防失败患者具有更为活跃的骨吸收状态及更低的腰椎骨密度。

3D氨基质子转移加权成像联合弥散加权成像鉴别良、恶性骨与软组织肿瘤

目的探讨3D氨基质子转移加权成像(APTWI)、弥散加权成像(DWI)及二者联合鉴别良、恶性骨与软组织肿瘤的价值。方法前瞻性对96例骨盆或下肢骨与软组织肿瘤患者采集平扫MRI、APTWI及DWI。分别基于APTWI及DWI获得偏移量为3.5 ppm的非对称性磁化传递率(MTRasym)图及表观弥散系数(ADC)图,测量病灶MTRasym(3.5 ppm)最大值(MTRasym_(max))、均值(MTRasym_(mean))及最小值(MTRasym_(min)),以及ADC最大值(ADC_(max))、均值(ADC_(mean))及最小值(ADC_(min));比较良、恶性肿瘤各参数差异,绘制受试者工作特征曲线,计算曲线下面积(AUC),评估APTWI、DWI及二者联合的鉴别诊断效能。结果96例中,良性41例、恶性55例。恶性肿瘤MTRasym(MTRasym_(max)、MTRasym_(mean)和MTRasym_(min))均明显高于,而ADC(ADC_(max)、ADC_(mean)和ADC_(min))均明显低于良性肿瘤(P均<0.05)。MTRasym_(max)和ADC_(min)鉴别良、恶性肿瘤的AUC分别为0.791和0.873,差异无统计学意义(P=0.122);二者联合的AUC为0.944,高于单一项(P<0.001、P=0.041)。结论APTWI联合DWI鉴别良、恶性骨与软组织肿瘤的效能较高。

动态对比增强MRI评估化学治疗用于兔VX2恶性骨肿瘤模型早期效果

目的观察动态对比增强MRI(DCE-MRI)评估化学治疗(简称化疗)用于兔VX2恶性骨肿瘤模型早期效果的价值。方法以30只实验兔成功建立VX2恶性骨肿瘤模型,以其中14只为化疗组,经静脉注射顺铂7 mg/kg体质量,以另16只为对照组,经静脉注射等量生理盐水。分别于造模2周后(干预前)及干预后3天采集平扫MRI及DCE-MRI,对MRI与病理所见进行点对点对照,获取瘤体区域容积转移常数(K^(trans))、速率常数(K_(ep))、血管外细胞外容积分数(V_(e))及血浆容积分数(V_(p)),以及微血管密度(MVD)。比较组内干预前、后MRI结果,以及干预后组间MRI结果,以受试者工作特征(ROC)曲线及曲线下面积(AUC)评估各参数判断是否曾接受化疗的效能,分析干预后DCE-MRI各参数与MVD的相关性。结果化疗组干预前、后平扫MRI所见肿瘤最大径差异无统计学意义(P>0.05)。相比干预前,化疗组实体瘤区域K^(trans)、K_(ep)均降低、对照组均升高(P均<0.05),而2组V_(e)及V_(p)差异均无统计学意义(P均>0.05)。干预后化疗组K^(trans)及K_(ep)值均低于对照组(P均<0.05),而组间V_(e)及V_(p)差异均无明显统计学意义(P均>0.05)。以K^(trans)、K_(ep)、V_(e)及V_(p)判断是否曾接受化疗的AUC分别为0.964、0.933、0.317及0.455。干预后化疗组实体瘤区域MVD低于对照组(P<0.05);2组实体瘤区域K^(trans)、K_(ep)值均与MVD呈正相关(r=0.876、0.881,P均<0.05),而V_(e)或V_(p)值与MVD无显著相关性(r=0.118、0.202,P均>0.05)。结论DCE-MRI定量分析参数K^(trans)和K_(ep)可较为敏感地反映化疗用于VX2恶性骨肿瘤模型兔早期效果及其MVD变化。

维持性血液透析患者甲状旁腺切除术后早期骨饥饿综合征风险预测模型的构建与验证

目的:甲状旁腺切除术(parathyroidectomy,PTX)是治疗难治性继发性甲状旁腺功能亢进(secondary hyperparathyroidism,SHPT)的有效方法,但PTX后极易出现骨饥饿综合征(hungry bone syndrome,HBS),严重威胁维持性血液透析(maintenance hemodialysis,MHD)患者的生命健康。目前已有研究分析PTX后并发HBS的风险因素,但风险预测模型的预测性能和临床适用性仍待进一步验证。本研究旨在构建MHD伴SHPT患者PTX后并发HBS的风险预测模型,并验证其预测效果。方法:回顾性收集2020年1月至2021年12月在长沙捷奥肾病医院行PTX的MHD伴SHPT的368例患者为训练集,按照是否发生HBS分为HBS组和non-HBS组,对2组的一般资料、手术相关信息、生化指标等进行比较,应用多因素logistic回归筛选HBS的影响因素,建立风险预测模型。采用受试者操作特征(receiver operator characteristic,ROC)曲线、决策曲线、校准曲线对模型进行评价。收集2022年1至12月在中南大学湘雅三医院行PTX的MHD伴SHPT的170例患者为验证集进行外部验证。结果:MHD伴SHPT患者PTX后HBS发生率为60.60%,logistic回归分析结果显示:术前骨骼受累(OR=3.908,95%CI 2.179~7.171)、术前血钙(OR=7.174,95%CI 2.291~24.015)、术前全段甲状旁腺激素(intact parathyroid hormone,i PTH)(OR=1.001,95%CI 1.001~1.001)、术前碱性磷酸酶(alkaline phosphatase,ALP)(OR=1.001,95%CI 1.000~1.001)、术后第1天血钙(OR=0.006,95%CI0.001~0.038)是MHD患者伴SHPT行PTX后并发HBS的独立危险因素(均P<0.01)。构建的风险预测模型在内部训练集和外部验证集中均表现出良好的预测结果,内部验证集的准确度为0.821,灵敏度为0.890,特异度为0.776,约登指数为0.666,曲线下面积(area under curve,AUC)为0.882(95%CI 0.845~0.919);外部验证集的准确度为0.800,灵敏度为0.806,特异度为0.799,约登指数为0.605,AUC为0.863(95%CI 0.795~0.932)。结论:术前骨骼受累、术前血钙、术前iPTH、术前ALP、术后第1天血钙水平是MHD伴SHPT患者行PTX后并发HBS的影响因素,基于上述因素构建的风险预测模型可靠。

乳腺癌细胞条件培养基对骨髓间充质干细胞生物学行为的影响

目的探讨MCF-7乳腺癌细胞条件培养基对骨髓间充质干细胞(BMSC)增殖、凋亡和迁移的影响及分子机制。方法正常环境下培养的BMSC为对照组,以MCF-7细胞条件培养基培养的BMSC为MCF-7条件培养基组,向MCF-7条件培养基组添加10 nmol/L GSK690693(Akt抑制剂)为Akt抑制剂组,向MCF-7条件培养基组添加10µmol/L Reparixin(CXCR1/2抑制剂)为CXCR1/2抑制剂组。MTT实验检测各组BMSC增殖情况,Annexin V-FITC/PI双标记流式细胞凋亡实验检测各组BMSC凋亡率,Transwell细胞迁移实验检测各组BMSC的迁移能力,酶联免疫吸附试验检测两种细胞培养上清液和MCF-7细胞条件培养基中白细胞介素(IL)-8蛋白含量,Western blot检测各组BMSC的蛋白激酶B(Akt)/磷酸化Akt(p-Akt)和哺乳动物雷帕霉素靶蛋白(mTOR)/磷酸化mTOR(p-mTOR)蛋白表达。结果与对照组相比,MCF-7条件培养基组BMSC的细胞增殖水平、迁移数目以及p-Akt和p-mTOR蛋白相对表达量均增高,细胞凋亡率降低(P<0.05);与MCF-7条件培养基组相比,CXCR1/2抑制剂组和Akt抑制剂组BMSC的细胞增殖水平、迁移数目以及p-Akt和p-mTOR蛋白相对表达量均降低,细胞凋亡率增加(P<0.05);MCF-7细胞条件培养基和MCF-7培养上清液中IL-8蛋白含量均较BMSC培养上清液中IL-8蛋白含量高(P<0.05)。结论MCF-7细胞条件培养基通过激活Akt-mTOR信号通路促进BMSC增殖和迁移,抑制BMSC凋亡,其中IL-8-CXCR1/2轴发挥关键作用。

高载能超声骨刀的优化设计与性能评估

针对超声骨刀在手术过程中切割效率低和产生骨组织热损伤的问题,设计了具有二级放大结构的高载能超声骨刀。基于驻波理论的等效长度法,结合有限元仿真对其二级放大结构进行设计和优化,测试了其振动性能并进行了骨切割试验。结果表明:具有二级放大结构的超声骨刀的谐振频率为23306 Hz,振幅为140μm,骨切割表面平整且无损伤,满足临床手术需求。

口腔专科医院非计划二次手术的回顾性分析

目的探讨口腔专科医院非计划二次手术发生的特点及影响因素。方法选取北京大学口腔医院2016—2021年所有二次手术患者信息,对非计划二次手术的病种、发生原因等进行统计分析,通过logistic回归进一步分析舌恶性肿瘤非计划二次手术的相关性因素。结果2016—2021年共发生非计划二次手术468例(1.17%),与第一次手术的间隔时间为0~20 d。构成比排在前3位的病种为颌面部恶性肿瘤、颌面部良性肿瘤、颌面部感染,导致非计划二次手术的主要原因为皮瓣血管危象、手术后血肿出血,占比为90.17%(422/468)。非计划二次手术组男性319例,女性149例,男女之比为2.14∶1,年龄53.00(36.00,62.00)岁,住院时间14.00(12.00,18.00)d,总费用为68694.91(51773.01,89850.04)元;对照组男性19932例,女性19495例,年龄31.00(18.00,53.00)岁,住院时间7.00(4.00,10.00)d,总费用为12338.96(8869.90,28650.17)元,比较差异有统计学意义(P<0.05)。非计划二次手术术式以有皮瓣为主,占比为76.07%。2016—2021年三四级手术中非计划二次手术发生率为3.62%(397/10966),高于一二级手术的0.25%(71/28929)。年龄、饮酒史、高血压、皮瓣手术是影响舌恶性肿瘤非计划二次手术的主要危险因素(P<0.05)。结论应针对口腔颌面外科专业非计划二次手术危险因素,加强围手术期和手术分级管理,以提升医疗质量。

结直肠癌肝转移患者的血浆胆汁酸谱特征及临床价值

目的分析不同转移情况结直肠癌患者血浆胆汁酸含量及胆汁酸谱分布的差异,并评估血浆胆汁酸含量比值联合肿瘤标志物对结直肠癌肝转移的诊断价值。方法纳入2021年4月至2022年1月于上海中医药大学附属曙光医院就诊的结直肠腺癌肝转移或无转移患者163例,其中无转移组82例、肝转移组81例。收集患者的临床资料,用Karnofsky功能状态(KPS)评分评估生存质量;收集患者外周血样本,检测总胆汁酸及肿瘤标志物[癌胚抗原(CEA)和糖类抗原125(CA125)]水平,用高效液相色谱-串联质谱法检测血浆中15种胆汁酸的含量。分析两组患者胆汁酸含量及胆汁酸谱分布的差异,并绘制ROC曲线分析胆汁酸含量比值联合肿瘤标志物对结直肠癌肝转移的临床诊断效能。结果两组结直肠癌患者年龄、性别、肿瘤位置、病理分化程度、KPS评分差异无统计学意义(均P>0.05)。肝转移组患者总胆汁酸、CEA、CA125均较无转移组患者升高(均P<0.001),血浆胆汁酸谱中甘氨胆酸、脱氧胆酸、牛磺脱氧胆酸、甘氨脱氧胆酸、甘氨熊脱氧胆酸、石胆酸和甘氨石胆酸含量均较无转移组患者升高(均P<0.05),血浆次级胆汁酸含量高于无转移组患者(P<0.001),次级胆汁酸与初级胆汁酸含量比值高于无转移组患者(P<0.001)。次级胆汁酸与初级胆汁酸含量比值联合CEA、CA125诊断结直肠癌肝转移的灵敏度为71.60%,特异度为80.49%,AUC为0.820(95%CI 0.754~0.885,P<0.001)。结论结直肠癌肝转移患者血浆胆汁酸含量升高,胆汁酸谱异于无转移患者;次级胆汁酸与初级胆汁酸含量比值联合CEA、CA125对结直肠癌肝转移有较高的诊断价值。

帕米膦酸二钠对肺癌骨转移性疼痛及骨纤维结构的影响研究

目的观察帕米膦酸二钠对肺癌骨转移性疼痛的及骨纤维结构的影响。方法南阳医学高等专科学校附属中医院2021年1月至2022年12月收治的109例肺癌骨转移患者,所有患者均伴有不同程度的骨痛症状。采用随机数字表法对入组患者进行分组,即常规组(54例)和试验组(55例)。常规组予以内科综合止痛治疗,试验组在常规组的治疗基础上采用帕米膦酸二钠配合治疗,比较两组患者的骨纤维结构改善情况、疼痛介质变化情况、骨痛缓解情况及预后情况。结果治疗前,两组患者的骨纤维结构相关指标差异无统计学意义(P>0.05);治疗后,试验组的骨钙素、Ⅰ型胶原C端肽、Ⅰ型胶原氨基端前肽均低于常规组(P<0.05)。治疗前,两组患者的疼痛介质差异无统计学意义(P>0.05);治疗后,试验组的前列腺素、血清乳酸均低于常规组(P<0.05)。治疗前,两组患者的骨痛程度差异无统计学意义(P>0.05);在不同治疗方案下,试验组治疗1~3个周期后的视觉模拟疼痛量表评分均低于常规组(P<0.05)。在不同治疗方案下,两组不良反应发生率比较,差异无统计学意义(P>0.05);试验组的肺癌患者生存质量测定量表中,身体状况评分,社交/家庭状况评分,情感状况评分及功能状况评分均高于常规组(P<0.05)。结论帕米膦酸二钠能有效改善肺癌骨转移患者的骨纤维结构,可通过下调疼痛介质水平而缓解骨痛症状,用药安全性良好,对改善患者远期生活质量有积极意义。

慢性肾脏病继发甲状旁腺功能亢进患者甲状旁腺全切术后骨饥饿综合征影响因素分析

目的分析维持性血液透析治疗的慢性肾脏病合并难治性继发性甲状旁腺功能亢进(rSHPT)患者甲状旁腺全切除(tPTX)术后发生骨饥饿综合征(HBS)的影响因素。方法纳入行tPTX治疗的慢性肾脏病合并rSHPT患者116例。观察术后HBS发生情况并将患者分为HBS组和非HBS组。比较两组临床资料,选择单因素分析结果差异有统计学意义的因素纳入Logistic回归,分析HBS独立影响因素;采用多元线性回归分析HBS组患者静脉补钙时长和总补钙量的影响因素。结果术后88例(75.86%)患者发生HBS(HBS组)、28例未发生HBS(非HBS组)。HBS组男性比例、静脉补钙时长、总补钙量、术前全段甲状旁腺激素(iPTH)、手术前后碱性磷酸酶(ALP)水平高于非HBS组,年龄、术后1周血红蛋白、手术前后校正血钙水平低于非HBS组(P均<0.05)。Logistic回归分析结果显示,年龄、术前校正血钙、术后1周ALP是慢性肾脏病合并rSHPT患者tPTX术后发生HBS的独立影响因素(P均<0.05)。多元线性回归分析结果显示,年龄、术前iPTH、术后4 h校正血钙、术后血磷是HBS组总补钙量的独立影响因素(P均<0.05);年龄、术前iPTH、术后4 h校正血钙、ALP比值是HBS组静脉补钙时长的独立影响因素(P均<0.05)。结论年龄、术前血钙、术后ALP水平是慢性肾脏病合并rSHPT患者tPTX术后发生HBS的影响因素;低龄、术后4 h低血钙、术前高iPTH的患者术后补钙需求量更大。

慢性肾病继发性甲状旁腺功能亢进症术后骨饥饿综合征^(99)Tc^(m)-MIBI骨摄取

目的分析慢性肾病继发性甲状旁腺功能亢进症行甲状旁腺切除术后骨饥饿综合征(HBS)患者^(99)Tc^(m)-甲氧基异丁基异腈(MIBI)骨摄取情况,为临床诊疗提供参考。资料与方法回顾性分析2014年6月—2021年12月于南通大学附属江阴医院行甲状旁腺切除术的106例继发性甲状旁腺功能亢进症的影像及临床资料,采用视觉评估分析甲状旁腺平面显像骨骼显像剂摄取情况,根据术后有无发生HBS分为HBS组和非HBS组。比较两组患者临床特征、实验室指标及^(99)Tc^(m)-MIBI骨摄取的差异。结果106例中,42例(39.62%)^(99)Tc^(m)-MIBI骨摄取阳性,多表现为弥漫性骨骼显像剂摄取,以胸骨、锁骨及肋骨多见。与非HBS组相比,HBS组的年龄较小(t=-3.058),碱性磷酸酶和甲状旁腺激素水平较高(Z=-5.148、-2.218),血清校正钙较低(Z=-2.102),^(99)Tc^(m)-MIBI骨摄取的阳性率及部位数较高[50%比28%,2(1,3)比1(1,1);χ^(2)=5.344,Z=-2.970],差异均有统计学意义(P均<0.05)。结论慢性肾病继发性甲状旁腺功能亢进症行甲状旁腺切除术后发生HBS患者的碱性磷酸酶和甲状旁腺激素水平更高,更易发生^(99)Tc^(m)-MIBI骨摄取。

血液系统疾病相关骨损害研究进展

血液系统疾病是继发性骨质疏松症(osteoporosis, OP)的重要病因,除了疾病自身致病因素外,相关治疗方案亦对骨代谢产生负面影响,由此导致了此人群中高OP患病率及骨质疏松性骨折风险。然而,其发病机制目前尚未明确,同时缺乏相关诊疗管理建议。因此,本综述分别从致病危险因素与机制、骨损害表现及诊治进展总结了常见血液系统疾病导致继发性OP最新进展,以期为血液系统疾病相关继发性OP的诊疗及管理提供新的思路。

双荧光标记的人高骨转移肺腺癌细胞株的建立及其转录组学特征分析

背景与目的骨是肺腺癌常见的转移部位,但肺腺癌骨转移的机制尚不明确。目前肺腺癌骨转移机制研究缺乏易于示踪且稳定高骨转移的肺腺癌细胞模型,因此,本研究旨在建立绿色荧光蛋白(green f luorescent protein,GFP)和萤火虫荧光素酶(firefly luciferase,LUC)双标记的人高骨转移肺腺癌细胞株,为肺腺癌骨转移的研究提供新的实验工具。方法人肺腺癌细胞系A549-GFP-LUC经左心室注射至裸鼠体内构建骨转移模型,经连续3次体内驯化,获取人高骨转移肺腺癌细胞株A549-GFP-LUC-BM3;CCK-8(cell counting kit-8)、克隆形成实验比较A549-GFP-LUC-BM3细胞株和亲本细胞的体外增殖能力,划痕实验、Transwell实验以及Western blot比较迁移和侵袭能力;并进一步将A549-GFP-LUC-BM3细胞和亲本细胞行测序转录组学分析。结果成功建立人高骨转移肺腺癌细胞A549-GFP-LUC-BM3,相较于亲本细胞,该细胞骨转移发生率显著提高,且体外增殖、迁移和侵袭能力显著增强。转录组学测序结果显示,相较于亲本细胞,A549-GFP-LUC-BM3细胞中共筛选到差异基因2954个,其中1021个基因上调,1933个基因下调;基因本体(Gene Ontology,GO)功能富集显示差异基因主要定位于细胞外周、质膜以及细胞外基质等细胞组分,分子功能主要富集在信号受体结合、钙离子结合和细胞外基质结构成分等,生物过程富集在细胞黏附和生物黏附等;京都基因与基因组百科全书(Kyoto Encyclopedia of Genes and Genomes,KEGG)富集分析显示差异基因在细胞色素P450(cytochrome P450,CYP)对外源性物质的代谢、视黄醇代谢、细胞黏附分子、CYP对药物代谢、类固醇激素的生物合成以及核因子κB(nuclear factor kappa B,NF-κB)信号通路上显著富集。结论成功建立GFP和LUC双标记的人高骨转移肺腺癌细胞株,该细胞株在生物学行为水平和转录组测序水平均提示具有高骨转移潜能。