Screening and early diagnosis of osteoporosis through X-ray and ultrasound based techniques

Effective prevention and management of osteoporosis would require suitable methods for population screenings and early diagnosis. Current clinicallyavailable diagnostic methods are mainly based on the use of either X-rays or ultrasound(US). All X-ray based methods provide a measure of bone mineral density(BMD), but it has been demonstrated that other structural aspects of the bone are important in determining fracture risk, such as mechanical features and elastic properties, which cannot be assessed using densitometric techniques. Among the most commonly used techniques, dual X-ray absorptiometry(DXA) is considered the current 'gold standard' for osteoporosis diagnosis and fracture risk prediction. Unfortunately, as other X-ray based techniques, DXA has specific limitations(e.g., use of ionizing radiation, large size of the equipment, high costs, limited availability) that hinder its application for population screenings and primary care diagnosis. This has resulted in an increasing interest in developing reliable pre-screening tools for osteoporosis such as quantitative ultrasound(QUS) scanners, which do not involve ionizing radiation exposure and represent a cheaper solution exploiting portable and widely available devices. Furthermore, the usefulness of QUS techniques in fracture risk prediction has been proven and, with the last developments, they are also becoming a more and more reliable approach for assessing bone quality. However, the US assessment of osteoporosis is currently used only as a pre-screening tool, requiring a subsequent diagnosis confirmation by means of a DXA evaluation. Here we illustrate the state of art in the early diagnosis of this 'silent disease' and show up recent advances for its prevention and improved management through early diagnosis.

Evolving screening and surveillance techniques for Barrett's esophagus

Barrett's esophagus(BE) is a change in the esophageal lining and is known to be the major precursor lesion for most cases of esophageal adenocarcinoma(EAC).Despite an understanding of its association with BE for many years and the falling incidence rates of squamous cell carcinoma of the esophagus, the incidence for EAC continues to rise exponentially. In association with this rising incidence, if the delay in diagnosis of EAC occurs after the onset of symptoms,then the mortality at 5 years is greater than 80%. Appropriate diagnosis and surveillance strategies are therefore vital for BE. Multiple novel optical technologies and other advanced approaches are being utilized to assist in making screening and surveillance more cost effective. We review the current guidelines and evolving techniques that are currently being evaluated.

Computed tomography colonography in 2014:An update on technique and indications

Twenty years after its introduction, computed tomographic colonography (CTC) has reached its maturity, and it can reasonably be considered the best radiological diagnostic test for imaging colorectal cancer (CRC) and polyps. This examination technique is less invasive than colonoscopy (CS), easy to perform, and standardized. Reduced bowel preparation and colonic distention using carbon dioxide favor patient compliance. Widespread implementation of a new image reconstruction algorithm has minimized radiation exposure, and the use of dedicated software with enhanced views has enabled easier image interpretation. Integration in the routine workflow of a computer-aided detection algorithm reduces perceptual errors, particularly for small polyps. Consolidated evidence from the literature shows that the diagnostic performances for the detection of CRC and large polyps in symptomatic and asymptomatic individuals are similar to CS and are largely superior to barium enema, the latter of which should be strongly discouraged. Favorable data regarding CTC performance open the possibility for many different indications, some of which are already supported by evidence-based data: incomplete, failed, or unfeasible CS; symptomatic, elderly, and frail patients; and investigation of diverticular disease. Other indications are still being debated and, thus, are recommended only if CS is unfeasible: the use of CTC in CRC screening and in surveillance after surgery for CRC or polypectomy. In order for CTC to be used appropriately, contraindications such as acute abdominal conditions (diverticulitis or the acute phase of inflammatory bowel diseases) and surveillance in patients with a long-standing history of ulcerative colitis or Crohn’s disease and in those with hereditary colonic syndromes should not be overlooked. This will maximize the benefits of the technique and minimize potential sources of frustration or disappointment for both referring clinicians and patients.

A Critical Analysis of Machine Learning and Deep Learning Methods for Cervical Cancer Screening

Cervical cancer is a serious public health issue worldwide, and early identification is crucial for better patient outcomes. Recent study has investigated how ML and DL approaches may be used to increase the accuracy of vagina tests. In this piece, we conducted a thorough review of 50 research studies that applied these techniques. Our investigation compared the outcomes to well-known screening techniques and concentrated on the datasets used and performance measurements reported. According to the research, convolutional neural networks and other deep learning approaches have potential for lowering false positives and boosting screening precision. Although several research used small sample sizes or constrained datasets, this raises questions about how applicable the findings are. This paper discusses the advantages and disadvantages of the articles that were chosen, as well as prospective topics for future research, to further the application of ml and dl in cervical cancer screening. The development of cervical cancer screening technologies that are more precise, accessible, and can lead to better public health outcomes is significantly affected by these findings.

基于两步单源点筛选的改进退化解混和估计算法

退化解混和估计(Degenerate unmixing estimation technique,DUET)算法是一种典型的欠定盲源分离算法,其采用的二进制时频掩蔽会保留部分干扰信号。提出了基于两步单源点筛选的改进DUET算法,首先使用余弦角算法进行单源点筛选,再采用计算相似度的方法进行第二步单源点筛选。通过两步单源点筛选获得更精确的目标信号和干扰信号后,设计用于抵消干扰信号的滤波器取代DUET中的二进制时频掩蔽,达到抑制干扰信号和提取目标信号的目的。仿真实验结果表明,该方法在正定盲源分离和欠定盲源分离两种情况下都有较优的盲源分离性能。

胃癌患者围术期营养管理方案的构建

目的构建胃癌患者围术期营养管理方案,为临床营养管理实践提供参考。方法采用循证方法检索文献并提取最佳证据,结合9名临床专家经验访谈,形成胃癌患者围术期营养管理方案初稿。采用德尔菲法对15名专家进行专家函询。结果2轮专家函询有效回收率均为100%,专家权威程度分别为0.92、0.95,总体肯德尔和谐系数分别为0.205、0.218(均P<0.05)。最终形成包含营养管理模式、营养风险筛查和评估、术前营养干预、术后营养干预、营养支持监测与护理、出院宣教6项一级指标,16项二级指标,42项三级指标的营养管理方案。结论胃癌患者围术期营养管理方案涵盖围术期营养管理全过程,具有较好的可靠性和实用性,可进一步开展临床验证研究。

基于曲面拟合的光学偏折系统显示屏标定方法

针对透射式光学偏折系统中最关键的标定环节,提出使用曲面拟合方式拟合显示屏幕面形分布。建立基于透射式光学偏折术的波前检测仿真模型,分析两种不同的显示屏面形拟合方法对波前测量的影响。仿真结果显示:平面屏幕模型波前像差均方根误差(RMS)值为0.8375μm,而曲面屏幕模型仿真波前像差RMS值仅为0.0596μm。采用透射式光学偏折系统对球面透镜进行波前测量,曲面屏幕模型中波前像差RMS值为0.1371μm,平面屏幕模型中波前像差RMS值为1.4326μm。实验结果表明:使用曲面拟合效果明显优于平面拟合效果,证明了曲面拟合屏幕模型的可行性。

循环肿瘤DNA在消化道肿瘤早期筛查中的研究进展

消化道肿瘤发病率高,起病隐匿,且预后较差。传统的筛查方法存在创伤性、滞后性、敏感度及特异度低等不足,导致其在消化道肿瘤早期筛查中的推广应用受到限制。循环肿瘤DNA(circulating tumor DNA,ctDNA)是由肿瘤细胞坏死或凋亡后释放到体液中的游离DNA片段,携带有突变、重排和甲基化等肿瘤特异性改变的遗传信息,与传统组织活检相比,ctDNA检测具有敏感度和特异度高、无创、易获得以及可重复性好的优势,在消化道肿瘤早期筛查中有很大潜力。本文通过对ctDNA在消化道肿瘤早期筛查中的研究现状作一综述,旨在评估ctDNA在消化道肿瘤诊断中的潜在价值,为探索消化道肿瘤的早期诊断手段提供理论依据。

小麦耐盐种质筛选及栽培调控技术研究进展

小麦耐盐种质筛选及配套栽培调控技术研究是小麦耐盐品种选育、盐碱地小麦减损稳产的前提。本文简介了小麦耐盐种质筛选流程、耐盐性评价指标与方法,重点总结了山东、河北、新疆和江苏4省的耐盐小麦品种(系)概况以及抗盐相关栽培调控技术研究进展,提出了研究存在筛选方法不统一、盐碱地实地筛选研究缺乏和栽培调控技术不系统等问题,建议统一室内筛选方法、利用室外盐池和盐碱地开展耐盐种质筛选及配套抗盐栽培调控技术研发,并基于多组学技术从遗传学和生理学角度系统探究小麦耐盐种质的耐盐机理以及栽培调控原理。

生姜蛋白酶水解产物中二肽基肽酶-Ⅳ抑制肽的虚拟筛选及活性分析

根据生姜蛋白酶的水解特异性,从其水解物中虚拟筛选出高活性肽段,进行体外活性验证和体内吸收入血成分研究。利用Peptide Ranker和分子对接虚拟筛选出高活性肽段,建立体外酶促反应体系测定活性肽对二肽基肽酶-Ⅳ(DPP-Ⅳ)的抑制活性(IC50),并且在此基础上,引入表面等离子体共振(SPR)技术深入研究DPP-Ⅳ与活性肽的相互作用,并开展大鼠灌胃实验研究活性肽在胃肠道消化系统中的稳定性。通过计算机模拟,虚拟筛选得到Gly-Pro-Ser-Gly-Pro-Hyp-Gly-Pro-Hyp-Gly-Pro-Hyp-Gly(GPSGPXGPXGPXG)DPP-Ⅳ抑制肽。体外酶促实验表明GPSGPXGPXGPXG对DPP-Ⅳ具有较强的抑制作用,IC50为457.3μmol/L,SPR实验进一步表明二者之间具有快速结合和快速解离的动力学过程,但是大鼠体内实验提示,该多肽无法维持胃肠道稳定性,不是以原型形式被消化道吸收,而是部分以二肽和三肽的形式进入血液循环系统,包括Pro-Hyp、Gly-Pro-Hyp和Pro-Hyp-Gly等寡肽。该研究表明筛选得到的活性肽口服经消化道吸收后无法保持结构完整性,会被体内的肽酶水解,这为后续进行体内的药代动力学和药效学研究提供理论支撑。

早期检测羟氯喹视网膜病变的研究现状

羟氯喹(hydroxychloroquine,HCQ)被越来越多地应用于各种自身免疫性疾病的治疗,然而长期服用HCQ可导致不可逆的视网膜毒性病变,并且随着检测技术的进步,其发病率比以往认知的更高,而早期检测到HCQ所致的视网膜毒性改变可以极大地降低晚期进展的风险。目前指南推荐的检查方法包括频域光学相干断层扫描(spectral-domain optical coherence tomography,SD-OCT)、眼底自发荧光(fundus autofluorescence,FAF)、多焦视网膜电图和自动视野检查。近年来研究发现,一些新的视网膜成像技术可能有助于识别早期病变,在此总结了目前在HCQ视网膜病变患者中应用的检查方法及新的成像技术,如定量自发荧光、微视野和逆模式成像等,并考虑未来使用这些新兴技术进行早期疾病检测的前景。

豆薯抗氧化成分提取工艺优化及其活性成分分析

采用酶解辅助乙醇浸提豆薯抗氧化活性成分。以ABTS、DPPH自由基清除率为评价指标,通过单因素试验和正交试验对提取工艺进行优化。在最佳提取条件下,测定豆薯提取液中总酚、总黄酮和维生素C含量,并分析其抗氧化活性组分。结果表明:最佳提取工艺条件为酶添加量0.4%(以豆薯干粉质量计)、提取时间60 min、提取温度50℃、料液比1∶10(g/mL);在此条件下制备的豆薯提取液对ABTS、DPPH自由基清除率分别为90.45%、56.28%,总酚、总黄酮和维生素C含量分别为(111.31±2.35)、(92.41±3.07)、(20.77±2.31)mg/100 g。豆薯提取液的主要抗氧化成分为香兰素、大豆甙元、芒柄花素和大豆素。

Strategic insights into the cultivation of pancreatic cancer organoids from endoscopic ultrasonography-guided biopsy tissue

BACKGROUND The frequent suboptimal efficacy of endoscopic ultrasound-guided fine-needle biopsy(EUS-FNB)to culture pancreatic cancer(PC)organoids(PCOs)poses a major challenge in the advancement of personalized medicine for advanced PC.AIM To explore how to obtain appropriate puncture tissues from EUS-FNB and optimize the strategy for efficiently constructing PCOs,providing an efficient tool for the advancement of personalized medicine.METHODS Patients who underwent EUS-FNB for the diagnosis of PC tissue were prospectively enrolled.We refined the endoscopic biopsy procedures and organoid cultivation techniques.All tissue specimens verified by on-site pathological assessment were cultured in a semi-suspended medium in a microfluidic environment.We assessed differences in PCOs cultured beyond and below five generations examining patient demographics,specimen and organoid attributes,and the sensitivity of organoids to a panel of clinical drugs through cell viability assays.RESULTS In this study,16 patients with PC were recruited,one sample was excluded because onsite cytopathology showed no tumor cells.Successful organoid generation occurred in 93.3%(14 of 15)of the EUS-FNB specimens,with 60%(9 of 15)sustaining over five generations.Among these patients,those with a history of diabetes,familial cancer,or larger tumors exhibited enhanced PCO expandability.The key factors influencing longterm PCOs expansion included initial needle sample quality(P=0.005),rapid initiation of organoid culture postisolation(P≤0.001),and high organoid activity(P=0.031).Drug sensitivity analysis revealed a partial response in two patients following therapeutic intervention and surgery and stable disease in four patients,indicating a moderate correlation between organoid response and clinical outcomes.CONCLUSION Optimal initial needle sampling,rapid and precise biopsy sample processing,process isolated samples as soon as possible,and sufficient cellular material are crucial for successful cultivating PCOs.High organoid activity is an important factor in maintaining their long-term expansion,which is essential for shortening the time of drug sensitivity analysis and is the basis of PC research.

J亚群禽白血病病毒血液核酸筛查技术的建立

为缩短J亚群禽白血病病毒(subgroup J avian leukosis virus, ALV-J)检测周期,进一步加快禽白血病净化进程,本研究结合SYBR GreenⅠqPCR和混样检测,建立了一种适用于低ALV-J流行率场景下的快速筛检ALV-J的血液核酸筛查技术(ALV-J blood quantitative polymerase chain reaction, ALV-J-B-qPCR)。根据GenBank中ALV-J pol及env基因序列,设计ALV-J的特异性引物,并优化反应条件,建立了ALV-J SYBR GreenⅠqPCR检测方法。以ALV-J病毒分离为阳性的鸡抗凝血为实验材料,分别制备抗凝血DNA、血细胞DNA、外周血淋巴细胞DNA、外周血淋巴细胞cDNA和血浆cDNA 5类血液检测模板进行ALV-J的PCR检测,筛选最佳检测模板;进一步比较蒸馏水破裂红细胞法提取混合血液DNA的混样方法,血液混样总体积为200μL的混样方法,血液混样总体积为10μL的混样方法共3种混样方法的检测准确性,筛选最佳混样方法。综合上述qPCR方法、检测模板与混样方法,成功建立了ALV-J-B-qPCR。运用ALV-J-B-qPCR分别进行预期流行率为1%~2%、4%~5%场景下的模拟筛查试验,并与病毒分离法比较。qPCR方法的特异性、灵敏性和重复性试验显示,该方法仅特异性扩增ALV-J,对标准质粒的最低检测限度为1×10^(2)copies·μL^(-1),批内与批间变异系数均<1%。对90份临床送检血液样品的检测结果显示,该qPCR方法对ALV-J的检出率(15.6%)高于p27抗原ELISA和普通PCR的检出率(12.2%)。检测模板筛选试验中,抗凝血DNA最符合检测准确度高、操作复杂度和成本低的要求,为最佳检测模板。混样方法摸索试验中,混样总体积为10μL(混样规模<12份)的混样方法检测准确性最高,为最佳混样方法。在样本数为400份,预期流行率为4%~5%场景的模拟筛查中,ALV-J-B-qPCR检出率为6.25%,比病毒分离法高2.00%;在样本数为400份,预期流行率为1%~2%场景的模拟筛查中,ALV-J-B-qPCR检出率为2.25%,比病毒分离法高0.75%。本研究建立的ALV-J-B-qPCR技术具有灵敏性高、检测快速和节约成本的优势,为种禽场加快ALV净化进程提供了新的思路和方法。

宫颈脱落细胞特殊染色技术在宫颈病变筛查中的应用价值

目的:探讨宫颈脱落细胞特殊染色技术在宫颈病变筛查中的临床应用价值。方法:选取2022年8月-2023年5月在山东第二医科大学附属医院及潍坊市人民医院进行宫颈病变筛查的女性共2000例,所有对象均进行宫颈脱落细胞特殊染色技术(FRD)检测、人乳头瘤病毒(HPV)和液基薄层细胞(TCT)检测。3种筛查方法任一结果阳性病例行阴道镜检查,阴道镜下有病变者行宫颈活检。以宫颈组织病理结果为金标准,比较FRD、TCT、HPV、HPV+TCT组的检测效能及受试者工作特征曲线下面积(AUC)。结果:FRD检测灵敏度为83.8%、特异度为90.0%,Kappa值为0.618,AUC为0.869;TCT检测的灵敏度为65.1%、特异度为89.5%,Kappa值为0.485,AUC为0.773;HPV检测的灵敏度为94.6%、特异度为71.7%,Kappa值为0.387,AUC为0.832;HPV+TCT联合检测的灵敏度为98.9%、特异度为70.2%,Kappa值为0.391,AUC为0.846。结论:宫颈脱落细胞特殊染色试验用于宫颈病变筛查有较好的效果,可用于基层宫颈病变筛查。

探析工业电机设备故障的诊断与检排技术

针对电机设备常见故障的诊断特点,介绍了电机设备常见故障的诊断方法,研究了电机设备常见故障的种类、原因分析及检排方法,提出了三相异步电动机故障分析及排除。

NT超声检查技术在早孕期胎儿异常筛查中的应用效果分析

目的评价颈项透明层(NT)超声检查在早孕期胎儿异常筛查中的价值。方法选取1100例检查的孕妇,全部行NT超声检查,然后再将NT超声所示的胎儿异常与最终染色体基因检测及出生结果比较。结果在1100例进行NT超声检查中,出现胎儿异常共1.91%(21/1100)。其中,NT检查胎儿异常为NT增厚、水囊瘤的分别占比57.14%(12/21)、14.29%(3/21),出现腹腔内囊肿、左侧脉络丛异常回声、脐膨出、单脐动脉、三尖瓣反流、胎盘囊肿各占比4.76%(1/21)。而在实际的分娩过程中出现19例胎儿异常,总体诊断率为90.48%。结论NT超声检查技术是一种有效地早期诊断胎儿结构异常的方法,有效地评估胎儿染色体非整倍体风险,能为产科和妇科临床工作提供有价值的数据,具有较高的临床应用价值。

宫颈脱落细胞特殊染色技术在宫颈癌筛查中的应用效果

目的探讨宫颈脱落细胞特殊染色技术在宫颈癌筛查中的应用效果。方法选取本院妇科门诊101名宫颈癌筛查女性为研究对象,均进行液基薄层细胞(TCT)和宫颈脱落细胞特殊染色技术检查,以阴道镜下宫颈活检病理结果为金标准,比较两种检查方法的诊断效能。结果宫颈组织病理学检查显示阳性35例,阳性率为34.7%;TCT检查的敏感度为31.7%、特异度为61.0%、阳性预测值为54.3%、阴性预测值为37.9%、准确度为43.6%,低于宫颈脱落细胞特殊染色技术的46.5%、74.1%、57.1%、65.2%、62.3%。结论宫颈脱落细胞特殊染色技术为无损伤检查,具有便携性高、操作简单、检测快速、经济实用和不依赖病理医师等特点,适用于人群普查或检测技术设备相对落后的偏远地区宫颈癌普查,也适合基层医院宫颈癌普查。

两癌筛查技术在农村妇女宫颈癌和乳腺癌防治中的应用进展

宫颈癌和乳腺癌属于女性常见癌症疾病,其致病因素和雌激素分泌异常、不良性生活、遗传因素等有关。乳腺癌发生在女性乳腺部位,而宫颈癌发生于女性子宫颈部,均会对患者的身体健康造成恶劣影响,加大患者精神压力的同时还会严重威胁患者的生命安全。因两癌临床特征均具有隐匿性和无特异性,患者察觉度低且容易和其他疾病混淆,一旦发现,病情已经发展为中晚期,死亡风险很高。越早鉴别,对宫颈癌和乳腺癌患者治疗的优势也就越大,同时患者预后恢复效果也就越好。因此,两癌筛查和鉴别对保障患者生命安全有极大的积极意义。查阅了相关文献,就两癌筛查技术在农村妇女宫颈癌和乳腺癌防治中的应用进行了综述。

Multitarget stool DNA for colorectal cancer screening:A review and commentary on the United States Preventive Services Draft Guidelines

Multitarget stool DNA(mt-sDNA) testing was approved for average risk colorectal cancer(CRC) screening by the United States Food and Drug Administration and thereafter reimbursed for use by the Medicare program(2014).The United States Preventive Services Task Force(USPSTF) October 2015 draft recommendation for CRC screening included mt-s DNA as an "alternative" screening test that "may be useful in select clinical circumstances",despite its very high sensitivity for early stage CRC.The evidence supporting mt-s DNA for routine screening use is robust.The clinical efficacy of mt-s DNA as measured by sensitivity,specificity,life-years gained(LYG),and CRC deaths averted is similar to or exceeds that of the other more specifically recommended screening options included in the draft document,especially those requiring annual testing adherence.In a population with primarily irregular screening participation,tests with the highest point sensitivity and reasonable specificity are more likely to favorably impact CRC related morbidity and mortality than those depending on annual adherence.This paper reviews the evidence supporting mt-s DNA for routine screening and demonstrates,using USPSTF's modeling data,that mt-s DNA at three-year intervals provides significant clinical net benefits and fewer complications per LYG than annual fecal immunochemical testing,high sensitivity guaiac based fecal occult blood testing and 10-year colonoscopy screening.