Soybean(Glycine max)rhizosphere organic phosphorus recycling relies on acid phosphatase activity and specific phosphorusmineralizing-related bacteria in phosphate deficient acidic soils

Bacteria play critical roles in regulating soil phosphorus(P) cycling. The effects of interactions between crops and soil P-availability on bacterial communities and the feedback regulation of soil P cycling by the bacterial community modifications are poorly understood. Here, six soybean(Glycine max) genotypes with differences in P efficiency were cultivated in acidic soils with long-term sufficient or deficient P-fertilizer treatments. The acid phosphatase(AcP) activities, organic-P concentrations and associated bacterial community compositions were determined in bulk and rhizosphere soils. The results showed that both soybean plant P content and the soil AcP activity were negatively correlated with soil organic-P concentration in P-deficient acidic soils. Soil P-availability affected the ɑ-diversity of bacteria in both bulk and rhizosphere soils. However, soybean had a stronger effect on the bacterial community composition, as reflected by the similar biomarker bacteria in the rhizosphere soils in both P-treatments. The relative abundance of biomarker bacteria Proteobacteria was strongly correlated with soil organic-P concentration and AcP activity in low-P treatments. Further high-throughput sequencing of the phoC gene revealed an obvious shift in Proteobacteria groups between bulk soils and rhizosphere soils, which was emphasized by the higher relative abundances of Cupriavidus and Klebsiella, and lower relative abundance of Xanthomonas in rhizosphere soils. Among them, Cupriavidus was the dominant phoC bacterial genus, and it was negatively correlated with the soil organic-P concentration. These findings suggest that soybean growth relies on organic-P mineralization in P-deficient acidic soils, which might be partially achieved by recruiting specific phoCharboring bacteria, such as Cupriavidus.

PHLPP与喉鳞状细胞癌转移的相关性及作用机制研究

目的探讨PH值域和亮氨酸丰富重复蛋白质磷酸酶蛋白(PHLPP)与喉鳞状细胞癌转移的相关性及作用机制。方法采用回顾性研究方法,选取2016年7月至2022年7月在河北工程大学附属医院治疗的89例喉鳞状细胞癌患者病灶标本,同时选取病灶周边正常组织作为对照。采用免疫组织化学法检测PHLPP蛋白表达;同时选取喉鳞状细胞癌HEP-2细胞株,随机分为PHLPP沉默组、PHLPP过表达组和空白对照组,采用MTT法检测各组细胞增殖,采用Transwell小室试验检测各组细胞迁移和侵袭,采用蛋白质印迹法检测各组PHLPP、BAX、PI3K和p-AKT蛋白表达。结果喉鳞状细胞癌组织PHLPP蛋白阳性表达率为38.20%,明显低于正常组织(95.51%),差异有统计学意义(P<0.05)。临床分期Ⅲ~Ⅳ期、有淋巴结转移、有远端转移的患者PHLPP蛋白阳性表达率分别为20.59%、17.50%、0,均显著低于临床分期Ⅰ~Ⅱ期、无淋巴结转移、无远端转移(79.41%、82.50%、100.00%),差异均有统计学意义(P<0.05)。PHLPP沉默组细胞培养24、48、72 h时吸光度值明显高于PHLPP过表达组和空白对照组;PHLPP过表达组细胞培养24、48、72 h时吸光度值明显低于空白对照组,差异均有统计学意义(P<0.05)。PHLPP沉默组细胞迁移和侵袭数均明显高于PHLPP过表达组和空白对照组(P<0.05);而PHLPP过表达组细细胞迁移和侵袭数均明显低于空白对照组,差异均有统计学意义(P<0.05)。PHLPP过表达组PHLPP、BAX蛋白表达量均明显高于PHLPP沉默组和空白对照组,而PI3K、p-AKT蛋白表达量均明显低于PHLPP沉默组和空白对照组,差异均有统计学意义(P<0.05);PHLPP沉默组PHLPP、BAX蛋白表达量均明显低于空白对照组,而PI3K、p-AKT蛋白表达量均明显高于空白对照组,差异均有统计学意义(P<0.05)。结论喉鳞状细胞癌组织PHLPP表达下调,与临床分期、淋巴结转移和远处转移有关;调控PHLPP表达对癌细胞增殖、迁移和侵袭有所影响,可能与调控BAX、PI3K和p-AKT蛋白有关。

Inhibiting phosphatase and actin regulator 1 expression is neuroprotective in the context of traumatic brain injury

Studies have found that the phosphatase actin regulatory factor 1 expression can be related to stroke,but it remains unclear whether changes in phosphatase actin regulatory factor 1 expression also play a role in traumatic brain injury.In this study we found that,in a mouse model of traumatic brain injury induced by controlled cortical impact,phosphatase actin regulatory factor 1 expression is increased in endothelial cells,neurons,astrocytes,and microglia.When we overexpressed phosphatase actin regulatory factor 1 by injection an adeno-associated virus vector into the contused area in the traumatic brain injury mice,the water content of the brain tissue increased.However,when phosphatase actin regulatory factor 1 was knocked down,the water content decreased.We also found that inhibiting phosphatase actin regulatory factor 1 expression regulated the nuclear factor kappa B signaling pathway,decreased blood-brain barrier permeability,reduced aquaporin 4 and intercellular adhesion molecule 1 expression,inhibited neuroinflammation,and neuronal apoptosis,thereby improving neurological function.The findings from this study indicate that phosphatase actin regulatory factor 1 may be a potential therapeutic target for traumatic brain injury.

Antagonizing adipose tissue-derived exosome miR-103-hepatocyte phosphatase and tensin homolog pathway alleviates autophagy in non-alcoholic steatohepatitis:A trans-cellular crosstalk

BACKGROUND Obesity plays a vital role in the occurrence and development of non-alcoholic steatohepatitis(NASH).However,the underlining mechanism is still unclear,where adipose tissue(AT)derived exosomes may actively participate.MicroRNAs(miRNAs)are commonly secreted from exosomes for cell communication.Though the regulation of miR-103 on insulin sensitivity has been reported,the specific role of AT-derived exosomes miR-103 in NASH is still vague and further investigation may provide novel therapeutic choices.AIM To determine the specific role of AT-derived exosomes miR-103 in developing NASH through various methods.METHODS The expression levels of miR-103 in the AT-derived exosomes and livers were detected and compared between NASH mice and control.The effect of miR-103 on NASH progression was also explored by antagonizing miR-103,including steatosis and inflammation degree changes.The interaction between miR-103 and the autophagy-related gene phosphatase and tensin homolog(PTEN)was confirmed by dual-luciferase reporter assay.The role of the interaction between miR-103 and PTEN on autophagy was verified in NASH-like cells.Finally,the effects of miR-103 from adipose-derived exosomes on NASH and autophagy were analyzed through animal experiments.RESULTS The expression of miR-103 was increased in NASH mice,compared to the control,and inhibition of miR-103 could alleviate NASH.The results of the dual-luciferase reporter assay showed miR-103 could interact with PTEN.MiR-103-anta decreased p-AMPKa,p-mammalian target of rapamycin(mTOR),and p62 but increased the protein levels of PTEN and LC3-II/I and the number of autophagosomes in NASH mice.Similar results were also observed in NASH-like cells,and further experiments showed PTEN silencing inhibited the effect of miR-103-anta.AT derivedexosome miR-103 aggravated NASH and increased the expressions of p-AMPKa,p-mTOR,and p62 but decreased the protein levels of PTEN and LC3-II/I and the number of autophagosomes in mice.CONCLUSION AT derived-exosome increased the levels of miR-103 in the liver,and miR-103 aggravated NASH.Mechanically,miR-103 could interact with PTEN and inhibit autophagy.

Single-cell analysis identifies phospholysine phosphohistidine inorganic pyrophosphate phosphatase as a target in ulcerative colitis

BACKGROUND Ulcerative colitis(UC)is a chronic gastrointestinal disorder characterized by inflammation and ulceration,representing a significant predisposition to colorectal cancer.Recent advances in single-cell RNA sequencing(scRNA-seq)technology offer a promising avenue for dissecting the complex cellular interactions and molecular signatures driving UC pathology.AIM To utilize scRNA-seq technology to dissect the complex cellular interactions and molecular signatures that underlie UC pathology.METHODS In this research,we integrated and analyzed the scRNA-seq data from UC patients.Moreover,we conducted mRNA and protein level assays as well as pathology-related staining tests on clinical patient samples.RESULTS In this study,we identified the sustained upregulation of inflammatory response pathways during UC progression,characterized the features of damaged endothelial cells in colitis.Furthermore,we uncovered the downregulation of phospholysine phosphohistidine inorganic pyrophosphate phosphatase(LHPP)has a negative correlation with signal transducer and activator of transcription 3.Significant downregulation of LHPP in UC patient tissues and plasma suggests that LHPP may serve as a potential therapeutic target for UC.This paper highlights the importance of LHPP as a potential key target in UC and unveils its potential role in inflammation regulation.CONCLUSION The findings suggest that LHPP may serve as a potential therapeutic target for UC,emphasizing its importance as a potential key target in UC and unveiling its role in inflammation regulation.

Root phosphatase activity is a competitive trait affiliated with the conservation gradient in root economic space

Background:The diversity of resource acquisition strategies of plant roots determines the species coexistence patterns to a certain extent.However,few root physiological traits have been investigated,such as root phosphatase activity(PA)that affects plant phosphorus(P)uptake.Methods:Root PA and classical root functional traits were investigated for 21 coexisting species in a deciduous broad-leaved forest in warm temperate-subtropical transition zone,China.We analyzed the root order variation of absorptive fine root PA,clarified the attribution of root PA in root economic space(RES)and the different P acquisition strategies of co-occurring species based on the multidimensional RES theory,and determined the dominant factors affecting interspecific variation in root PA.Results:There was no distinct pattern of PA variation with root order in the first three root orders of absorptive fine roots,and root PA was constrained by phylogeny.Root PA is a competitive trait affiliated with the conservation gradient in RES.The tight linkages among root PA,mycorrhizal colonization,diameter,specific root length,and nitrogen concentration suggested trade-offs among P acquisition strategies of co-occurring species,i.e.species with long and fine roots acquire inorganic P by actively exploring the soil and secreting phosphatase to mineralize and hydrolyze organic P,while species with short and thick roots obtain P mainly by investing C in mycorrhizal partners.Conclusions:Collectively,our study provides an insight into the forest species coexistence in climatic transition zones,i.e.species coexistence mechanisms based on diverse phosphorus acquisition strategies.

Cancerous inhibitor of protein phosphatase 2A enhances chemoresistance of gastric cancer cells to oxaliplatin

BACKGROUND Cancerous inhibitor of protein phosphatase 2A(CIP2A)is a newly discovered oncogene.It is an active cell proliferation regulatory factor that inhibits tumor apoptosis in gastric cancer(GC)cells.CIP2A is functionally related to chemoresistance in various types of tumors according to recent studies.The underlying mechanism,however,is unknown.Further,the primary treatment regimen for GC is oxaliplatin-based chemotherapy.Nonetheless,it often fails due to chemoresistance of GC cells to oxaliplatin.AIM The goal of this study was to examine CIP2A expression and its association with oxaliplatin resistance in human GC cells.METHODS Immunohistochemistry was used to examine CIP2A expression in GC tissues and adjacent normal tissues.CIP2A expression in GC cell lines was reduced using small interfering RNA.After confirming the silencing efficiency,3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide tetrazolium and flow cytometry assays were used to evaluate cell proliferation and apoptosis caused by oxaliplatin treatment.Further,the key genes and protein changes were verified using realtime quantitative reverse transcription PCR and Western blotting,respectively,before and after intervention.For bioinformatics analysis,we used the R software and Bioconductor project.For statistical analysis,we used GraphPad Prism 6.0 and the Statistical Package for the Social Sciences software version 20.0(IBM,Armonk,United States).RESULTS A high level of CIP2A expression was associated with tumor size,T stage,lymph node metastasis,Tumor Node Metastasis stage,and a poor prognosis.Further,CIP2A expression was higher in GC cells than in normal human gastric epithelial cells.Using small interfering RNA against CIP2A,we discovered that CIP2A knockdown inhibited cell proliferation and significantly increased GC cell sensitivity to oxaliplatin.Moreover,CIP2A knockdown enhanced oxaliplatin-induced apoptosis in GC cells.Hence,high CIP2A levels in GC may be a factor in chemoresistance to oxaliplatin.In human GC cells,CIP2A regulated protein kinase B phosphorylation,and chemical inhibition of the protein kinase B signaling pathway was significantly associated with increased sensitivity to oxaliplatin.Therefore,the protein kinase B signaling pathway was correlated with CIP2Aenhanced chemoresistance of human GC cells to oxaliplatin.CONCLUSION CIP2A expression could be a novel therapeutic strategy for chemoresistance in GC.

Transient hyperphosphatasemia in a toddler with COVID-19 infection:A case report and literature review

BACKGROUND Transient hyperphosphatasemia(TH)is a condition characterized by elevated serum alkaline phosphatase(ALP)in the clinical setting with no evidence of bone or liver disease among children under the age of 5.Typically,it will resolve spontaneously in a few months in the majority of cases.TH has been found to be associated with viral infections.Two cases of TH associated with coronavirus disease 2019(COVID-19)infection in toddlers have been previously reported.CASE SUMMARY A previously healthy 2-year-old boy presented with fever and positive real-time polymerase chain reaction for COVID-19.Prior to his illness,the patient had been in close contact with his grandfather,who later developed COVID-19.The physical examination on admission was unremarkable.He remained asymptomatic throughout 7 d of hospitalization.On the 5th day of his illness,blood tests showed markedly elevated serum ALP(4178 U/L).Results from the simultaneous testing of the remaining liver profiles and metabolic bone panels were normal.Two months after discharge from the hospital,the patient continued to thrive well.The skeletal surveys revealed no significant abnormalities.The serum ALP declined into the normal range adjusted for his age.This evidence is consistent with the diagnosis of TH.CONCLUSION TH can occur in COVID-19-infected toddlers.Serial measurements of ALP levels have been shown to gradually decline into the normal range within a few months.Therefore,being aware of this transient abnormality will help clinicians to avoid additional unnecessary investigations.

Overexpression of mitogen-activated protein kinase phosphatase-1 in endothelial cells reduces blood-brain barrier injury in a mouse model of ischemic stroke

Ischemic stroke can cause blood-brain barrier(BBB)injury,which worsens brain damage induced by stroke.Abnormal expression of tight junction proteins in endothelial cells(ECs)can increase intracellular space and BBB leakage.Selective inhibition of mitogen-activated protein kinase,the negative regulatory substrate of mitogen-activated protein kinase phosphatase(MKP)-1,improves tight junction protein function in ECs,and genetic deletion of MKP-1 aggravates ischemic brain injury.However,whether the latter affects BBB integrity,and the cell type-specific mechanism underlying this process,remain unclear.In this study,we established an adult male mouse model of ischemic stroke by occluding the middle cerebral artery for 60 minutes and overexpressed MKP-1 in ECs on the injured side via lentiviral transfection before stroke.We found that overexpression of MKP-1 in ECs reduced infarct volume,reduced the level of inflammatory factors interleukin-1β,interleukin-6,and chemokine C-C motif ligand-2,inhibited vascular injury,and promoted the recovery of sensorimotor and memory/cognitive function.Overexpression of MKP-1 in ECs also inhibited the activation of cerebral ischemia-induced extracellular signal-regulated kinase(ERK)1/2 and the downregulation of occludin expression.Finally,to investigate the mechanism by which MKP-1 exerted these functions in ECs,we established an ischemic stroke model in vitro by depriving the primary endothelial cell of oxygen and glucose,and pharmacologically inhibited the activity of MKP-1 and ERK1/2.Our findings suggest that MKP-1 inhibition aggravates oxygen and glucose deprivation-induced cell death,cell monolayer leakage,and downregulation of occludin expression,and that inhibiting ERK1/2 can reverse these effects.In addition,co-inhibition of MKP-1 and ERK1/2 exhibited similar effects to inhibition of ERK1/2.These findings suggest that overexpression of MKP-1 in ECs can prevent ischemia-induced occludin downregulation and cell death via deactivating ERK1/2,thereby protecting the integrity of BBB,alleviating brain injury,and improving post-stroke prognosis.

血清BALP/TALP比值诊断儿童和青少年骨肉瘤的临床意义

目的分析血清骨型碱性磷酸酶(BALP)/总碱性磷酸酶(TALP)比值用于诊断儿童和青少年骨肉瘤的价值及预测预后的意义。方法回顾性纳入2018年9月至2021年9月间在北京大学人民医院骨肿瘤科接受治疗的200例四肢骨肉瘤患者(骨肉瘤组),以及同期就诊的50例良性骨肿瘤患者(良性骨肿瘤组)及50例正常对照者(对照组)。采用化学发光免疫分析仪检测血清中BALP和TALP含量,并计算BALP/TALP。比较其含量与骨肉瘤临床病理特征的关系。采用受试者工作曲线(ROC)评价BALP/TALP诊断骨肉瘤的效能,并计算曲线下面积(AUC)。Kaplan-meier法绘制生存曲线,生存差异行Log-rank检验。采用Cox风险比例回归模型分析影响骨肉瘤预后的因素。结果骨肉瘤组血清BALP、TALP、BALP/TALP分别为71.52 IU/L(44.26,135.68)、192.00 IU/L(162.00,233.50)和0.37(0.21,0.67),均高于良性骨肿瘤组、健康对照组,差异具有统计学意义(P<0.05)。血清BALP/TALP水平诊断骨肉瘤的灵敏度为82.0%、特异度为89.5%,约登指数为0.715,截断值为0.19,AUC为0.925(95%CI:0.901~0.949,P<0.001)。血清BALP/TALP水平与肿瘤直径、分化程度、组织学类型、Enneking分期和局部/远隔转移等有关(P<0.05);与年龄、性别、肿瘤位置、Huvos分级等均无关。血清BALP/TALP水平≥0.37的骨肉瘤患者中位生存期低于血清BALP/TALP水平<0.37者(P<0.05)。Cox风险比例回归模型分析,血清BALP/TALP水平≥0.37为影响骨肉瘤患者预后的独立危险因素(P=0.001)。结论血清BALP/TALP水平诊断儿童与青少年骨肉瘤效能较高,且能有效预测预后。

SHP-2在肿瘤相关巨噬细胞中的研究进展

肿瘤相关巨噬细胞(TAMs)是肿瘤免疫微环境(TIME)中的优势细胞群,是TIME中免疫系统抑制和肿瘤细胞增殖最重要的调节细胞。Src同源2蛋白酪氨酸磷酸酶2(SHP-2)是一种非受体蛋白酪氨酸磷酸酶,该磷酸酶在从细胞表面到细胞核的信号传递中发挥重要作用,且是介导细胞增殖和分化的关键细胞内调节因子,参与多种生长因子和细胞因子的信号通路。最近的研究表明,SHP-2是决定TAMs功能的一个关键酶,但是由于其功能多变,在不同的实体瘤微环境中发挥不同甚至是相反的作用。基于此,本文综述了SHP-2在TAMs功能及在相关实体瘤中的作用,为肿瘤的免疫和靶向治疗提供坚实的科学依据。

新型酸性磷酸酶“Turn-on”型荧光底物

酸性磷酸酶(ACP)是前列腺癌、戈谢病、肾病等疾病的重要生物标记物,因此开发灵敏、高选择性的ACP检测方法具有重要的意义。目前,已发展出多种ACP检测方法,包括免疫法、光谱法、色谱法、电化学法等;其中,荧光检测方法因灵敏度高、选择性好、快速、准确等优点备受关注。通过席夫碱反应,利用2-氨基苯硼酸(2-APBA)二聚体和磷酸吡哆醛(PLP)合成了一种新型的ACP“Turn-on”型荧光底物APBA-PLP(ABPL)。反应后,PLP的—CHO基团和2-APBA二聚体的—NH 2基团的特征峰消失,同时ABPL的C N基团的特征峰出现;此外,^(1)H和^(1)H—^(1)H COSY核磁波谱的信号峰与ABPL的结构相对应。以上表征结果证实了ABPL的成功合成。进一步,将ABPL应用于ACP检测。我们发现向ABPL水溶液中加入ACP后,体系的荧光强度增强,机理为:2-APBA二聚体为聚集诱导发光增强(AIEE)分子,其AIEE特性源于2-APBA二聚体的高度有序堆积;当2-APBA二聚体分子上引入PLP后(即合成ABPL),分子的高度有序堆积结构被破坏;加入ACP后,PLP水解为吡哆醛并从2-APBA二聚体分子上脱落,2-APBA二聚体分子又可重新进行高度有序堆积,表现为体系的荧光增强。在0~5 U·L^(-1)活性范围内,376.5 nm处的相对荧光强度与ACP活性之间呈现出良好的线性关系(R 2=0.99)。此外,当ACP、果胶酶、木瓜蛋白酶和脂肪酶的活性分别为4、50000、80000和10000 U·L^(-1)时,四种酶对应的相对荧光强度分别为0.2、-0.006、0.03和0.05。该结果表明ABPL对ACP具有高选择性。ABPL分子易合成,对ACP具有线性和高选择性响应,为设计合成可用于ACP检测的新型高效荧光底物提供了新策略。

非小细胞肺癌组织中lncRNA GAS5、LHPP表达与上皮间质化相关性及临床意义

目的探讨非小细胞肺癌(NSCLC)患者癌组织中长链非编码核糖核酸生长抑制特异性基因5(lncRNA GAS5)、磷酸赖氨酸磷酸组氨酸无机焦磷酸盐磷酸酶(LHPP)表达与上皮间质化(EMT)相关性及临床意义。方法收集2018年6月至2020年1月在河北北方学院附属第一医院行手术切除的NSCLC 90例患者的癌组织及癌旁组织,采用实时荧光定量聚合酶链反应检测lncRNA GAS5、LHPP和EMT相关蛋白[E-钙黏蛋白(E-Cad)、N-钙黏蛋白(N-Cad)和波形蛋白(VIM)]表达。分析NSCLC患者癌组织中lncRNA GAS5、LHPP mRNA与临床病理特征的关系,并通过Pearson相关性分析NSCLC患者癌组织中lncRNA GAS5、LHPP mRNA与EMT相关蛋白表达的相关性。采用Kaplan-Meier法绘制不同lncRNA GAS5、LHPP mRNA表达的NSCLC患者生存曲线,多因素Cox回归分析NSCLC患者预后的影响因素。结果NSCLC患者癌组织中lncRNA GAS5、LHPP mRNA、E-Cad mRNA表达低于癌旁组织,N-Cad mRNA、VIM mRNA表达高于癌旁组织,差异有统计学意义(P<0.05)。Pearson相关性分析显示,NSCLC患者癌组织中lncRNA GAS5与E-Cad mRNA表达呈正相关(r=0.724,P<0.001),与N-Cad mRNA、VIM mRNA表达呈负相关(r=-0.699、-0.689,P<0.001);lncRNA GAS5与LHPP mRNA表达呈正相关(r=0.651,P<0.001)。不同分化程度、肿瘤TNM分期、淋巴结转移的NSCLC患者癌组织中lncRNA GAS5、LHPP mRNA表达比较差异有统计学意义(P<0.05)。Kaplan-Meier生存曲线分析显示,lncRNA GAS5高表达组的3年总生存率[68.18%(30/44)]高于lncRNA GAS5低表达组的3年总生存率[36.96%(17/46)];LHPP mRNA高表达组的3年总生存率[67.39%(31/46)]高于LHPP mRNA低表达组的3年总生存率[36.36%(16/44)],差异有统计学意义(χ^(2)=10.274、10.322,P<0.05)。低分化、肿瘤TNM分期Ⅲ期、有淋巴结转移为NSCLC患者死亡的独立危险因素,lncRNA GAS5≥1.32、LHPP mRNA≥1.12为独立保护因素(P<0.05)。结论NSCLC患者癌组织中lncRNA GAS5、LHPP mRNA低表达,与EMT相关蛋白表达、分化程度、肿瘤TNM分期、淋巴结转移和预后有关,可能成为NSCLC诊治的新靶点。

淫羊藿苷对前列腺癌原位移植瘤小鼠肿瘤生长及细胞周期的影响

目的探讨淫羊藿苷对前列腺癌原位移植瘤SCID小鼠肿瘤生长、细胞周期、磷酸酶及张力蛋白同源物(phosphatase and tensin homolog,PTEN)基因表达的影响。方法40只雄性SCID小鼠,根据随机数字表法随机均分为模型对照组、低剂量组、中剂量组、高剂量组,每组10只。采用SCID小鼠前列腺腺体背外侧包膜内注射人前列腺癌LNCaP细胞株悬液的方法构建前列腺癌原位移植瘤小鼠模型。造模2周后,模型对照组予以0.9%氯化钠注射液,低剂量组予以10 mg/kg淫羊藿苷,中剂量组予以40 mg/kg淫羊藿苷,高剂量组予以80 mg/kg淫羊藿苷。灌胃处理1次/d,治疗时间为5周。在灌胃给药治疗前及治疗5周后,分别取各组小鼠5只,对比各组肿瘤质量、肿瘤体积、肿瘤抑制率。采用流式细胞学方法检测LNCaP细胞周期,计算各周期比值。采用实时定量PCR检测前列腺肿瘤组织中PTEN mRNA相对含量。结果治疗后,模型对照组肿瘤质量、肿瘤体积较治疗前明显增加(P<0.05);中剂量组及高剂量组肿瘤质量、肿瘤体积较治疗前明显降低(P<0.05),且显著低于模型对照组(P<0.05)。中剂量组及高剂量组肿瘤抑制率显著高于低剂量组(P<0.05)。中剂量组及高剂量组肿瘤细胞S期较治疗前明显增加(P<0.05),且显著高于模型对照组(P<0.05);中剂量组及高剂量组肿瘤细胞G_(0)/G_(1)期较治疗前明显减少(P<0.05),且显著低于模型对照组(P<0.05)。中剂量组及高剂量组PTEN mRNA相对含量较治疗前明显增加(P<0.05),且显著高于模型对照组(P<0.05)。结论淫羊藿苷可能通过上调PTEN表达、改变细胞周期分布来抑制前列腺癌LNCaP细胞增殖,从而有效抑制前列腺癌原位移植瘤SCID小鼠肿瘤生长。

碱性磷酸酶、乳酸脱氢酶及Gleason分级用于评估低风险转移性激素敏感型前列腺癌预后的价值

目的探究碱性磷酸酶(ALP)、乳酸脱氢酶(LDH)及Gleason分级用于评估低风险转移性激素敏感型前列腺癌(mHSPC)预后的价值,为低风险mHSPC患者的诊疗提供科学参考。方法回顾性分析2015年至2021年丽水市人民医院低风险mHSPC患者,以出现去势抵抗性前列腺癌(CRPC)作为不良预后的主要结局指标,将48例出现CRPC的患者纳入观察组,未出现CRPC的48例患者纳入对照组。比较两组患者ALP、LDH和Gleason分级状况,采用受试者工作特征(ROC)曲线分析ALP、LDH、Gleason分级对mHSPC出现不良预后的预测作用。结果观察组患者ALP和LDH水平明显高于对照组,观察组Gleason分级4~5级患者占比明显高于对照组(P<0.05)。高ALP(≥300 U/L)、高LDH(≥200 U/L)、高Gleason分级(4~5级)三者联合曲线下面积为0.879,灵敏度为92.1%,特异度为87.6%。结论高ALP、高LDH、高Gleason分级是低风险mHSPC患者发生不良预后的相关因素,联合使用可为低风险mHSPC患者的临床诊治方案提供重要参考。

LHPP通过调控NOX2/SHP2通路活性抑制结直肠癌的增殖、侵袭和转移

目的探讨组氨酸磷酸酶(LHPP)通过氧化应激通路对结直肠癌增殖、侵袭和迁移的影响,并初步阐明其作用机制。方法使用Liposome3000进行细胞转染操作。将质粒OE-NC、OE-LHPP和寡核苷酸片段si-NC、si-LHPP分别转染进SW480细胞中,通过Western Blot检测LHPP、NOX2、p-SHP2的蛋白表达量;将质粒OE-NC、OE-LHPP组转染进SW480细胞中并同时使用NCA刺激,通过Western Blot检测NOX2、p-SHP2、p-PI3K、p-ERK1/2、MMP-9、Cyclin D1的蛋白表达量;将质粒OE-NC、OE-LHPP转染进SW480和SW620细胞中,并同时使用NAC刺激,通过划痕实验检测细胞的迁移距离,Transwell实验检测通过孔的细胞数量,克隆形成实验检测细胞的增殖能力。结果SW480细胞中OE-LHPP组LHPP和NOX2蛋白表达水平明显高于OE-NC组(P<0.05),但p-SHP2蛋白表达水平明显低于OE-NC组(P<0.01);SW480细胞中si-Si-LHPP组LHPP和NOX2蛋白表达水平明显低于OE-NC组(P<0.01),但p-SHP2蛋白表达水平明显高于si-NC组。与OE-NC组相比,SW480细胞中OE-LHPP的NOX2蛋白表达水平明显升高(P<0.01),但p-SHP2、p-PI3K、p-ERK1/2、MMP-9、Cyclin D1蛋白表达水平明显降低(P<0.01),SW480和SW680细胞迁移距离缩短、穿过孔的细胞数量减少和细胞克隆形成数量减少;加入NAC干预后,消除了SW480和SW680细胞中OE-NC组和OE-LHPP组在NOX2、p-SHP2、p-PI3K、p-ERK1/2、MMP-9、Cyclin D1的差异,也消除了细胞划痕、细胞侵袭和细胞增殖的差异。结论LHPP通过促进氧化应激抑制SHP2、PI3K和ERK通路活性进而抑制结直肠癌细胞的增殖、侵袭和迁移的影响进而缓解结直肠癌的进展。

间充质干细胞外泌体对缺血性脑卒中大鼠神经功能恢复的影响

目的探讨间充质干细胞外泌体(MSCs-EXO)对缺血性脑卒中大鼠神经功能恢复的影响。方法大鼠骨髓间充质干细胞原代培养,超速离心法提取其MSCs-EXO,大脑中动脉夹闭模型(MCAO)法制作大鼠缺血性脑卒中模型,MSCs-EXO经鼻给药,设为MSCs-EXO组,通过改良神经功能缺损评分(mNSS)和错步试验评估其神经功能恢复情况,并与未治疗模型组(MCAO组)做对比。PKH26标记MSCs-EXO并结合免疫荧光染色观察其在缺血半暗带(IP)中的分布,荧光定量PCR及Western blot检测IP区域脑组织中PTEN的表达水平,并与正常大鼠及MCAO组大鼠进行对比。结果MSCs-EXO治疗组的神经功能恢复高于MCAO组,差异有统计学意义(P<0.05)。免疫荧光染色显示标记外泌体可以进入IP区域神经细胞,荧光定量PCR及Western blot检测显示MSCs-EXO治疗组及MCAO组中PTEN水平均较正常升高,但MSCs-EXO治疗组的PTEN水平低于MCAO组,差异有统计学意义(P<0.05)。结论MSCs-EXO能够促进缺血性脑卒中大鼠的神经功能恢复,这可能与其下调IP区域PTEN表达水平相关。

术前血清碱性磷酸酶、骨桥蛋白与基底节区脑出血患者神经内镜清除术预后的关系

目的分析术前血清碱性磷酸酶(ALP)与骨桥蛋白(OPN)与基底节区脑出血患者神经内镜清除术预后的关系,评估其对患者预后的预测价值。方法回顾性采集2019年1月至2023年6月于商丘市第一人民医院完成神经内镜下微创血肿清除术治疗的65例基底节区脑出血患者的资料。记录研究所需实验室指标结果数据,包括术前及术后血清ALP、OPN水平,统计术后1个月患者预后情况,分析脑出血患者术前血清ALP、OPN与预后的关系。结果65例基底节区脑出血患者预后不良14例,占比21.54%。术前及术后,预后不良组患者血清ALP、OPN高于预后良好组(P<0.05)。经过点二列相关性分析,术前血清ALP、OPN与脑出血患者预后不良呈正相关关系(r>0,P<0.05)。绘制受试者工作特征(ROC)曲线,结果显示,术前血清ALP、OPN预测脑出血患者预后不良的曲线下面积(AUC)均>0.70,联合预测的AUC>0.80,联合预测价值更高。结论基底节区脑出血患者神经内镜清除术前ALP、OPN越高,预后不良的可能性越大,术前ALP、OPN可以作为基底节区脑出血患者神经内镜清除术后预后不良的有效预测指标。

红景天苷对类风湿关节炎患者血清脯氨酸羟化酶2及蛋白磷酸酯酶2A和丝裂原活化蛋白激酶表达水平的影响

目的分析红景天苷对类风湿关节炎(RA)患者血清脯氨酸羟化酶2(PHD2)及蛋白磷酸酯酶2A(PP2A)和丝裂原活化蛋白激酶(MAPK)表达水平的影响。方法选取青海省中医院2022年12月至2023年7月收治的RA患者96例。采用随机数字表法分为对照组和观察组,各48例。对照组采用常规西医治疗,观察组在常规西医治疗的同时予以红景天苷治疗,2组均治疗3个月。比较治疗前后2组中医证候评分、临床症状与体征、实验室检查指标[包括红细胞沉降率(ESR)、C反应蛋白(CRP)、类风湿因子(RF)、抗环瓜氨酸肽抗体(anti-CCP)]、临床疗效,健康状况评定量表(HAQ)与28个关节疾病活动度评估(DAS28)评分,血清PHD2、PP2A、MAPK水平与基因表达,不良反应。结果治疗后2组主症、次症评分均低于治疗前且观察组均低于对照组(均P<0.05)。治疗后观察组临床症状与体征均轻于对照组,ESR、CRP、RF和anti-CCP水平均低于对照组(均P<0.05)。观察组总有效率高于对照组[95.8%(46/48)比80.4%(37/46)](P=0.020)。治疗后观察组HAQ与DAS28评分均低于对照组[(5.0±1.0)分比(7.2±1.2)分、(3.1±0.5)分比(4.1±0.7)分](t=9.528、7.444,均P<0.001)。治疗后观察组PHD2、MAPK水平及基因表达均低于对照组,PP2A水平及基因表达均高于对照组,差异均有统计学意义(均P<0.05)。2组不良反应发生率差异无统计学意义(P=0.528)。结论红景天苷治疗RA可增强临床效果、减轻患者症状、改善实验室指标且安全。推测与降低PHD2和MAPK表达、增加PP2A表达有关。

阿仑磷酸钠辅助PVP治疗对老年骨质疏松性压缩性骨折BALP、PTH及N-MID-OT水平的影响

目的分析阿仑磷酸钠辅助经皮椎体成形术(PVP)治疗对老年骨质疏松性压缩性骨折骨碱性磷酸酶(BALP)、甲状旁腺激素(PTH)及N端中段骨钙素(N-MID-OT)水平的影响。方法选取2019年1月至2022年2月唐山市丰润区人民医院收治的老年骨质疏松性压缩性骨折患者107例,按照治疗方式不同分为观察组和对照组,对照组采取PVP治疗(n=52),观察组采取阿仑磷酸钠辅助PVP治疗(n=55)。对比两组Oswestry功能障碍指数问卷表(ODI)、视觉模拟量表(VAS)、骨代谢指标(BALP、PTH、N-MID-OT水平)、不良反应及再骨折发生率。结果两组术后2个月、6个月、12个月ODI评分均下降,且观察组术后各时间段ODI评分均低于对照组,差异有统计学意义(P<0.05)。两组术后2个月、6个月、12个月VAS评分均下降,且观察组术后各时间段VAS评分均低于对照组,差异有统计学意义(P<0.05)。两组术后BALP、PTH及N-MID-OT水平均下降,且观察组术后BALP、PTH及N-MID-OT水平均低于对照组,差异有统计学意义(P<0.05)。两组不良反应总发生率对比,差异无统计学意义(P>0.05),但观察组再骨折发生率(7.28%)明显低于对照组(25.00%),差异有统计学意义(P<0.05)。结论阿仑磷酸钠辅助PVP治疗可有效改善老年骨质疏松性压缩性骨折患者椎体功能,减轻其疼痛程度,改善患者体内BALP、PTH及N-MID-OT水平,促进其术后恢复。