Prevalence of Anti-Cardiolipin and Anti-β2 Glycoprotein Antibodies in Indian Systemic Lupus Erythematosus Patients

Anti-phospholipid antibodies (APA) like anti-cardiolipin antibodies (ACA) and anti-β2glycoprotien (anti-β2GP) are important cause of venous and arterial thrombosis and other occlusive vascular diseases. The prevalence of these antibodies in SLE patients at the time of diagnosis is not known in Indian SLE patients. This study was conducted to evaluate the prevalence of ACA and anti-β2GP autoantibodies in SLE patients and to correlate them with disease activity and immune parameters such as C3, C4 and CRP levels. where 85 SLE patients referred from Rheumatology Department, KEM hospital, Mumbai were studied. SLE disease activity was evaluated by SLE Disease Activity Index (SLEDAI) score at the time of evaluation. All patients studied were in an active stage of disease of which 37.6% patients had renal disorders, which were categorized as Lupus Nephritis (LN) and 62.3% patients did not show any renal manifestations (non-LN). ACA and anti-β2GP autoantibodies, to IgG and IgM subclasses were tested by ELISA. C3, C4 and CRP levels were detected by nephelometer. It was observed that 12.9% patients were IgG-ACA and IgM-ACA positive and ACA positivity was noted more among LN group Anti-β2GP autoantibody positivity was 27.1% for IgG and 31.8% for IgM., IgG-anti-β2GP antibodies were slightly higher in non-LN patients, whereas a higher incidence of IgM-anti-β2GP antibodies were detected in LN patients. Hence detection both ACA and anti-β2GP antibodies along with associated immune parameters were helpful to evaluate their possible association with disease severity in SLE patients. A long term follow up of patients having ACA and anti-β2GP antibodies without thrombotic event is also needed to detect their possible thrombotic event in future along with their clinical presentation.

血清anti-β2GPI、FSTL1、PD-1对系统性红斑狼疮免疫功能、疾病活动度的影响

目的探究血清抗β2糖蛋白I抗体(anti-β2GPI)、卵泡抑素样蛋白(FSTL1)、程序性死亡受体1(PD-1)对系统性红斑狼疮(SLE)患者免疫功能、疾病活动度的影响。方法选取我院2019年1月~2022年6月SLE患者113例作为观察组,另选取同期健康体检者105例作为对照组。比较两组、不同疾病活动度患者血清anti-β2GPI、FSTL1、PD-1水平,评价各血清指标与疾病活动度的关系,并根据观察组血清表达水平分为高表达者、低表达者,对比两者免疫功能(CD4+、CD8+、CD4+/CD8+),分析各血清指标与免疫功能相关性。结果观察组血清anti-β2GPI、FSTL1、PD-1高于对照组(P<0.05);血清anti-β2GPI、FSTL1、PD-1高表达患者CD4+、CD4+/CD8+低于低表达患者,CD8+高于低表达患者(P<0.05);血清anti-β2GPI、FSTL1、PD-1与CD4+、CD4+/CD8+呈负相关,与CD8+呈正相关(P<0.05);血清anti-β2GPI、FSTL1、PD-1水平随疾病活动度增加呈升高趋势,且重度活动患者>中度活动患者>轻度活动患者>病情稳定患者(P<0.05);血清anti-β2GPI、FSTL1、PD-1与疾病活动度显著相关(P<0.05)。结论血清anti-β2GPI、FSTL1、PD-1高表达可能参与SLE患者细胞免疫功能紊乱、疾病活动度加重的发生过程。

CLINICAL SIGNIFICANCE OF DETECTING SERUM ANTIBODIES TO NUCLEOPROTEIN AND GLYCOPROTEIN G_2 OF HANTAAN VIRUS IN PATIENTS WITH HEMORRHAGIC FEVER WITH RENAL SYNDROME

Antibody blocking enzyme linked immunosorbent assays, respectively detecting antibodies to Hantaan virus nucleoprotein (NPAb) and glycoprotein GZ (G,Ab), were developed using monoclonal antibody L133, L13r3, LV48A and LVZB28B NPAb and GZAb in 291 serum samples from 65 patientswith kemorrkagic fever with renal syudrome (HFRS) were detfrmlned by these methods. The positive rates or NPAb were 90N on day 2-3 and 100 % on day 8-9 arter onset of disease, respectively.NPAb titers Increased during fever period and reached Peak levels during kypotensive and oliguric periods of HFRS. It was suggested that NPAb might be an important component Involved in the immunopathogenlc lin'alrmeut of HFRS and the detection of NPAb might be useful for the early diagnosis or HFRS. The I,osltlve rates and titers of GZAh were very low during the rirst three periods,namely rever, hypoteuslve and ollgurlc periods, and reached high levels during the convalescent period. GRAb titers were negatively related to the I,rotelnurla levels during the course of HFRS. It wasIndicated that GZAb might be the main component or neutralizing autlhodles to Hantaan virus Infection and the efrlclent production or GZAb was a good marker ror predicting the recovery and betterprognosis of HFRS.

Role of M₃Muscarinic Acethylcholine Receptor Antibodies as a New Marker in Primary Sjögren Syndrome

Aims: This paper investigates the presence of M3 muscarinic acetylcholine receptor autoantibody present in the serum of patients with primary Sj?gren syndrome (pSS). Main methods: We detected the levels of M3mAChR peptide IgG, PGE2, IL-1β in serum of SS patients using the enzyme-linked immune sorbent assay (ELISA). To measure the quantity of nitrite/nitrate, we used Griess reagent system. Key findings: Titres of M3mAChR antibody in sera from SS patients are significantly enhanced compared to healthy subjects (control). The enhancement of these autoantibodies is accompanied by the increase of the levels of PGE2, IL-1β and nitrite/nitrate in serum. Under in vitro conditions, the synthetic human M3 peptide impaires the increment of M3mAChR antibody but not that of nati-Ro/SSA antibody. In positive anti-Ro/SSA antibody patients, the increment of M3mAChR peptide IgG and the measured pro-inflammatory substances is related. Significance: On this basis, anti M3mAChR peptide IgG can be said to act as a modulator of the immune system and to play a role in the host-chronic increment of proinflammatory substances in SS patients with positive Ro/SSA antibody. This association between the antibody and the pathogenesis of SS disease may result in useful predicting SS.

Inhibitory Effect of Anti-HER-2 Anti-CD3 Bi-specific Antibody on the Growth of Gastric Carcinoma

To evaluate the effect of anti-HER-2 × anti-CD3 bi-specific antibody（BsAb） on the growth of HER-2/neu-expressing human gastric carcinoma in vitro and in vivo, an MTT assay was carried out to test the inhibitive rates of herceptin, anti-CD3 and BsAb antibodies on SGC-7901 gastric carcinoma cells. Immunocytochemistry methods were used to test the HER-2 level of SGC-7901. Nude mice models were employed to test the effect of HER-2 CD3 BsAh combined with effector ceils（ peripheral blood lymphatic cells of healthy human beings） on the growth of tumors in animals. Compared with that of the untreated control group, the tumor cell growth rates in vitro and in vivo will both be significantly inhibited when treated with effector cells combined with anti-CD3 McAb, herceptin or HER2 CD3 BsAb （p 〈0. 05）, and the growth inhibition is the most remarkable in the group treated with HER2 CD3 BsAb combined with effector cells. The growth of tumor xenografts will also be significantly inhibited in the group treated with HER2 CD3 BsAb combined with effector cells when compared with that in the group treated with anti-CD3 McAb or the group treated with herceptin combined with effector cells（p 〈0. 05）. We can conclude that HER-2/neu is possibly a useful target for immunotherapy of gastric carcinoma, and anti-HER2 × anti-CD3 BsAb has evident anti-tumor efficacy both, in vitro and in vivo.

Molecular Docking Study of the Binding Interaction of Hydroxychloroquine, Dexamethasone and Other Anti-Inflammatory Drugs with SARS-CoV-2 Protease and SARS-CoV-2 Spikes Glycoprotein

Aims: The outbreak of the novel coronavirus disease 2019 (COVID-19), caused by severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), is still accountable for millions of deaths worldwide and declared as a global pandemic by the World Health Organisation. Despite efforts, there is still limited evidence available on a successful potent inhibitor with a low toxicity profile that can aid in the prevention and/or treatment of COVID-19. This study will focus on four main aspects: 1) screening 19 Food Drug and Administration (FDA) approved drugs using computational molecular docking;2) assessing drug toxicity profiles using biological data;3) recommending potential therapies against COVID-19 and 4) supplementing currently used therapies. Methods: 19 FDA approved drugs were investigated against the crystal structure of SARS-CoV-2 protease (6LU7) and SARS-CoV-2 glycoprotein (6VXX) using a computational molecular docking software, Molecular Operating Environment (MOE). Separately, on MOE, 6LU7 and 6VXX were loaded, prepared, and the binding pockets located. The drug’s canonical SMILES were imported, minimised, and docked on the prepared proteins using a search algorithm to establish the highest stability conformation. Drugs were ranked depending on binding properties and biological data to assess safety;steric clashes and voids in the binding site were also analysed. Results and discussion: Out of the nineteen (19) FDA approved drugs, 18 inhibited 6LU7 and 13 inhibited 6VXX. High-ranked drugs based on binding properties for 6LU7 were hydroxychloroquine, dexamethasone, naproxen, etoricoxib, and ibuprofen. For 6VXX were hydroxychloroquine, celecoxib, etoricoxib, meloxicam, and parecoxib. Considering safety profile, the top 3 drugs in descending order for 6LU7 were etoricoxib, naproxen and dexamethasone and for 6VXX were etoricoxib, meloxicam, and parecoxib. Compared to the literature, the results were consistent for dexamethasone which was effective against 6LU7. However, for hydroxychloroquine and ibuprofen, there was conflicting literature regarding safety and efficacy. Conclusion and future work: The findings suggest that against COVID-19 etoricoxib might be effective as a therapeutic and prophylactic measure. Naproxen and dexamethasone would be more effective as treatment only while meloxicam and parecoxib as prophylaxis. However, future studies are needed to validate these findings. Compared to previous literature, the findings in this study also support the use of dexamethasone over hydroxychloroquine and ibuprofen for COVID-19 based on the binding and safety properties. Despite this, future research should explore the impressive binding properties displayed by hydroxychloroquine and ibuprofen to aid in developing a new drug against COVID-19.

隐丹参酮对ACA、Anti-β_2-GP_1阳性大鼠抗体水平及TLR4/NF-_κB信号通路影响的研究

目的研究隐丹参酮对抗心磷脂抗体(ACA)、抗β2糖蛋白1抗体(anti-β2-GP1)阳性模型SD大鼠抗体水平及TLR4/NF-κB信号通路的影响。方法将SD雌性大鼠随机分为6组,即隐丹参酮组(0.03μg/g)、丹参注射液组(6μl/g)、阿司匹林组(0.04μg/g)、水溶剂组(与隐丹参酮组相同体积吐温80与0.9%Na Cl溶液的混合液)、模型组(与隐丹参酮组相同体积0.9%Na Cl溶液)、空白组(与隐丹参酮组相同体积0.9%Na Cl溶液)。采用腹腔注射地塞米松注射液及盐酸肾上腺素注射液造模,共16日。于造模完成后第1天开始灌胃给药,连续2周。造模完成后及灌胃结束后采血,采酶联免疫吸附法(ELISA法)检测血清中ACA、Anti-β2-GP1水平,再将雌雄大鼠合笼,受孕的第12天将大鼠处死。用ELISA法检测血清中肿瘤坏死因子α(TNF-α)的水平并计算活胎数。取大鼠子宫蜕膜组织,采用免疫组化链霉菌抗生物素蛋白-过氧化物酶连结法(SP)法测定Toll样受体4(TLR4)蛋白的表达水平。结果 1隐丹参酮可以有效降低血清中ACA、Anti-β2-GP1的水平,提高大鼠活胎数。2隐丹参酮可以使大鼠子宫蜕膜细胞内TLR4的表达水平降低,从而降低血清中TNF-α水平,降低妊娠风险。结论隐丹参酮可有效降低ACA、Anti-β2-GP1阳性大鼠的流产率,其机制可能与抑制TLR4/NF-κB信号通路有关。

老年脑梗死患者血清ACA、抗β2GP1、Hcy和hs-CRP水平变化及其与疾病严重程度的关系

目的:探讨老年脑梗死患者血清抗心磷脂抗体(ACA)、抗β2糖蛋白1抗体(抗β2GP1)、同型半胱氨酸(Hcy)和超敏C反应蛋白(hs-CRP)水平变化及其与疾病严重程度的关系。方法:选取148例老年脑梗死患者为观察组,根据神经功能缺损(NDS)评分分为轻度组(n=30)、中度组(n=32)及重度组(n=86);另选同期76名体检健康老年人为对照组。比较观察组和对照组及观察组不同病情程度患者的血清ACA、抗β2GP1、Hcy、hs-CRP水平,分析其与疾病严重程度的关系。结果:观察组患者血清ACA、抗β2GP1、Hcy、hs-CRP水平高于对照组(P<0.05)。不同病情程度脑梗死患者血清ACA、抗β2GP1、Hcy、hs-CRP水平比较:重度组>中度组>轻度组(P<0.05)。相关性分析显示,血清ACA、抗β2GP1、Hcy、hs-CRP水平与老年脑梗死患者病情严重程度均呈正相关关系(r=0.636、0.614、0.563、0.571,P<0.05)。ROC曲线分析显示,血清ACA对轻中度与重度的区分有更高的鉴别价值(P<0.05),敏感度和特异性分别为90.70%、87.10%。结论:老年脑梗死患者血清ACA、抗β2GP1、Hcy、hs-CRP水平均升高,且与病情严重程度正相关,可作为鉴别脑梗死严重程度的有效指标。

孕早期阴道超声s-Flow检查联合血清ACA及anti-β2GPI评估先兆流产患者不良妊娠结局价值

目的:探讨孕早期行阴道双向能量多勒普技术(s-Flow)联合血清抗心磷脂抗体(ACA)及抗β2-糖蛋白Ⅰ(anti-β2GPI)检查预测先兆流产患者不良妊娠结局价值。方法:收集本院妇产科2018年6月-2020年6月收治的320例先兆流产孕妇临床资料,检测超声血流分型、血清ACA、anti-β2GPI水平,根据妊娠结果分为正常组(n=241例)和不良组(n=79例)。采取logistic回归分析影响不良妊娠结局的因素,受试者工作特征(ROC)曲线评估上述指标的预测价值。结果:两组血流信号分级比较有差异(P<0.05),不良组血清ACA、anti-β2GPI水平高于正常组(P<0.05)。logistic回归分析,阴道s-Flow技术血流信号分级、血清ACA、anti-β2GPI均为不良妊娠结局发生的独立危险因素(P<0.05)。评估不良妊娠结局的曲下面积阴道s-Flow技术血流信号分级0.578;血清ACA截断值>3.87 mIU/ml时曲下面积0.787,anti-β2GPI截断值>7.29 U/ml时曲下面积为0.745,以阴道s-Flow技术血流信号分级、ACA、anti-β2GPI联合预测不良妊娠结局的曲下面积0.881,敏感度81.0%、特异度79.3%。结论:孕早期行阴道s-Flow技术联合血清ACA及antiβ2GPI抗体检测对评估妊娠结局有较好效能。

Elevated pancreatic enzymes, IgM, soluble interleukin-2 receptor in anti-GADab(+) type 1 diabetes

Type 1 diabetes can be classified into immune-mediated diabetes (type 1A) and idiopathic diabetes, which lacks immunological evidence for beta cell autoimmunity (type 1B). Type 1A diabetes is characterized by the presence of the anti-glutamic acid decarboxylase antibody (anti-GADab). Fulminant type 1 diabetes is classified as type 1B diabetes, and characterized by the absence of anti-GADab, flu-like symptoms, and elevated serum exocrine pancreatic enzymes. We report a type 1 diabetic patient who showed flu-like symptoms, elevated serum exocrine pancreatic enzymes, and an extremely high-titer of anti-GADab, manifesting the characteristics of both type 1A and fulminant type 1 diabetes.

血清抗糖蛋白210抗体阳性的原发性胆汁性胆管炎患者临床特征分析

目的总结血清抗糖蛋白210(抗gp210)抗体阳性的原发性胆汁性胆管炎(PBC)患者临床特征。方法2017年1月~2021年1月我院诊治的PBC患者63例,其中血清抗gp210抗体阳性患者21例(观察组),血清抗线粒体抗体(AMA)或AMA-M2阳性42例(对照组)。给予所有患者熊去氧胆酸(UDCA)13~15 mg·kg^(-1) d^(-1)治疗6个月。采用ELISA法检测血清白细胞介素-2(IL-2)、IL-6和IL-10水平,采用免疫比浊法检测血清IgA、IgG和IgM。结果观察组年龄和性别与对照组比差异均无统计学意义(P>0.05),但观察组乏力发生率为47.6%,显著高于对照组的35.7%(P<0.05);治疗前,观察组血清总胆红素(TBIL)、ALT和AST水平分别为30.1(18.5,66.1)μmol/L、73(42,110)U/L和87(64,126)U/L,均显著高于对照组【分别为20.1(10.4,31.5)μmol/L、53(27,90)U/L和68(53,101)U/L,P<0.05】,而血清白蛋白水平为32.2(29.8,35.2)g/L,显著低于对照组【34.6(30.4,36.8)g/L,P<0.05】;在治疗6个月后,观察组血清白蛋白水平为37.8(35.4,38.5)g/L,仍显著低于对照组【42.3(37.4,45.1)g/L,P<0.05】;治疗前,观察组血清IL-6和IL-10水平分别为12.7(5.8,11.3)pg/ml和125.1(87.4,120.6)pg/ml,均显著高于对照组【分别为9.1(7.0,11.7)pg/ml和103.6(90.1,117.0)pg/ml,P<0.05】;在治疗后,观察组血清IL-2和IL-6水平分别为29.1(18.4,36.5)pg/ml和7.2(5.2,8.5)pg/ml,均显著高于对照组【分别为21.0(9.7,26.3)pg/ml和5.4(4.0,6.9)pg/ml,P<0.05】,而血清IL-10水平为139.5(107.6,152.9)pg/ml,也显著低于对照组【154.8(122.7,168.2)pg/ml,P<0.05】;治疗后,观察组血清IgM、IgG和IgA水平分别为3.1(2.5,3.7)g/L、13.7(12.0,14.6)g/L和3.8(2.9,3.8)g/L,均显著高于对照组【分别为2.2(1.9,2.6)g/L、11.2(10.1,13.4)g/L和2.8(2.5,3.3)g/L,P<0.05】。结论血清抗gp210抗体阳性的PBC患者病情似乎更趋严重,对UDCA治疗应答稍差,值得临床扩大观察和研究。

Autoantibodies against myelin antigens in patients with neuromyelitis optica

In this study, we investigated the clinical relevance of anti-myelin antibodies in patients with neuromyelitis optica (NMO);titers of antibodies against myelin oligodendrocyte glycoproteins, proteolipid proteins and myelin basic proteins were measured in the sera of patients with NMO and compared to healthy controls, as well as to patients with other diseases. The frequency of presence of anti-myelin antibodies in patients with NMO was significantly higher than that in healthy and diseased controls. The expanded disability status scale scores correlated with the titers of the anti-myelin antibodies. Patients with anti-myelin antibody exhibited other autoantibodies significantly more frequently than patients without the antibody. Anti-myelin antibodies may be useful markers for predicting severe clinical courses in patients with NMO.

Waning of Anti-Spike IgG Antibody Titer after COVID-19 Vaccination: Myth or Reality?

This observational prospective study was conducted on 25 patients who had received a full 3-dose COVID-19 vaccination scheme with a follow-up ranging from 12 to 19 months after the last injection. The aim of the study was focused on a single biological indicator the anti-spike IgG antibody titer. The age of the patients ranged from 51 to 85 years old. 15 out 25 patients (60%) presented a comorbidity. Our data showed a persistent positive anti-spike IgG antibodies titer ranging from 105 to 5680 BAU/mL (mean: 2661 BAU/mL) in all patients. In view of these results, systematic administration of a SARS-CoV-2 vaccine booster is questionable and should be individually tailored according to the patient medical condition and the anti-spike IgG antibody level.

Role of C-Peptide in Relation to Levels of Anti-GAD and Islet Cell Antibodies in Characterizing Types of Diabetes in the Young, in Eastern India

Background: Measuring fasting C-peptide (FCP) and antibodies against Glutamic acid decarboxylase (GADA) and Islet cell antibodies (ICA) are not so commonly explored in children and young adults. Objectives: To assess the levels of FCP, GADA and ICA in subjects below the age of 25 years with DM and compare their levels to differentiate between Autoimmune and Non-Autoimmune Type 1 DM. Methodology: Blood samples of 93 subjects diagnosed with DM, reporting to the tertiary care hospital, were analysed for ICA, GADA and FCP. Receiver operating characteristics (ROC) curves were analysed to check the ability of autoimmune markers, BMI and C-peptide to differentiate between Autoimmune (Ai) and Non-Autoimmune (NonAi) diabetes. Results: 30/93 (32.2%) were positive for anti-GAD ab and/or ICA and categorised as Autoimmune (Ai), the most common antibody being, anti-GAD ab (80%) in them. The level of FCP among Ai compared to NonAi, was significantly low (p 20.75 nmol/l) as a very dependable test for diagnosing Ai, Type 1 DM, in children and young adults. Its sensitivity and specificity are in the range of 86.2% and 96.8% respectively. Low level of C-peptide (Conclusion: This study revealed predominant positivity for anti-GAD ab (80%) among Ai+ patients. ROC analysis shows GADA above 20.75 nmol/l and Fasting C-peptide < 0.36 nmol/l as a good indicator for diagnosing Ai in children and young adults.

tau蛋白、胶质纤维状酸性蛋白及抗β2糖蛋白1抗体水平与高血压脑出血患者预后的相关性分析

目的分析tau蛋白、胶质纤维状酸性蛋白(glial fibrillary acidic protein,GFAP)以及抗β2糖蛋白1抗体(anti-β2 glycoprotein 1 antibody,aβ2-GP1)水平与高血压脑出血(hypertensive intracerebral hemorrhage,HICH)患者预后的相关性。方法将70例HICH患者纳入研究组,另将同时期进行健康体检的70例人员纳入对照组。比较两组tau蛋白、GFAP以及aβ2-GP1水平。比较不同预后HICH患者tau蛋白、GFAP、aβ2-GP1水平和美国国立卫生院卒中量表(National Institute of Health Stroke Scale,NIHSS)评分;并分析HICH患者相关指标与NIHSS评分的相关性。使用受试者工作特征(receiver operation characteristic,ROC)曲线分析相关指标预测HICH患者不良预后的临床价值。结果与对照组比较,观察组tau蛋白、GFAP以及aβ2-GP1水平均较高(P<0.05)。预后不良的HICH患者tau蛋白、GFAP、aβ2-GP1水平和NIHSS评分均较高(P<0.05);相关指标与NIHSS评分均呈正相关(均P<0.05)。相关指标预测HICH患者预后不良的最佳临界值:tau蛋白≥258.15ng/L、GFAP≥16.15ng/L、aβ2-GP1≥18.35 RU/mL,此时ROC曲线下面积(area under the curve,AUC)为0.908(95%CI:0.828~0.988,P<0.05)、0.871(95%CI:0.781~0.961,P<0.05)、0.839(95%CI:0.728~0.949,P<0.05),敏感度为77.27%、77.27%、72.73%,特异度为97.92%、85.42%、89.58%。结论HICH患者tau蛋白、GFAP以及aβ2-GP1水平较高,神经损伤较重、预后不良的HICH患者相关指标更高,监测HICH患者tau蛋白、GFAP以及aβ2-GP1水平可用于不良预后的评估。

IL-2/抗IL-2抗体通过增加中枢神经系统内调节性T细胞数量减轻小鼠颅脑创伤

目的探讨IL-2/抗IL-2抗体增加颅脑创伤(TBI)小鼠中枢神经系统内调节性T细胞(Treg)数量对小鼠TBI的影响。方法所用动物为10周龄C57BL/6健康雄性小鼠,分为Sham组、TBI组、TBI+IL-2/抗IL-2抗体组。TBI+IL-2/抗IL-2抗体组在造模2 h后连续3 d给予IL-2(1.0μg)+抗IL-2抗体(5.0μg)腹腔注射。提取三组小鼠在3、5、7 d的脑组织进行流式细胞术,检测Treg数量,同时将第7日小鼠脑组织进行免疫荧光染色,以明确TBI后中枢神经系统存在Treg浸润,另外对三组小鼠1、3、5、7 d的行为学结果分别进行分析。同时检测造模第7日各组小鼠脑组织含水量、神经元凋亡及炎症因子表达情况。结果与Sham组相比,TBI组及TBI+IL-2/抗IL-2抗体组小鼠中枢神经系统内确实存在Treg浸润情况,且Treg在脑创伤后逐渐增多,Sham组未见Treg浸润,TBI+IL-2/抗IL-2抗体组相较于TBI组Treg明显增多(P<0.05),包括神经元凋亡减少、脑水肿减轻及炎症因子表达降低,预后明显改善。结论IL-2/抗IL-2抗体可以增加中枢神经系统内Treg的数量并在一定程度上能够减轻小鼠TBI症状。

25例儿童抗髓鞘少突胶质细胞糖蛋白免疫球蛋白G抗体相关疾病药学服务的切入点探讨

目的:探讨临床药师对抗髓鞘少突胶质细胞糖蛋白免疫球蛋白G抗体相关疾病(MOGAD)药学监护的切入点、侧重点,为临床药学实践工作提供参考。方法:临床药师以2021-2022年在我院治疗的25例MOGAD患儿为研究对象,深入开展个体化药学服务,设置重点监护患儿,评估疗效并调整治疗方案,监测药品不良反应,关注药物相互作用。结果:25例患儿中,男12例,年龄(6.3±3.0)岁,体质量21.0(18.0,33.3)kg;女13例,年龄(7.7±3.3)岁,体质量25.0(17.9,33.9)kg。所有患儿均符合糖皮质激素治疗指征,7例患儿发生了不良反应,5例(20.0%)高眼压,1例(4.0%)肝酶异常,1例(4.0%)呕吐,总体不良反应发生率为28.0%。2例复发患儿加用免疫抑制剂治疗,1例患儿药物治疗存在相互作用。结论:临床药师作为多学科治疗团队中的一员,全程参与药物治疗管理,主动为患者提供药学监护服务,有助于促进合理用药,体现了药师工作价值。

血清hs-CRP、sCD40L、β_(2)GP1、ACA与急性脑梗死病情严重程度及预后的相关性

目的分析血清hs-CRP、sCD40L、β_(2)GP1、ACA与ACI患者病情严重程度及预后的相关性。方法采取回顾性研究,选择2021年6月至2023年6月医院收治的130例ACI患者临床资料作为研究对象。患者均接受阿替普酶静脉溶栓治疗,根据美国国立卫生研究院卒中量表评分(NIHSS)评估患者病情严重程度,将评分<16分患者临床资料纳入轻中组,将评分≥16分患者临床资料纳入重度组;治疗2周后,参照改良Rankin量表评分(mRS)评估患者预后,将评分<3分患者临床资料纳入预后良好组,将评分≥3分患者临床资料纳入预后不良组;统计患者基线资料,采用双变量相关性Pearson(N)分析,ACI患者血清hs-CRP、sCD40L、β_(2)GP1、ACA水平与认知功能的相关;采用二元Logistic回归分析血清hs-CRP、sCD40L、β_(2)GP1、ACA与急性脑梗死病情严重程度及预后的相关性;采用接受者操作特性曲线(ROC)分析血清hs-CRP、sCD40L、β_(2)GP1、ACA水平对ACI患者预后不良的预测价值。结果治疗后,ACI患者Fib、D-D低于治疗前(P<0.05);治疗后,ACI患者hs-CRP、sCD40L、β_(2)GP1、ACA低于治疗前(P<0.05);ACI患者治疗前的MoCA评分分低于治疗后(P<0.001);Pearson(N)分析结果显示,ACI患者血清hs-CRP、sCD40L、β_(2)GP1、ACA水平与MoCA评分呈负相关(r<0,P<0.05);重度组TOAST分型为心源性栓塞患者占比高于轻中度组,Fib、D-D、hs-CRP、sCD40L、β_(2)GP1、ACA水平高于轻中度组(P<0.05);二元Logistic回归分析结果显示,TOAST分型为心源性栓塞、其他原因/不明原因,血清Fib、D-D、hs-CRP、sCD40L、β_(2)GP1、ACA高表达是ACI患者病情为重度的危险因素(OR>1,P<0.05);预后不良组TOAST分型为心源性栓塞患者占比高于预后良好组,发病至溶栓时间长于预后良好组,Fib、D-D、hs-CRP、sCD40L、β_(2)GP1、ACA水平高于预后良好组(P<0.05);二元Logistic回归分析结果显示,TOAST分型为心源性栓塞,发病至溶栓时间长、血清Fib、D-D、hs-CRP、sCD40L、β_(2)GP1、ACA高表达是ACI患者预后不良的危险因素(OR>1,P<0.05);绘制ROC曲线结果显示,血清hs-CRP、sCD40L、β_(2)GP1、ACA水平及联合检测ACI患者预后不良的ACU均>0.70,有一定预测价值,其中联合检测最高。结论TOAST分型、血清Fib、D-D、hs-CRP、sCD40L、β_(2)GP1、ACA水平与ACI患者病情严重程度相关,同时在此基础上发病至溶栓时间与ACI患者预后关系密切。

抗心磷脂抗体及抗β2糖蛋白1抗体检测血脂正常脑梗死患者的临床意义

目的研究抗心磷脂抗体(ACA)及抗β2糖蛋白1抗体(anti-β2-GP1)在脑梗死患者中的表达及其临床意义。方法选取确诊的脑梗死患者211例,按照是否合并高脂血症,分为血脂正常脑梗死组(n=121)和高脂血症合并脑梗死组(n=90)。采用酶联免疫吸附测定(ELISA)对两组患者血清IgA、IgG、IgM型ACA和anti-β2-GP1进行测定并比较两组阳性率的差异;同时比较不同年龄、性别、病灶数量的血脂正常脑梗死组患者ACA和anti-β2-GP1阳性率差异及脑梗死患者两类抗体之间的相关性。结果血脂正常脑梗死组和高脂血症合并脑梗死组的ACA阳性率分别为14.0%和4.4%(χ~2=4.295,P=0.038),anti-β2-GP1阳性率分别为17.4%和5.6%(χ~2=6.651,P=0.010)。血脂正常脑梗死组患者中,90例单发性脑梗死和31例多发性脑梗死患者的ACA阳性率分别为8.9%和29.0%(χ~2=7.748,P=0.005),anti-β2-GP1阳性率分别为10.0%和38.7%(χ~2=13.250,P=0.000);在血脂正常脑梗死组患者中,≤50岁67例,>50岁54例,ACA阳性率分别为20.9%和5.6%(χ~2=4.626,P=0.031),anti-β2-GP1阳性率分别为25.4%和7.4%(χ~2=5.534,P=0.019);ACA和anti-β2-GP1阳性率在性别上差异无统计学意义(P>0.05);一致性χ~2检验显示211例脑梗死患者ACA和anti-β2-GP1有相关性(P<0.05)。结论 ACA及anti-β2-GP1可能是血脂正常中青年脑梗死患者的重要发病原因之一,临床应加强对这类人群ACA及anti-β2-GP1的联合检测。

抗IgG、IgM、IgA型心磷脂抗体和抗β_2糖蛋白1抗体在系统性红斑狼疮患者中的意义

目的探讨抗IgG、IgM、IgA型心磷脂抗体和抗β2糖蛋白1抗体在系统性红斑狼疮(systemic lupus erythematosus,SLE)患者中的意义。方法分别采用化学发光免疫分析法和酶联免疫吸附法检测372例SLE患者、80例其他结缔组织病患者及60例健康体检者血清中抗IgG、IgM、IgA型心磷脂抗体和抗β2糖蛋白1抗体。同时分析这4个指标与SLE及其病情严重程度的相关性。结果在检测的372例SLE患者组中,抗IgG、IgM、IgA型心磷脂抗体和抗β2糖蛋白1抗体的阳性率分别为31.45%、14.52%、10.22%和29.03%,其表达水平分别为(90.39±35.43)U/ml、(41.25±23.16)U/ml、(32.27±15.77)U/ml、(61.42±21.69)U/ml,与SLEDAI积分呈正相关(P<0.05)。在80例疾病对照组中,抗IgG、IgM、IgA型心磷脂抗体和抗β2糖蛋白1抗体的阳性率分别为7.50%、2.50%、0和1.25%。而在60例正常对照组中,4项检测结果均为阴性。抗IgG型心磷脂抗体阳性与血小板减少、白细胞减少、血栓形成、习惯性流产和肾脏病变有关;抗IgM型心磷脂抗体阳性与血小板减少、白细胞减少、血栓形成和肾脏病变有关;抗IgA型心磷脂抗体阳性与血小板减少、血栓形成和肾脏病变有关;抗β_2糖蛋白1抗体阳性与血小板减少、白细胞减少、溶血性贫血、血栓形成、习惯性流产和肾脏病变有关。结论抗IgG、IgM、IgA型心磷脂抗体和抗β_2糖蛋白1抗体在SLE的发病及病情发展中起到了非常重要的作用,定量和联合检测对SLE的诊断、病情严重程度的评价、判断预后及疗效观察等均有重要的临床意义。