Development of a Ready-to-Use PSMA-11 Kit Formulation and Biological Evaluation of Binding Affinity

Introduction: 68Ga-PSMA-11 is considered the gold standard in detection of micro and oligometastases in advanced prostate cancer, being used for therapeutic planning, as well as, potentially, for evaluating response to treatment. The development of ready-to-use lyophilized kit of PSMA-11 adds quality and safety to the routine use of this radiopharmaceutical and represents a pharmacotechnical challenge as it must preserve the integrity and specificity of the ligand. Methods: PSMA-11 kit formulation was proposed, considering radiolabeling parameters and the preservation of the peptide during the lyophilization process, using mannitol as an excipient. Critical temperature characterization studies were carried out using DSC equipment and the freeze-drying process was developed. The direct radiolabeling conditions were evaluated and standardized using 68Ge/68Ga generator eluate from two different manufacturers (ITG and Eckert & Ziegler). The radiochemical purity was evaluated by TLC and HPLC. Biological evaluation was carried out with lyophilized PSMA-11 to demonstrate the integrity of the peptide and preservation of biological activity after the lyophilization process. Results: Based on critical temperature characterization studies, the freeze-drying cycle was designed to reach a freezing temperature of around −40˚C and primary drying at 2˚C. Using 20 mg of mannitol, an intact and elegant lyophilized cake was obtained. PSMA-11 lyophilized kit was directly labeled with 68Ga eluate from 68Ge/68Ga GMP generators (ITG and Eckert & Ziegler) resulting in % RP > 95% at pH 4.0 to 4.5. The results obtained from in vitro and in vivo biological competition studies confirmed the preservation of PSMA-11 affinity for the receptor after lyophilization. Conclusion: A lyophilized formulation (Kit) of PSMA-11 was successfully obtained, which preserved the integrity and biological activity of the peptide and guaranteed radiolabeling efficiency.

基于CT影像学在预测胃肠道间质瘤KIT突变的研究进展

胃肠道间质瘤(gastrointestinal stro mal tumor,GIST)是罕见的胃肠道肿瘤,其高恶性转化率致使肿瘤容易转移至肝脏和腹膜。手术是GIST的标准治疗方法。但具有酪氨酸激酶抑制剂(tyrosine kinase inhibitors,TKIs)伊马替尼治疗敏感的KIT突变GIST患者术后复发风险高,辅助伊马替尼治疗可提高生存率。对于晚期无法手术的KIT突变GIST患者,使用TKIs中位总生存期显著提高。目前,临床上明确GIST的KIT突变常需要通过侵入性组织活检进行评估,寻求非侵入性和更快速的评估方法,有助于临床针对不同患者制定个体化治疗方案,进而降低其复发率及死亡率。现阶段,越来越多研究关注影像学检查在预测GIST的KIT突变中的潜在应用价值。此外,影像组学可以挖掘及量化肉眼无法评估的高维信息,辅助临床决策并进一步推动精准医学的发展。本文就CT影像学检查和影像组学在预测GIST KIT突变研究进展进行文献回顾及综述。

独家焦点——2025宝马XM BY KITH与2025宝马XM KITH概念车

近日,宝马(BMW)和奇思(Kith)成功合作推出新款车型。宝马XM及其与传奇车型宝马M1的联系是这家高档汽车制造商与罗尼·菲格(Ronnie Fieg)的世界知名品牌Kith第三次合作的焦点。这款高性能插电式混合动力车型将于2025年推出,其被命名为2025宝马XM by Kith,并采用独家外观和内饰设计。

基于干细胞因子/C-kit信号通路探讨鼠李糖乳酪杆菌Glory LG12的润肠通便作用

目的:基于干细胞因子(stem cell factor,SCF)/C-kit信号通路探讨鼠李糖乳酪杆菌Glory LG12的润肠通便作用。方法:雄性ICR小鼠随机分为空白组、模型组以及鼠李糖乳酪杆菌Glory LG12低剂量(1.5×10^(6)CFU/只)、中剂量(1.5×10^(7)CFU/只)和高剂量(1.5×10^(8)CFU/只)组,各组小鼠分别连续灌胃相应的药物15 d后,灌胃盐酸洛哌丁胺混悬液(4 mg/kg)建立便秘模型,测定各组小鼠的体质量、首粒黑便排出时间、5 h内黑便排出数量及质量、小肠推进率、血清中胃肠调节肽和炎性细胞因子水平及小鼠结肠组织SCF、C-kit转录水平,并观察结肠病理结构。结果:与模型组相比,中、高剂量的鼠李糖乳酪杆菌Glory LG12均能缩短小鼠的首粒黑便排出时间(P<0.001),增加小鼠5 h内排黑便的粒数和质量(P<0.01、P<0.001),提高小肠内的墨汁推进率(P<0.001);升高小鼠血清中胃动素、胃泌素、P物质和白细胞介素(interleukin,IL)10的质量浓度,降低内皮素1、生长抑素、血管活性肠肽和IL-6的质量浓度;增加结肠组织中SCF和C-kit mRNA相对表达量(P<0.01、P<0.001);修复受损结肠屏障。结论:鼠李糖乳酪杆菌Glory LG12能够通过调节SCF/C-kit通路,进而影响胃肠调节肽和炎性细胞因子的释放,发挥其促进胃肠蠕动的功能,改善便秘症状。

Ready-to-Use型药物临床应用研究进展

目的为药物剂型的研发和临床用药选择提供参考。方法检索Ready-to-Use(RTU)型药物的相关文献,总结其临床应用的优势。结果RTU型药物可与给药系统结合,无需配置即可使用。在疾病治疗方面,可缩短救治准备时间,减少延时给药风险,改善救治结局,提高患者用药的自我管理能力。在用药安全方面,可降低相关血流感染、局部感染的发生率,减少医疗事故的发生,化学、生物、辐射、核(CBRN)事件发生时减少医务人员的职业暴露。结论随着研发技术的提升,药物种类的扩展,RTU型药物将来可能逐渐取代安瓿瓶等小针剂的使用,为临床患者和医务人员带来获益与便利。

c-KIT受体蛋白在犬皮肤肥大细胞瘤中的作用及其应用

皮肤肥大细胞瘤(MCT)是犬发生率较高的皮肤肿瘤类型之一,多发于老年犬,是危害犬类健康的重要疾病之一。c-KIT受体蛋白是一种跨膜蛋白,具有酪氨酸激酶活性,可调控肥大细胞的生长和分化。本文旨在阐明c-KIT受体蛋白在犬皮肤MCT中的作用及其应用,总结了c-KIT受体蛋白在肥大细胞增殖调控中的作用,深入探讨了c-KIT受体蛋白检测在犬皮肤MCT诊断中的应用价值,明确了c-KIT受体蛋白在犬皮肤MCT发生发展中的作用,同时也为进一步研究c-KIT受体蛋白在犬皮肤MCT中的发病机制提供了重要参考。

基于转录测序技术对KIT基因在听觉色素障碍类疾病初步研究

目的 利用KITF860S突变耳聋小鼠模型研究探讨KIT基因突变导致听觉色素障碍类疾病致聋的分子机制。方法 利用稳定遗传的KITF860S小鼠模型家系,并对家系中不同表型个体进行长期听觉电生理测试、同窝不同表型小鼠病理切片、进行全基因组转录测序分析其表达差异基因。结果 该小鼠模型家系内杂合型小鼠在初期与野生型小鼠听力表型并无明显差距,在5月龄时表现为渐进性听力下降,纯合型小鼠在听力形成初期即表现为先天性中重度听力下降,10周龄时即表现为全聋表现。转录测序结果显示,以野生型小鼠为对照,氧化磷酸化通路在KIT基因纯合突变及杂合突变中均表现为下调,紧密连接通路在KIT基因不同组别比较中为不同上下调表现。结论本研究结果表明,KIT基因突变所致听觉色素障碍类疾病表现与氧化磷酸化、紧密连接等通路相关目的基因靶蛋白表达异常有一定相关性,最终导致听力损失。对KIT基因突变致病分子机制的研究对于丰富人类耳聋基因库具有重要意义,也为后续相关综合征类疾病基因治疗提供理论基础。

Effective Therapeutic Feeding with Chickpea Sesame Based Ready-To-Use Therapeutic Food (CS-RUTF) in Wasted Adults with Confirmed or Suspected AIDS

Wasting has been observed as a common feature of the human immunodeficiency virus (HIV) disease since the first reports and its presence increases the risk of death. There is no consensus on how to manage wasting associated with HIV. The goal of this study was to assess the effectiveness of a locally made Chickpea Sesame Based RUTF (CS-RUTF) in treating wasting associated with HIV in developing countries. Chronically sick adults from Mangochi Health District (Malawi) with wasting and confirmed or presumptive clinical diagnosis of HIV were recruited for the study. Subjects received a daily ration of 500 grams of CS-RUTF for 3 to 5 months. Nutrition status changes and mortality were used to assess the effectiveness of the intervention. There were 3 patterns of anthropometric responses continuous weight gain (WG), static weight (SW) and continuation weight loss (WL). The distribution of the 3 patterns is 53.9% (82/154) for the WG pattern, 9.1% (14/154) for the SW pattern and 37.0% (57/154) for the WL pattern. For the WG pattern, the overall median weight gain was 4.6 (2.4 to 7.1) kg. It was 5.7 (3.5 to 7.8) kg for those who completed 3 months of sup-plementation. MUAC and BMI changes followed similar pattern than weight change. Not being on HAART, acute diarrhoea during follow up, episode of reduced appetite during follow up, missing at least one visit were identified as risk factors for intervention failure. Overall, 38.5% (72/187) of study participants died during the intervention. In conclusion, despite that the study confirms the limited impact of food based interventions on mortality among wasted HIV positive individuals, it also suggests that supplementation with CS-RUTF may be an effective intervention for reversing wasting associated with HIV if combined with HAART and specific treatment of severe opportunistic infection causing diarrhoea and reducing appetite.

KIT杂合大片段缺失导致斑驳病一家系的临床表型

目的鉴定一个斑驳病家系的致病基因突变。方法收集斑驳病患者及其家系成员的临床资料,采集外周血,进行全外显子组测序。通过qPCR验证目的基因的缺失;采用gap-PCR结合Sanger测序法确定具体缺失的大小以及位点。结果在先证者4号染色体上存在约1.74 Mb的杂合大片段缺失突变,其中包括了全部KIT(斑驳病的致病基因)。该缺失在家系中呈基因型-表型共分离,在dbSNV数据库中未见该区域的缺失报道。该缺失是目前报道的最小的因KIT全长缺失而导致斑驳病表型的片段缺失。结论KIT缺失是导致该家系斑驳病表型的原因。

温胃阳汤对功能性消化不良大鼠肥大细胞活化及SCF/c-Kit信号通路的影响

目的:基于肥大细胞活化及干细胞因子(stem cell factor,SCF)/受体酪氨酸激酶c-Kit信号通路探讨温胃阳汤治疗大鼠功能性消化不良的作用机制。方法:将60只SD大鼠随机分为空白组,模型组,雷尼替丁组及温胃阳汤低、中、高剂量组,每组10只。空白组大鼠不予造模,其他各组采用夹尾刺激加不规则喂养复合番泻叶法建立大鼠功能性消化不良模型,模型建立后,空白组及模型组灌胃给予生理盐水,温胃阳汤低、中、高剂量组和雷尼替丁组则分别用温胃阳汤(0.743 g/mL、1.485 g/mL和2.970 g/mL)及盐酸雷尼替丁胶囊(3 g/L)灌胃。治疗结束后,以碳墨推进法测定小肠推进率;采用甲苯胺蓝染色观察大鼠十二指肠组织肥大细胞并计数;ELISA测定大鼠十二指肠中肥大细胞类胰蛋白酶(mast cell tryptase,MCT)和组胺(histamine,HA)的含量;RT-qPCR检测十二指肠中SCF和c-Kit mRNA的表达;Western blot和免疫组化检测十二指肠中SCF和c-Kit蛋白的表达水平。结果:与模型组相比,温胃阳汤治疗显著提高大鼠的小肠推进率(P<0.05);ELISA结果显示,温胃阳汤治疗可减少大鼠十二指肠黏膜组织肥大细胞数量及MCT和HA含量(P<0.05);Western blot和免疫组化结果表明,温胃阳汤治疗可上调大鼠十二指肠组织c-Kit和SCF蛋白的表达水平(P<0.05),增加SCF和c-Kit阳性细胞数(P<0.05);RT-qPCR结果显示,WWYD治疗可上调大鼠十二指肠组织c-Kit和SCF mRNA的表达(P<0.01)。而且,小肠推进率分别与MCT和HA含量呈负相关,与SCF和c-Kit的表达呈正相关。结论:温胃阳汤能促进大鼠十二指肠动力,其作用机制可能与抑制大鼠十二指肠MCT和HA的生成,及激活SCF/c-Kit信号通路有关。

难治性晚期KIT外显子9突变胃肠间质瘤患者的治疗探索:靶向联合治疗加肿瘤减灭术

KIT外显子9突变是胃肠间质瘤第二常见的基因突变类型,较其他类型呈现恶性度更高的生物学行为。大多数KIT外显子9突变胃肠间质瘤经标准序贯治疗后并不能获得满意的无进展生存期。本文报道了1例44岁晚期KIT外显子9突变女性患者,在标准二线治疗进展后予阿伐替尼联合舒尼替尼治疗,1个月后肿瘤退缩达15.7%,获得手术机会。患者术后继续靶向联合治疗,截至2023年7月,共有6个月未见肿瘤复发。

KIT突变与核心结合因子急性髓系白血病患儿临床特征和预后的关系

目的 分析核心结合因子急性髓系白血病(CBF-AML)患儿KIT位点表达及其与患儿临床特征和预后的关系。方法 选取2014年2月-2022年8月郑州大学附属儿童医院初诊确诊CBF-AML患儿72例,收集其相关临床资料。根据细胞遗传学分析结果分为RUNX1-RUNX1T1组(60例)和CBFβ-MYH11组(12例);根据KIT基因突变情况分为KIT阳性组(31例)和KIT阴性组(41例)。比较KIT阳性组和KIT阴性组相关临床特征和预后差异。结果 KIT阳性组和KIT阴性组性别、年龄、初诊白细胞计数、初诊外周血和骨髓原始细胞比例、髓外白血病、第一疗程完全缓解(CR)率,以及5年无事件生存率和5年总生存率差异均无统计学意义(P>0.05)。结论 KIT突变对CBF-AML患儿临床表现和预后无明显影响。

基于SCF/c-kit信号通路探讨理气通便方对气滞型慢传输型便秘大鼠肠道动力的影响

目的 基于SCF/c-kit信号通路探讨理气通便方对气滞型慢传输型便秘(STC)大鼠肠道动力的影响。方法 将36只Wistar雌性大鼠按随机数字表法分为对照组6只和造模组30只。造模组采用“洛哌丁胺混悬液+夹尾刺激”复制气滞型STC大鼠模型,连续刺激14 d。当大鼠表现出激惹、易怒、烦躁等情况,正常喂养饲料时出现大便干硬、排便数量减少等表现时,说明气滞型便秘模型造模成功。将造模成功的大鼠按照随机数字表法分为模型组、西药组、低剂量组、中剂量组和高剂量组各6只,低、中、高剂量组分别按5.15、10.3、20.6 g/(kg·d)给予理气通便方药液灌胃;西药组按0.18 mg/(kg·d)给予琥珀酸普芦卡必利片混悬液灌胃;对照组和模型组按10 mL/(kg·d)给予无菌水灌胃,每日1次,连续灌胃14 d。比较6组末次给药后6 h的粪便排出量、粪便含水量和小肠推进率;HE染色观察结肠组织病理变化;免疫组化检测结肠组织c-kit蛋白表达水平;Western blot检测结肠组织c-kit、SCF蛋白表达量。结果 HE染色显示:对照组大鼠结肠黏膜完整,杯状细胞和腺体排列整齐,未见炎症细胞聚集;模型组结肠黏膜出现肠腺排列欠整齐,黏膜下层间质血管扩张;各给药组结肠黏膜肠腺排列整齐,未观察到明显上皮损伤。与对照组比较,模型组粪便排出量、粪便含水量和小肠推进率均明显降低(P<0.05),结肠组织c-kit蛋白表达水平和c-kit、SCF蛋白表达量均明显降低(P<0.05)。与模型组比较,西药组、中剂量组、高剂量组粪便排出量、粪便含水率和小肠推进率均明显提高(P<0.05),低剂量组粪便排出量和粪便含水率均明显提高(P<0.05);给药组结肠组织c-kit蛋白表达水平均明显提高(P<0.05);低、中、高剂量组结肠组织c-kit蛋白表达量均明显提高(P<0.05),高剂量组SCF蛋白表达量明显提高(P<0.05)。结论 理气通便方可提高气滞型STC模型大鼠结肠组织中ICC的表达及调控SCF/c-kit信号通路,恢复对胃肠道节律的正常调控来改善便秘的症状。

基于drop-off ddPCR方法检测急性髓系白血病C-KIT基因N822位点突变及其临床应用

目的:建立急性髓系白血病(acute myeloid leukemia, AML)患者C-KIT基因N822位点突变的drop-off微滴式数字PCR(droplet digital PCR,ddPCR)定量检测方法,并评价其临床应用价值。方法:针对C-KIT基因第17外显子设计一对引物及探针,优化drop-off ddPCR反应条件及体系,评价该方法的特异性、灵敏度、重复性,使用所建立的方法对140例已行Sanger测序的AML初诊患者骨髓标本进行检测,并用二代测序(next generation sequencing, NGS)验证结果;用drop-off ddPCR对3例阳性患者化疗后C-KIT突变频率进行动态监测。结果:drop-off ddPCR检测C-KIT基因N822位点突变的最适退火温度为54℃,空白检测限为1.62拷贝数/μL,最低检测下限为10.12拷贝数/μL,线性良好。140例AML初诊患者样本中Sanger测序检出2例阳性(1.4%),而ddPCR共检出突变7例(5.0%),突变频率为0.29%~7.41%;进一步应用常规NGS方法对ddPCR阳性样本进行验证,共检出阳性3例(2.1%),等位基因频率为1.26%~8.00%。动态监测3例阳性患者C-KIT突变频率,结果显示治疗达完全缓解时C-KIT突变频率明显下降甚至降低至0。结论:本研究建立了检测C-KIT基因N822位点突变的drop-off ddPCR技术,具有良好的方法学检测性能,其灵敏度高于Sanger测序和NGS,有望用于阳性患者缓解后的可检测残留疾病监测及治疗指导。

哺乳动物毛色候选基因c-KIT的研究进展

哺乳动物的皮毛颜色主要受毛发中黑色素的种类和数量影响。c-KIT基因编码一种酪氨酸激酶跨膜受体,被称为肥大/干细胞生长因子受体,与黑色素生物合成相关。c-KIT基因突变会抑制干细胞生长因子受体功能,导致黑色素细胞的生成、成熟、增殖、分化和迁移等过程受到影响。本文就哺乳动物毛色形成的机制和主效基因、c-KIT基因的作用机理及其对哺乳动物毛色的影响进行综述,以期为深入研究哺乳动物毛色遗传机制以及不同毛色的选种和选育提供参考依据。

SCF/c-Kit在小鼠隐睾模型中的表达变化及意义

目的:观察干细胞因子(SCF)与原癌基因c-Kit在小鼠隐睾模型睾丸组织中的表达变化。方法:将妊娠BALB/c小鼠随机分成A、B、C、D、E五组;在妊娠第12~21天持续10 d经给予氟他胺灌胃,剂量依次为0 mg/kg、150 mg/kg、300 mg/kg、500 mg/kg、700 mg/kg,在子代小鼠出生后第8周时采用Real-Time PCR法检测其睾丸组织SCF mRNA的相对表达量,运用量子点技术检测c-Kit在组织中的表达情况。结果:小鼠隐睾模型诱导成功。五组中小鼠睾丸组织SCF mRNA的相对表达量分别为1.00±0.01、0.78±0.04、0.61±0.03、0.45±0.05、0.35±0.03,SCF mRNA的表达依次降低,与A组相比(P<0.05)。c-Kit在实验组的表达明显少于对照组。结论:在氟他胺诱导的小鼠隐睾模型中,小鼠睾丸组织SCF mRNA与c-Kit表达的下降可能是隐睾小鼠生精功能受损的重要原因之一。

基于Raspberry Pi及Drone Kit的无人机飞行控制教学实践应用

基于开源硬件Raspberry Pi,Pixhawk及开源软件Drone Kit,设计了高校无人机飞行控制教学实践课程。课程中使用Raspberry Pi作为无人机的机载计算机与Pixhawk飞控芯片协同工作,通过使用MAVLink协议通信。学生在实践操作中需要掌握硬件各接口的功能属性进行无人机组装,在调测环境下,基于Drone Kit开发无人机飞行控制程序。所提的实践课程可以提高学生的动手实践能力,新环境下的创新应用能力能加深对飞行控制技术的理论理解。

A Clinical Study to Assess the Effectiveness of Oral Combination Kit Therapy in Syndromic Management of Abnormal Vaginal Discharge (FEMINE Study) in Kinshasa, Democratic Republic of Congo

Background: Vaginal discharge is one of most common and nagging problems that women face. About 20% - 25% of women who visit gynecology department complain of vaginal discharge and leucorrhoea. An orally administered combination kit, containing 2 g secnidazole, 1 g azithromycin and 150 mg fluconazole (Azimyn FS Kit), has been successfully evaluated in clinical trials and used in several countries for management syndromic vaginal discharge due to infections. Methods: This is a longitudinal study which aimed to verify the clinical efficacy of the combined oral kit containing secnidazole, azithromycin and fluconazole (Azimyn FS Kit®) in the syndromic treatment of abnormal vaginal discharge in patients received in outpatient consultations in Kinshasa/DR Congo from March to September 2023. Results: Majority of patients had whitish vaginal discharge (51.6%) of average abundance (56.2%), accompanied by pruritus in 72.1% of cases, and dyspareunia in 23.5% of cases and hypogastralgia in 40.2% of cases. One week after treatment with the Azimyn FS® combined kit, at the greatest majority of patients (97.3%), abnormal vaginal discharge had decreased by more than 50% (84.1%). Two weeks after treatment with the Azimyn FS® combined kit, almost all patients (97.3%) no longer had abnormal vaginal discharge which had completely disappeared. Conclusion: A single dose of secnidazole, azithromycin and fluconazole in the form of an oral combi-kit (Azimyn FS Kit) has shown excellent therapeutic effectiveness in the syndromic treatment of abnormal vaginal discharge wherein patients were treated without diagnostic confirmation.

基于SCF/C-kit信号通路探讨益髓破血方改善脑出血小鼠肠动力“通腑”作用机制

目的观察益髓破血方对脑出血小鼠排便情况与结肠组织干细胞因子(stem cell factor,SCF)/酪氨酸激酶受体(kit proto-oncogene,C-kit)信号通路的影响,探讨益髓破血方调节脑出血小鼠肠动力通腑作用机制。方法将54只SPF级健康雄性C57BL/6J小鼠随机均分为假手术组、模型组与方剂治疗组,采用鼠尾自体血注入法制作实验性脑出血模型,假手术组只进针不注射。方剂治疗组给予1 g/mL益髓破血方悬浊液灌胃,假手术组、模型组给予等体积生理盐水灌胃,每天1次。观察各组小鼠排便情况,记录第1天、第3天、第7天同时段6 h内的排便量以及末次灌胃后首次排便间隔时间,并于相同时间分段点处死小鼠取材,采用免疫组化和Western Blot法检测小鼠结肠组织中的SCF、C-kit蛋白。结果与假手术组比较,模型组小鼠第1天、第3天、第7天各6 h内排便量显著减少(P<0.05),末次灌胃首次排便时间明显滞后(P<0.05),结肠组织中SCF、C-kit蛋白表达显著减少(P<0.05),且随周期延长呈逐渐降低趋势;与模型组比较,方剂治疗组第1天、第3天、第7天各6 h内排便量相对增多(P<0.05),首次排便时间缩短(P<0.05),SCF、C-kit蛋白表达水平升高(P<0.05),且随时间推移逐渐向正常量恢复。结论益髓破血方干预治疗脑出血小鼠,可以增加肠动力,促进排便,发挥通腑作用使肠功能恢复,改善脑出血后便秘,其机制可能与SCF/C-kit信号通路有关。

Sensitivity of Commercial Enzyme Inhibition Colorimetric Pesticide Residue Rapid Test Kit to a Variety of Pesticides

[Objectives]To fully understand the quality of commercial enzyme inhibition-colorimetric pesticide residue rapid detection kits,so that they can play a greater role in the detection and supervision of agricultural products.[Methods]The sensitivity of 28 kinds of pesticides was determined by using the commercially available enzyme inhibition colorimetric rapid detection kit with Hendu brand.[Results]There was a significant difference in the sensitivity of the kit to each pesticide,and the kit was more sensitive to dichlorvos among the 28 pesticides tested.The sensitivity to methyl isosalifos,dimethoate,isocarbophos,fenthion and phorate was poor,and the sensitivity to quinalphos was different between 3.0 and 2.5 mL.[Conclusions]The large difference of the sensitivity of the enzyme inhibition-colorimetric rapid detection kit for pesticide residues to different kits is a reason for the false positive and false negative test results of the kit,which needs to be considered by relevant personnel.