猕猴桃黑头病菌的生物学特性及其致病性研究

明确猕猴桃黑头病病原菌的生物学及致病特性,研究不同培养条件下菌体的生长特性,及其对不同品种猕猴桃的致病性差异,为深入开展侵染机理、流行规律及病害防治关键技术等研究提供理论依据。结果表明,猕猴桃黑头病的病原菌Diaporthe eres在15~30℃、pH 5~11条件下均能生长,最适温度28℃,对高温敏感,高于35℃时菌体生长速度显著降低。菌体在多种碳源中均能生长,最适碳源为葡萄糖。更易利用有机氮源,最适氮源为酵母浸粉。钙离子对病原菌生长具有促进作用,菌体生长速度与钙离子含量呈正比。菌体不能产生有性孢子,只能以无性分生孢子进行繁殖。对‘翠香’、‘徐香’、‘瑞玉’猕猴桃具有明显的致病性,但是不侵染‘海沃德’、‘亚特’、‘秦美’猕猴桃。

某猕猴繁育场B病毒相关抗体检测报告

实验猕猴是医学科学研究中非常重要的实验动物,在我国有丰富的自然资源,近年来,全国各地又相继建立了多所猕猴繁育场。据报道,野生猕猴B病毒的感染率相当高,在急性感染期。病毒可直接在猴群内传播,随后则长期潜伏在呼吸道和/或泌尿生殖器官附近的神经节,也可长期潜伏在组织器官内,产生B病毒抗体。B病毒是一种人兽共患病原,人类感染可引起致死性脑炎。因此。

猕猴桃黑头病生防菌的筛选、鉴定及防效评价

研究旨在筛选对猕猴桃黑头病病原真菌(Diaporthe eres)有拮抗作用的菌株。通过平板对峙法从陕西周至县猕猴桃根际土壤中分离筛选到1株具有明显拮抗作用的菌株BKH。显微及菌落形态观察、生理生化试验和16S rDNA序列分析结果表明,该菌株为双向伯克霍尔德氏菌(Burkholderia ambifaria)。菌株BKH在平板上能显著抑制Diaporthe eres生长,抑菌率为72.5%,且对猕猴桃黑头病田间防效可达91.7%,在猕猴桃黑头病生物防治方面具有应用潜力。

猕猴桃花腐病发生原因与综合防治措施

猕猴桃花腐病危害大,严重影响果园效益。结合多年生产实践,总结了花腐病发生原因及综合防治措施,包括选择抗病品种、均衡树体营养、合理调配水肥、对症选择药剂等。

猕猴桃果实熟腐病菌生物学特性及其寄主抗病性鉴定研究

为掌握猕猴桃果实熟腐病的发生规律和为其综合防治提供理论依据,对该病害的两种主要病原菌葡萄座腔菌(Botryosphaeria dothidea)和拟茎点霉菌(Phomopsis sp.)的生物学特性、寄主范围和猕猴桃品种抗病性进行了鉴定研究,结果表明葡萄座腔菌和拟茎点霉菌均在25℃和pH 7.0的条件下生长最快;适合两者生长的碳氮源种类基本相同;葡萄座腔菌偏好利用马铃薯葡萄糖培养基、胡萝卜培养基和苜蓿煎汁培养基,而拟茎点霉菌偏好利用烟草煎汁培养基。伤口接种试验表明,供试的5科14种植物均能被上述两种病菌感染,都应属于其寄主范围的植物;供试的17个猕猴桃品种,只有3个品种为高抗品种,其余14个为感病品种。

猕猴桃枝枯病病原菌鉴定

通过病原菌的形态特征、致病性测定和rDNA-ITS序列分析,对引起猕猴桃枝枯病的病原菌进行了分离鉴定。结果表明:猕猴桃枝枯病的主要病原菌为拟茎点霉菌(Phomopsis sp.)、隔孢丛壳菌(Glomerella septospora)和葡萄座腔菌(Botryosphaeria dothidea),3种病菌所占比率分别为39%、38%和23%,且无论是孢子悬浮液接种还是菌丝体接种均只能通过伤口侵染而引起枝条发病。

猕猴桃膏药病病原菌初步鉴定及防治建议

为了初步明确猕猴桃膏药病的病原菌,通过病害症状观察、病原菌形态特征观察和分子技术测序分析对猕猴桃膏药病进行了病原菌鉴定。根据病害症状特征、病原菌形态特征和系统发育分析,将引起猕猴桃膏药病的病原菌初步鉴定为假柄隔担菌Septobasidium pseudopedicellatum。同时对病原菌的研究现状进行了讨论,并对膏药病防治措施予以阐述,以期为猕猴桃膏药病的研究和防治提供参考。

生防菌对猕猴桃两种病原真菌的抑制效果

为筛选对猕猴桃黑斑病和白纹羽病有良好防效的生防菌,选用前期获得的1种生防菌和市售的6种生防菌剂对其病原链格孢菌Alternaria alternata与褐座坚壳菌Rosellinia necatrix进行室内抑菌试验。结果表明,7种生防菌对上述两种病菌的抑菌效果较一致,抑菌效果最好的为生防菌株西姆芽孢杆菌JY-1,荧光假单胞杆菌、枯草芽孢杆菌、巨大芽孢杆菌和蜡质芽孢杆菌4种生防菌剂也有较好的抑菌效果,而解淀粉芽孢杆菌和哈茨木霉的抑菌效果较差。可选用上述4种防效较好的生防菌剂对猕猴桃黑斑病和白纹羽病进行生物防治,并对JY-1菌株进行开发利用。

21种化学药剂对猕猴桃黑点病菌(Diaporthe phaseolorum)的室内毒力及田间防效

旨在筛选猕猴桃黑点病防治药剂并明确其防治效果。采用菌丝生长速率法,测定21种不同化学药剂对猕猴桃黑点病菌的毒力,并选择其中16种药剂进行田间药效试验。结果显示,烯肟·戊唑醇w=20%悬浮剂(SC)等9种药剂对黑点病菌具有极强的抑菌效果,其EC_(50)值均达0.05~1.12μg/mL,表现为极度敏感;其次为抑霉唑w=20%水乳剂EW、辛菌胺醋酸盐w=1.8%水剂(AS)及腐霉利w=50%可湿性粉剂(WP),其EC_(50)值为14.02~37.37μg/mL,表现为高度敏感;氨基寡糖素w=5%(AS)、嘧环·咯菌腈w=62%水分散粒剂(WG)和吡唑醚菌酯w=25%乳油(EC)的EC_(50)值分别为118.49μg/mL、195.32μg/mL和255.18μg/mL,表现为中度敏感或低度敏感;而苯醚甲环唑w=10%(WG)等6种药剂其EC_(50)值分别远大于350μg/mL,为不敏感;供试的16种药剂在田间均表现出极显著防治效果,其中:苯甲·丙环唑w=30%(EC)450 g/hm^(2)、氟唑菌酰羟胺·苯醚甲环唑w=20%(SC)600 g/hm^(2)、嘧环·咯菌腈w=62%(WG)600 g/hm^(2)、腈苯唑w=24%(SC)900 g/hm^(2)、丙环唑·嘧菌脂w=18.7%(SC)600 g/hm^(2)、啶酰·咯菌腈w=30%(SC)900 g/hm^(2)及戊唑醇w=43%(SC)450 g/hm^(2)7种药剂处理平均防效达到84.32%~90.36%;其次为烯肟·戊唑醇w=20%(SC)900 g/hm^(2)、抑霉唑w=20%(EW)900 g/hm^(2)、吡唑醚菌酯w=25%(EC)720 g/hm^(2)、腐霉利w=50%(WP)750 g/hm^(2)、寡糖·吡唑酯w=27%(EW)900 g/hm^(2)及硝酸氨钙可溶性粒剂(SG)1500 kg/hm^(2)6种药剂处理,平均防效达到64.92%~81.78%;而其他3种药剂处理防效略差。结果表明,30%苯甲·丙环唑EC、20%氟唑菌酰羟胺·苯醚甲环唑SC、62%嘧环·咯菌腈WG、24%腈苯唑SC、18.7%丙环唑·嘧菌脂SC、30%啶酰·咯菌腈SC、43%戊唑醇SC、20%烯肟·戊唑醇SC、20%抑霉唑EW、25%吡唑醚菌酯EC、50%腐霉利WP、27%寡糖·吡唑嘧菌酯EW 12种药剂及土施农用硝酸氨钙SG对猕猴桃黑点病均具有良好的防治效果,可作为今后防治猕猴桃黑点病的优选药剂。

6种诱抗剂对奉新猕猴桃2种真菌病害的田间防效试验

为了筛选出防治猕猴桃黑斑病和果腐病的有效诱抗剂,对6种诱抗剂进行了田间药效试验。结果表明,芸苔素内酯和香菇多糖对黑斑病的防效显著,阿泰灵和赤·吲乙·芸苔的防效其次,超敏蛋白和氨基寡糖素的防效较差;阿泰灵对果腐病的防效较好,氨基寡糖素和芸苔素内酯其次,赤·吲乙·芸苔、超敏蛋白和香菇多糖几乎无效果。建议生产上选用芸苔素内酯、香菇多糖或阿泰灵对猕猴桃黑斑病和果腐病进行绿色防控。

利用小RNA测序鉴定江西奉新猕猴桃病毒种类

为探明江西省奉新县猕猴桃感染病毒的情况,2020年5月从该县山口、农合和新西蓝3个主要猕猴桃种植区共采集23份疑似病毒病叶片样品,利用小RNA深度测序技术对混合样品进行病毒检测,并通过RT-PCR和测序验证。结果共检测出4种病毒,分别是猕猴桃病毒A(Actinidia virus A,AcVA)、猕猴桃病毒B(Actinidia virus B,AcVB)、猕猴桃褪绿环斑相关病毒(Actinidia chlorotic ringspots associated virus,AcCRaV)和柑桔叶斑驳病毒(Citrus leaf blotch virus,CLBV),在23份样品中的检出率依次为87.0%、56.5%、65.2%和60.9%,多数样品存在病毒复合侵染,复合侵染率81.8%。表明引起奉新县猕猴桃病毒病的毒原主要有AcVA、AcVB、AcCRaV和CLBV 4种,优势毒原为AcVA,病毒复合侵染发生普遍。

不同药剂对猕猴桃花腐病的防治效果

【目的】明确6种药剂对猕猴桃花腐病的田间防治效果,筛选高效、安全的药剂用于指导猕猴桃的田间生产。【方法】采用随机区组设计开展田间试验,测定喷施6种药剂后猕猴桃花腐病的发病率及病情指数,通过计算防治前后发病率和病情指数的变化值来判断防治效果,并记录猕猴桃植株生长情况和花果发育性状来评价其安全性。【结果】6种药剂对猕猴桃花腐病呈不同水平的防治效果,且均对猕猴桃植株安全。防治前各处理组与对照组的发病率、病情指数均无显著性差异;连续两次施药防治后,各处理组和对照组的发病率较防治前均呈增加趋势,且发病情况变化值差异显著,其中对照组的发病情况变化值最大,发病率与病情指数增幅分别达13.29%和6.84;春雷·溴菌腈与四霉素·丙硫唑处理组的变化值最小,发病率增幅均小于1.50%,病情指数增幅均小于1.00。田间防治效果与发病情况相对应,连续两次施药后,春雷·溴菌腈处理表现出最高的防治效果,四霉素·丙硫唑次之,均达75%以上。各药剂施用后对猕猴桃植株均无药害症状和其他不良影响,且较对照组呈不同水平的保花保果增产作用。6种药剂中,春雷·溴菌腈、四霉素·丙硫唑最能有效延缓猕猴桃花腐病病原菌的传播与扩散,减轻发病程度,可以高效安全地防治猕猴桃花腐病。【结论】针对猕猴桃花腐病,筛选出春雷·溴菌腈、四霉素·丙硫唑两种高效安全的药剂,可在猕猴桃田间生产中进行推广。

5种杀菌剂对猕猴桃黑头病的室内抑菌活性及田间防效研究

为筛选对猕猴桃黑头病有效的杀菌剂,以猕猴桃黑头病病原菌Diaporthe eres为试验对象,采用菌丝生长速率法测定5种杀菌剂对其抑制作用,并进一步开展田间防效试验。结果表明,5种杀菌剂对病原菌菌丝生长均有较好的抑制作用,并且对猕猴桃黑头病的田间防效显著(P<0.05)。因此,这5种杀菌剂均可作为病害防治的有效药剂,特别是10%苯醚甲环唑水分散粒剂、25%吡唑醚菌酯悬浮剂和40%腈菌唑可湿性粉剂3种杀菌剂田间防效均达到85%以上,可作为优选药剂。

10种杀菌剂对葡萄座腔菌的室内毒力测定

葡萄座腔菌Botryosphaeria dothidea是猕猴桃果腐病的病原菌。为了给猕猴桃果腐病田间药效试验提供备用药剂,本文采用菌丝生长速率法测定了10种杀菌剂的毒力。结果表明,11%的精甲·咯·嘧菌悬浮种衣剂、43%戊唑醇悬浮剂、25%咪鲜胺乳油和18.7%丙环·嘧菌酯悬浮剂对葡萄座腔菌具有强毒力,EC50分别为0.022 5、0.049 0、0.079 8和0.149 4μg/mL;10%多抗霉素可湿性粉剂、42.8%氟菌·肟菌酯悬浮剂、24%腈苯唑悬浮剂、44%精甲·百菌清悬浮剂和2%春雷霉素水剂对葡萄座腔菌具有较强的毒力,EC50分别为0.527 5、0.579 6、2.430 4和3.306 3μg/mL;2%宁南霉素水剂的毒力最弱,EC50值高达81.464 3μg/mL。

猕猴桃褐腐病生防菌株GMH31发酵条件的优化

利用从药用植物牡蒿(Artemisia japonica)中分离筛选出的1株猕猴桃褐腐病生防菌株GMH31,采用含毒介质平板法进行抑菌试验,通过单因子试验和正交试验,对该菌株的最适发酵培养基成分(包括碳源、氮源、无机盐离子、微量元素)及发酵条件(包括发酵时间、温度、pH、转数、装液量、接种量)进行了优化。结果显示:尤韦可拟盘多毛孢菌株GMH31培养基组分最佳配比为麦芽糖35 g/L、氯化铵12 g/L、K_2HPO_40.1 g/L、甘氨酸0.015 g/L,最佳发酵条件为培养时间14 d、培养温度26℃、初始pH 6.0、摇床转速120 r/min、250 m L装液量100 m L、接菌量为装液量的6%。在最佳发酵培养基和培养条件下,GMH31菌株发酵滤液对猕猴桃褐腐病菌的抑制率提高了16.45%。

Increasing dietary fiber intake in terms of kiwifruit improves constipation in Chinese patients

AIM： To investigate if increased dietary fiber, in terms of kiwifruit, is effective in Chinese constipated patients. METHODS： 33 constipated patients and 20 healthy volunteers were recruited for a 4-wk treatment of kiwi fruit twice daily. Response during wk 1-4 was defined as an increase in complete spontaneous bowl, motion （CSBM）≥ 1/wk. Secondary efficacy included response during wk 1-4, individual symptoms and scores of bowel habits and constipation. Responses were compared with the baseline run-in period. Colonic transit time and anorectal manometry were performed before and after treatment. RESULTS： Responder rate was 54.5% in the constipated group. The mean CSBM increased after treatment （2.2±2.6 vs 4.4± 4.6, P = 0.013）. There was also improvement in the scores for bothersomeness of constipation （P = 0.02）, and satisfaction of bowel habit （P = 0.001）, and decreased in days of laxative used （P = 0.003）. There was also improvement in transit time （P = 0.003） and rectal sensation （P 〈 0.05）. However, there was no change in the bowel symptoms or anorectal physiology in the healthy subjects. CONCLUSION： Increasing dietary fiber intake is effective in relieving chronic constipation in Chinese population.

A Macaca mulatta model of fulminant hepatic failure

AIM:To establish an appropriate primate model of fulminant hepatic failure (FHF).METHODS:We have,for the first time,established a large animal model of FHF in Macaca mulatta by intraperitoneal infusion of amatoxin and endotoxin.Clinical features,biochemical indexes,histopathology and iconography were examined to dynamically investigate the progress and outcome of the animal model.RESULTS:Our results showed that the enzymes and serum bilirubin were markedly increased and the enzyme-bilirubin segregation emerged 36 h after toxin administration.Coagulation activity was significantly decreased.Gradually deteriorated parenchymal abnormality was detected by magnetic resonance imaging (MRI) and ultrasonography at 48 h.The liver biopsy showed marked hepatocyte steatosis and massive parenchymal necrosis at 36 h and 49 h,respectively.The autopsy showed typical yellow atrophy of the liver.Hepatic encephalopathy of the models was also confirmed by hepatic coma,MRI and pathological changes of cerebral edema.The lethal effects of the extrahepatic organ dysfunction were ruled out by their biochemical indices,imaging and histopathology.CONCLUSION:We have established an appropriate large primate model of FHF,which is closely similar to clinic cases,and can be used for investigation of the mechanism of FHF and for evaluation of potential medical therapies.

Hepatitis G virus genomic RNA is pathogenic to Macaca mulatta

AIM: To explore the pathogenicity and infectivity of hepatitis G virus (HGV) by observing replication and expression of the virus, as well as the serological and histological changes of Macaca mulatta infected with HGV genomic RNA or HGV RNA-positive serum.METHODS: Full-length HGV cDNA clone (HGVqz) was constructed and proved to be infectious, from which HGV genomic RNA was transcribed in vitro. Macaca mulatta BY1 was intra-hepatically inoculated with HGV genomic RNA, HGV RNA-positive serum from BY1 was intravenously inoculated into Macaca mulatta BM1, and then BB1 was infected with serum from BM1. Serum and liver tissue were taken regularly, and checked with RT-PCR, in situ hybridization and other immunological, serological,histological assays.RESULTS: Serum HGV RNA was detectable in all the 3Macaca mulattas, serological and histological examinations showed the experimental animals had slightly elevated alanine transaminase (ALT) and developed HGV viremia during the infectious period. The histology, immunohistochemistry, and in situ hybridization in liver tissues of the inoculated animals demonstrated a very mild hepatitis with HGV antigen expression in cytoplasm of hepatocytes.RT-PCR and quantitative PCR results showed that HGV could replicate in liver.CONCLUSION: The genomic RNA from full-length HGV cDNA is infectious to the Macaca mulatta and can cause mild hepatitis. HGV RNA-positive serum, from HGV RNA inoculated Macaca mulatta, is infectious to other Macaca mulattas. Macaca mulatta is susceptible to the inoculated HGV, and therefore can be used as an experimental animal model for the studies of HGV infection and pathogenesis.