Amanita

  • 文章类型: Journal Article
    鹅膏菌属是最突出的蘑菇属之一,由于其文化,经济,和医学的重要性。最近,世界上已经描述了许多新的天牛物种,增加属的丰富度。然而,几个进化枝具有神秘的多样性,许多物种复合物尚未解决。这是Validae部分的发红物种的情况,以Amanitarubescenss.l的名称被广泛引用。我们使用了四基因座矩阵(nucrDNA内部转录间隔区[ITS]和28S区域和RNA聚合酶II亚基2[rpb2]的基因,平移延伸因子1-α[tef1-α],和β-微管蛋白[tub2]),以解决Amanita节Validae内的系统发育关系。为了分析物种的多样性和分布模式,我们使用了广泛的ITS序列采样,包括环境DNA数据库。系统发育分析表明,Validae部分分为三个单系和高度支持的主要进化枝:Mappae,Validae,还有Rubescentes.Rubescentes进化枝中至少有11个物种级进化枝得到了高度支持:A.cruentilemurumnom。prov.A.Brunneolocularis,A.rubescenss.s.(欧洲进化枝),A.rubescenss.s.(亚洲进化枝),A.orsoniis.s.A.\'A.aureosubuculanom.prov.,A.novinupta,A.flavorubens,和两个未描述的北美物种。我们证明了A.rubescenss.s.有两个隔离的种群(欧洲和亚洲),并且在美国不是自然分布的。此外,我们发现美国在鲁比斯琴塞进化枝内的神秘物种比欧亚大陆多。
    Amanita is one of the most salient mushroom genera due to its cultural, economic, and medical importance. Recently, many new Amanita species have been described worldwide, increasing the genus richness. However, several clades have cryptic diversity, and many species complexes have not yet been resolved. This is the case of the rubescent species in the Validae section, which have been widely cited under the name Amanita rubescens s.l. We used a four-locus matrix (nuc rDNA internal transcribed spacer [ITS] and 28S regions and genes for RNA polymerase II subunit 2 [rpb2], translation elongation factor 1-α [tef1-α], and β-tubulin [tub2]) to solve the phylogenetic relationships within the Amanita section Validae. To analyze the diversity and distribution patterns of species, we used an extensive ITS sequence sampling including environmental DNA databases. The phylogenetic analyses demonstrated that the Validae section is divided into three monophyletic and highly supported major clades: Mappae, Validae, and Rubescentes. At least 11 species-level clades within the Rubescentes clade were highly supported: A. cruentilemurum nom. prov. A. brunneolocularis, A. rubescens s.s. (European clade), A. rubescens s.s. (Asiatic clade), A. orsonii s.s. A. \'orsonii,\' A. aureosubucula nom. prov., A. novinupta, A. flavorubens, and two undescribed North American species. We proved that A. rubescens s.s. has two segregated populations (European and Asiatic) and it is not naturally distributed in America. Furthermore, we found that America has more cryptic species within the Rubescentes clade than Eurasia.
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  • 文章类型: Journal Article
    蘑菇中毒是全球食源性疾病和相关死亡的重要原因。Amanita蘑菇经常引起这种中毒;然而,由于无法获得新鲜和完整的样品,因此识别这些有毒物种具有挑战性。通常需要分析残留物,呕吐物,或胃提取物以获得DNA序列,用于鉴定导致食物中毒的物种。这通常证明获得可用的DNA序列具有挑战性,所述可用的DNA序列可以使用常规分子生物学技术进行分析。因此,这项研究旨在开发一种DNA迷你条形码方法,用于鉴定天牛物种。在对Amanita蘑菇中DNA迷你条形码的通用引物进行评估和优化之后,我们发现内部转录间隔区(ITS)基因序列引物ITS-a是鉴定天牛物种最合适的DNA条形码引物。随后扩增并测序了43个Amanita样品。对获得的序列进行了种内和种间遗传距离分析,并构建了系统发育树。结果表明,所设计的引物在天牛样品中具有很强的普适性,可以准确鉴定出长度为290bp的目的基因片段。值得注意的是,DNA迷你条形码准确识别了43个天牛样本,证明与常规DNA条形码的高度一致性。此外,它有效地从消化样品中鉴定出DNA。总之,这种DNA迷你条形码是一种有前途的工具,用于检测意外摄入有毒的鹅膏菌。它可以用作最佳条形码,用于在天牛引起的蘑菇中毒事件中进行物种识别和可追溯性。关键点:•开发用于无新鲜样品的天牛物种鉴定的DNA迷你条形码方法。•ITS-a引物集经优化以在天牛样品中实现稳健的通用性。•迷你条形码适用于在蘑菇中毒情况下筛选有毒蘑菇物种。
    Mushroom poisoning contributes significantly to global foodborne diseases and related fatalities. Amanita mushrooms frequently cause such poisonings; however, identifying these toxic species is challenging due to the unavailability of fresh and intact samples. It is often necessary to analyze residues, vomitus, or stomach extracts to obtain DNA sequences for the identification of species responsible for causing food poisoning. This usually proves challenging to obtain usable DNA sequences that can be analyzed using conventional molecular biology techniques. Therefore, this study aimed to develop a DNA mini-barcoding method for the identification of Amanita species. Following the evaluation and optimization of universal primers for DNA mini-barcoding in Amanita mushrooms, we found that the internal transcribed spacer (ITS) gene sequence primer ITS-a was the most suitable DNA barcode primer for identifying Amanita species. Forty-three Amanita samples were subsequently amplified and sequenced. The sequences obtained were analyzed for intra- and inter-species genetic distances, and a phylogenetic tree was constructed. The findings indicated that the designed primers had strong universality among the Amanita samples and could accurately identify the target gene fragment with a length of 290 bp. Notably, the DNA mini-barcode accurately identified the 43 Amanita samples, demonstrating high consistency with the conventional DNA barcode. Furthermore, it effectively identified DNA from digested samples. In summary, this DNA mini-barcode is a promising tool for detecting accidental ingestion of toxic Amanita mushrooms. It may be used as an optimal barcode for species identification and traceability in events of Amanita-induced mushroom poisoning. KEY POINTS: • Development of a DNA mini-barcoding method for Amanita species identification without fresh samples. • The ITS-a primer set was optimized for robust universality in Amanita samples. • The mini-barcode is suitable for screening toxic mushroom species in mushroom poisoning cases.
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  • 文章类型: Journal Article
    白天牛,一种在东亚发现的致命蘑菇,在中国所有毒蘑菇中死亡率最高。本研究的目的是开发一种有效的,准确,和用户友好的基于PCR的方法,用于鉴定可以促进预防的近侧索杆菌,诊断,以及相关食物中毒的治疗。根据27个蘑菇物种的内部转录间隔区变异设计了天然特异性引物和探针。使用常规和实时PCR对23种非目标蘑菇物种进行了特异性确认,包括形态相似和密切相关的物种。与常规PCR相比,实时PCR更敏感(可检测的DNA浓度:1.36×10-2ng/μL与1.36×10-3)和有效(分析时间:1hvs.40分钟)。此外,实时PCR结果可以使用扩增曲线分析立即可视化。结果提供了两种基于PCR的可靠方法,可用于促进食品安全。
    Amanita exitialis, a deadly mushroom found in eastern Asia, causes the highest death rates among all poisonous mushrooms in China. The aim of the present study was to develop an efficient, accurate, and user-friendly PCR-based method for identifying A. exitialis that could facilitate the prevention, diagnosis, and treatment of associated food poisoning. A. exitialis-specific primers and probes were designed based on the internal transcribed spacer region variations of 27 mushroom species. Specificity was confirmed using conventional and real-time PCR for 23 non-target mushroom species, including morphologically similar and closely related species. Compared to conventional PCR, real-time PCR was more sensitive (detectable DNA concentration: 1.36 × 10-2 ng/μL vs. 1.36 × 10-3) and efficient (analysis time: 1 h vs. 40 min). Furthermore, the real-time PCR results could be immediately visualized using amplification curve analysis. The results present two robust PCR-based methods for A. exitialis identification that can facilitate food safety.
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  • 文章类型: Journal Article
    众所周知,在蘑菇中毒病例中,天鹅膏中毒是最致命的病例。它的主要毒性机制是它通过其毒素与DNA依赖性RNA聚合酶II酶的不可逆结合而导致细胞死亡。本研究旨在分析CDP-胆碱分子对天鹅膏蘑菇中毒病例的影响。取蛇毒蘑菇的提取物,并以0.3g/kg的剂量腹膜内给予雄性Wistar白化病大鼠。在实验阶段,将大鼠按100mg/kg的剂量分为3组,250mg/kg,和500毫克/千克,对照组给予1ml/kg剂量的0.9%等渗NaCl溶液。然后在第2小时腹膜内给予治疗,在第六个小时,大鼠被处死。通过组织病理学评估大鼠肝脏和肾脏组织的损伤程度。结论是,CDP-胆碱显着和剂量依赖性地减少或预防了由天麻引起的中毒图像中肝脏发生的损害,它显示出降低或预防肾脏损伤的趋势,虽然不显著。
    Amanita phalloides poisoning is known to be the most fatal case among mushroom poisoning cases. Its main mechanism of toxicity is that it leads to cell death by the irreversible binding of its toxins to the DNA-dependent RNA polymerase II enzyme. This study was planned to analyze the effects of the CDP-choline molecule on Amanita phalloides mushroom poisoning cases. The extract of the Amanita phalloides mushroom was taken and intraperitoneally administered to male Wistar Albino rats at a dose of 0.3 g/kg. In the experiment phase, the rats were divided into three groups of CDP-choline treatment according to the doses of 100 mg/kg, 250 mg/kg, and 500 mg/kg, and one control group was administered a 1 ml/kg dose of 0.9% isotonic NaCl solution. The treatments were then administered intraperitoneally at the 2nd hour, and at the 6th hour, the rats were sacrificed. The degree of damage in the liver and kidney tissues of the rats was evaluated histopathologically. It was concluded that CDP-choline reduced or prevented the damage that occurred in the liver significantly and dose-dependently in the toxicosis picture caused by Amanita phalloides, and it showed a tendency to lower or prevent the damage in the kidney, albeit not significantly.
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  • 文章类型: Journal Article
    由蛋黄粉引起的蘑菇中毒是全球蘑菇相关死亡的主要原因。Alpha-Amanitin(α-AMA),这些蘑菇中存在的有毒物质,导致肝毒性和肾毒性。我们研究的目的是通过用碘-131标记来确定α-AMA在Balb/c小鼠中的分布。给小鼠注射毒性剂量(1.4mg/kg)的用碘-131标记的α-AMA。小鼠在1号处死,2nd,第四,8th,24日,麻醉下第48小时.小鼠的器官被切除,并且在所有实验中都评估了它们的生物分布。每克肾脏的注射剂量百分比(ID/g%)值,肝脏,肺,第1小时的心脏组织分别为1.59±0.07、1.25±0.33、3.67±0.80和1.07±0.01。这项研究提供了对特定器官中α-AMA积累的潜在长期影响的见解。此外,这项研究产生了必要的数据,可用于证明解毒剂对未来毒性模型中α-AMA生物分布的影响。
    Mushroom poisonings caused by Amanita phalloides are the leading cause of mushroom-related deaths worldwide. Alpha-Amanitin (α-AMA), a toxic substance present in these mushrooms, is responsible for the resulting hepatotoxicity and nephrotoxicity. The objective of our study was to determine the distribution of α-AMA in Balb/c mice by labeling with Iodine-131. Mice were injected with a toxic dose (1.4 mg/kg) of α-AMA labeled with Iodine-131. The mice were sacrificed at the 1st, 2nd, 4th, 8th, 24th, and 48th hours under anesthesia. The organs of the mice were removed, and their biodistribution was assessed in all experiments. The percent injected dose per gram (ID/g %) value for kidney, liver, lung, and heart tissues at 1st hour were 1.59 ± 0.07, 1.25 ± 0.33, 3.67 ± 0.80 and 1.07 ± 0.01 respectively. This study provides insights into the potential long-term effects of α-AMA accumulation in specific organs. Additionally, this study has generated essential data that can be used to demonstrate the impact of antidotes on the biological distribution of α-AMA in future toxicity models.
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  • 文章类型: Journal Article
    背景:天鹅膏中毒是一个严重的健康问题,死亡率为10-40%。中毒的特征是严重的肝和肾毒性。迄今为止,尚未系统地评估天鹅膏中毒对血液学参数的影响。
    方法:从格罗宁根大学医学中心(UMCG)的医院数据库中回顾性地选择了疑似天麻类毒物中毒的患者。医疗数据-包括人口统计学;肝脏,肾,和血液参数;治疗;和结果-收集。使用毒物严重程度评分对中毒的严重程度进行评分。
    结果:在1994年至2022年之间,有28名患者因疑似天鹅膏菌中毒而进入UMCG。血红蛋白和血细胞比容浓度呈时间依赖性下降,白细胞,和血小板。28例患者中有6例发展为急性肝衰竭(ALF)。ALF患者显示肝酶升高较高,国际标准化比率,和PSS与没有ALF的患者相比。相反,这些患者的血红蛋白和血小板数量进一步下降.六名ALF患者中有三名死亡,一名患者接受了肝移植。
    结论:我们的研究表明,石膏粉中毒可能与患者的血液毒性有关。血液学参数的量化与中毒患者相关,尤其是那些与ALF。
    Amanita phalloides poisoning is a serious health problem with a mortality rate of 10-40%. Poisonings are characterized by severe liver and kidney toxicity. The effect of Amanita phalloides poisonings on hematological parameters has not been systematically evaluated thus far.
    Patients with suspected Amanita phalloides poisonings were retrospectively selected from the hospital database of the University Medical Center Groningen (UMCG). Medical data-including demographics; liver, kidney, and blood parameters; treatment; and outcomes-were collected. The severity of the poisoning was scored using the poison severity score.
    Twenty-eight patients were identified who were admitted to the UMCG with suspected Amanita phalloides poisoning between 1994 and 2022. A time-dependent decrease was observed for hemoglobin and hematocrit concentrations, leukocytes, and platelets. Six out of twenty-eight patients developed acute liver failure (ALF). Patients with ALF showed a higher increase in liver enzymes, international normalized ratios, and PSS compared to patients without ALF. Conversely, hemoglobin and platelet numbers were decreased even further in these patients. Three out of six patients with ALF died and one patient received a liver transplant.
    Our study shows that Amanita phalloides poisonings may be associated with hematotoxicity in patients. The quantification of hematological parameters is of relevance in intoxicated patients, especially in those with ALF.
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  • 文章类型: Journal Article
    了解经常拮抗的植物-草食动物相互作用以及宿主防御如何影响草食动物的饮食广度是生态学和进化生物学正在进行的研究领域。通常,产生高度有害化学防御的寄主植物/真菌仅由专家喂养。我们对可以在有害宿主上觅食和发育的通才物种知之甚少。以有毒宿主为食的通才的一个例子发生在以蘑菇为食的果蝇中。尽管这些物种被归类为通才,它们可接受的寄主包括致命的天牛物种。在这项研究中,我们使用行为分析来评估一种以蘑菇为食的物种之间的关联,果蝇,和致命的天鹅膏。我们进行了喂养测定以确认环肽毒素耐受性的存在。然后,我们完成了对雌性苍蝇和幼虫的宿主偏好测定,并且没有发现对有毒蘑菇的偏好。最后,我们评估了竞争对产卵偏好的影响。我们发现,在首选宿主上存在竞争者的卵与苍蝇增加了有毒蘑菇上产卵的数量有关。我们的结果强调了如何获得低竞争的宿主资源可能有助于维持通才物种与剧毒宿主之间的联系。
    Understanding the often antagonistic plant-herbivore interactions and how host defenses can influence herbivore dietary breadth is an area of ongoing study in ecology and evolutionary biology. Typically, host plants/fungi that produce highly noxious chemical defenses are only fed on by specialists. We know very little about generalist species that can feed and develop on a noxious host. One such example of generalists feeding on toxic host occurs in the mushroom-feeding Drosophila found in the immigrans-tripunctata radiation. Although these species are classified as generalists, their acceptable hosts include deadly Amanita species. In this study, we used behavioral assays to assess associations between one mushroom-feeding species, Drosophila guttifera, and the deadly Amanita phalloides. We conducted feeding assays to confirm the presence of cyclopeptide toxin tolerance. We then completed host preference assays in female flies and larvae and did not find a preference for toxic mushrooms in either. Finally, we assessed the effect of competition on oviposition preference. We found that the presence of a competitor\'s eggs on the preferred host was associated with the flies increasing the number of eggs laid on the toxic mushrooms. Our results highlight how access to a low competition host resource may help to maintain associations between a generalist species and a highly toxic host.
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  • 文章类型: Case Reports
    野生蘑菇中毒是全球公共卫生问题,含有阿马毒素的蘑菇是死亡的主要原因。Amanita和Galerina属的蘑菇含有阿马毒素。这里我们介绍了一个野生蘑菇中毒的案例,影响了三个人,导致两人死亡。食用后10-15小时内,他们出现了胃肠炎的症状,如呕吐,腹痛,和腹泻。一名人员迅速寻求医疗护理并康复,而另外两人在症状出现近两三天后寻求医疗帮助,到那时,他们的状况已经恶化并导致他们死亡。这些蘑菇被鉴定为Galerina属,实验室测试显示,从腐烂的残端不同部位收集的蘑菇中的毒素水平存在差异。较高水平的α-amanitin,β-amanitin,在树桩底部附近检测到γ-amanitin,但是在树桩顶部附近发现了微量的α-amanitin,而β-amanitin和γ-amanitin检测不到。该病例强调了在出现延迟发作的胃肠道症状时立即就医的重要性,因为这可能表明更严重的蘑菇中毒,尤其是amatoxin中毒.及时和适当的治疗同样重要。此外,在同一事件中食用不同单位的蘑菇会由于毒素水平的差异而导致不同的预后。
    Wild mushroom poisoning is a global public health concern, with mushrooms containing amatoxins being the main cause of fatalities. Mushrooms from the genus Amanita and Galerina contain amatoxins. Here we present a case of wild mushroom poisoning that affected three individuals, resulting in two fatalities. Within 10-15 hours after consumption, they experienced symptoms of gastroenteritis such as vomiting, abdominal pain, and diarrhea. One individual sought medical attention promptly and recovered, while the other two sought medical help nearly two or three days after the onset of symptoms, by which time their conditions had already worsened and led to their deaths. The mushrooms were identified belonging to genus Galerina, and laboratory test revealed variations in toxin levels among mushrooms collected from different parts of the decaying stump. The higher levels of α-amanitin, β-amanitin, and γ-amanitin were detected near the base of the tree stump, but trace levels of α-amanitin were found near the top of the stump, while β-amanitin and γ-amanitin were undetectable. This case emphasizes the importance of seeking immediate medical attention when experiencing delayed-onset gastrointestinal symptoms, as it may indicate more severe mushroom poisoning, particularly amatoxin poisoning. Timely and appropriate treatment is equally important. Additionally, consuming different units of the mushrooms in the same incident can lead to varying prognoses due to differences in toxin levels.
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  • 文章类型: Journal Article
    在人类中,由于代谢失衡和活性氧(ROS)的过量产生,已经引起了广泛的健康障碍。蘑菇中发现的不同生物学特性似乎是它们通常用作最喜欢的美味佳肴的原因。因此,今天,野生食用蘑菇作为各种生物化合物的来源的探索越来越重要。天牛,印度东部普遍消费的未充分利用的大型真菌之一,需要对其药用价值进行系统的研究。本研究旨在通过各种体外试验,探索A.konajensis乙醇提取物(EtAK1)的真菌化学含量,并筛选其抗氧化能力。GC-MS分析鉴定了EtAK1的化学组分。Further,基于结构的虚拟筛选鉴定的化合物进行了类似药物的性质和分子对接与人p38MAPK蛋白,人类肺癌的有效靶向途径。形态分子特征证明了收集的蘑菇的真实性。筛选试验表明EtAK1富含类黄酮,其次是酚类物质,β-胡萝卜素,还有番茄红素,具有较强的抗氧化活性,EC50值为640-710μg/mL。EtAK1的GC-MS分析确定蘑菇中存在19种生物活性化合物。硅分析显示,炭疽对氯苯甲酸酯,确定的化合物之一,显示与人p38MAPK的高结合亲和力(ΔG=-10.6kcal/mol)。这项研究的结果将为使用A.konajensis的myco药物的发明铺平道路,这可能导致一种治疗人类肺癌的新药。
    In humans, a wide range of health disorders have been induced due to an imbalanced metabolism and an excess generation of reactive oxygen species (ROS). Different biological properties found in mushrooms seem to be the reason for their customary use as a favourite delicacy. Therefore, exploration of wild edible mushrooms as a source of various biological compounds is gaining much importance today. Amanita konajensis, one of the underutilized macrofungi popularly consumed in Eastern India, demands a systematic study of its medicinal values. The study aims to explore the myco-chemical contents of A. konajensis ethanolic extract (EtAK1) and screen their antioxidant potency through various in vitro assays. GC-MS analysis identified the chemical components of EtAK1. Further, structure-based virtual screening of the identified compounds was analysed for drug-like properties and molecular docking with the human p38 MAPK protein, a potent targeting pathway for human lung cancer. The morpho-molecular features proved the authenticity of the collected mushroom. The screening assays showed that EtAK1 was abundant in flavonoids, followed by phenolics, β-carotene, and lycopene, and had strong antioxidant activity with EC50 values of 640-710 μg/mL. The GC-MS analyses of EtAK1 identified the occurrence of 19 bioactive compounds in the mushroom. In silico analysis revealed that anthraergostatetraenol p-chlorobenzoate, one of the compounds identified, displayed high binding affinity (ΔG = -10.6 kcal/mol) with human p38 MAPK. The outcome of this study will pave the way for the invention of myco-medicine using A. konajensis, which may lead to a novel drug for human lung cancer.
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  • 文章类型: Journal Article
    蛇毒蛇毒中毒占致命蘑菇中毒的大多数。最近,我们确定了血液毒性是天牛中毒的一个相关方面。在这项研究中,我们调查了鸡毒的主要毒素的影响,α-和β-amanitin,对体外造血细胞活力的影响。将造血细胞系暴露于α-amanitin或β-amanitin长达72小时,有或没有pan-caspase抑制剂Z-VAD(OH)-FMK,解毒剂N-乙酰半胱氨酸,水飞蓟宾,和青霉素,和有机阴离子转运多肽1B3(OATP1B3)抑制剂利福平和环孢菌素。通过锥虫蓝排除建立细胞活力,膜联蛋白V染色,和MTS分析。用Caspase-Glo测定法测定Caspase-3/7活性,和裂解的caspase-3通过Western分析定量。在暴露于原代CD34+造血干细胞中的α-amanitin后,定量细胞数量和集落形成单位。在所有细胞系中,α-amanitin浓度依赖性地降低了活力和线粒体活性。β-Amanitin毒性较小,但仍显著降低生存能力。α-Amanitin将caspase-3/7活性提高2.8倍,并将caspase-3裂解2.3倍。Z-VAD(OH)-FMK显着降低了α-amanitin诱导的毒性。在CD34+干细胞中,α-amanitin减少了集落和细胞的数量。解毒剂和OATP1B3抑制剂不能逆转α-amanitin诱导的毒性。总之,α-amanitin通过caspase依赖性机制诱导造血细胞凋亡。
    Amanita phalloides poisonings account for the majority of fatal mushroom poisonings. Recently, we identified hematotoxicity as a relevant aspect of Amanita poisonings. In this study, we investigated the effects of the main toxins of Amanita phalloides, α- and β-amanitin, on hematopoietic cell viability in vitro. Hematopoietic cell lines were exposed to α-amanitin or β-amanitin for up to 72 h with or without the pan-caspase inhibitor Z-VAD(OH)-FMK, antidotes N-acetylcysteine, silibinin, and benzylpenicillin, and organic anion-transporting polypeptide 1B3 (OATP1B3) inhibitors rifampicin and cyclosporin. Cell viability was established by trypan blue exclusion, annexin V staining, and a MTS assay. Caspase-3/7 activity was determined with Caspase-Glo assay, and cleaved caspase-3 was quantified by Western analysis. Cell number and colony-forming units were quantified after exposure to α-amanitin in primary CD34+ hematopoietic stem cells. In all cell lines, α-amanitin concentration-dependently decreased viability and mitochondrial activity. β-Amanitin was less toxic, but still significantly reduced viability. α-Amanitin increased caspase-3/7 activity by 2.8-fold and cleaved caspase-3 by 2.3-fold. Z-VAD(OH)-FMK significantly reduced α-amanitin-induced toxicity. In CD34+ stem cells, α-amanitin decreased the number of colonies and cells. The antidotes and OATP1B3 inhibitors did not reverse α-amanitin-induced toxicity. In conclusion, α-amanitin induces apoptosis in hematopoietic cells via a caspase-dependent mechanism.
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