Ganoderma lucidum spore oil enhances the effect of paclitaxel,improves the tolerance to paclitaxel and prolongs the survival in Lewis tumor-bearing mice

Purpose:This study aims to investigate whether Ganoderma lucidum spore oil(GLSO)could enhance the effect of paclitaxel(PTX),improve the tolerance to PTX and prolong the overall survival of Lewis tumor-bearing mice,which has never been reported before.Methods:The tumor,spleen,and thymus were weighed at the end of the experiment.Whole blood was collected for hematological index analysis,and the intact femur was removed to determine the bone marrow nucleated cell count(BMN).The percentage of lymphocytes in the spleen of mice was detected by flow cytometry,the activity of NK cells was detected by LDH assay,and the proliferation index of lymphocytes was determined by CCK-8 assay.The overall and mean survival time and life extension rate were calculated using SPSS software.Results:Our data showed that GLSO could enhance the anti-tumor effect of PTX and prolong the survival of mice.The underlying mechanisms of the above effects might be related to the toxic reduction effect of GLSO by relieving hematotoxicity,myelosuppression and immunosuppression.Specifically,GLSO could increase the number of blood cells and bone marrow cells,alleviate the thymic index,and elevate the number and activity of NK cells in mice treated with PTX.Conclusion:GLSO may enhance the efficacy of PTX by boosting the activity of immune NK cells and prolong survival by counteracting PTX-induced bone marrow alterations and improving hematopoiesis.These findings suggested the promising role of GLSO in combination with PTX to extend the survival and increase the tolerance of patients in clinical chemotherapy of lung cancer.

Ganoderma lucidum spore oil(GLSO),a novel antioxidant,extends the average life span in Drosophila melanogaster

In ancient China,Ganoderma lucidum was believed to be a medical fungus that could increase lifespan.Recently,pharmacologic studies have found that polysaccharide peptides and triterpenoids extracted from Ganoderma lucidum have various physiological effects as active compounds.However,the effects of spore oil isolated from Ganoderma lucidum remains unknown.In this study,the biological effects of Ganoderma lucidum spore oil(GLSO)were evaluated using a Drosophila melanogaster model.Compared with untreated groups,groups treated with GLSO had significantly longer average and maximum lifespan in both normal conditions and under oxidative stress.The activities of various antioxidant enzymes were measured to determine the antioxidant effect of GLSO.GLSO treatment markedly enhanced total superoxide dismutase(SOD)and catalase(CAT)activity and decreased levels of malondialdehyde(MDA).Further,we found dose-dependent increases in the mRNA expression of Cu,Zn-SOD,Mn-SOD,and CAT in GLSO-treated groups.These results suggest that GLSO may effectively eliminate free radicals and extend lifespan in Drosophila.Future work should investigate the value of GLSO as a functional food for the prevention of aging in larger animal models.

Volatile Components and Antitumor Activity of Ganoderma lucidum Spore Oil and Its Molecular Distillation Components

[Objectives]To compare the effects of molecular distillation on the flavor and antitumor activity of Ganoderma lucidum spore oil.[Methods]G.lucidum spore oil was separated and purified by molecular distillation technology,and the volatile components of different components of molecular distillation were analyzed by gas chromatography-ion mobility spectrometry(GC-IMS)technology.Human liver carcinoma cells(HepG2),human breast cancer cells(MCF-7),and human cervical cancer cells(Hela)were selected as the tumor cell lines to be tested,and the cell viability was detected by the MTT assay.[Results]Molecular distillation effectively reduced small molecular substances produced by oil oxidation in G.lucidum spore oil,such as heptanal,octanal,linalool,hexanal,E-2-octanal,3-ethylpyridine,etc.Among the heavy components,the content of esters was relatively high,mainly including ethyl levulinate,ethyl crotonate,and amyl butyrate.The MTT cytotoxicity test indicated that G.lucidum spore oil and its molecular distillation components had certain inhibitory effects on the growth of three tumor cells,and G.lucidum spore oil crude oil had the most significant antitumor activity.G.lucidum spore oil crude oil,heavy component,and light component had the most significant antitumor activity on HepG2 cells,followed by MCF-7 cells,and the weakest antitumor activity on Hela cells.The quality of G.lucidum spore oil became higher after molecular distillation,and the rancid smell was reduced,and molecular distillation had little effect on the antitumor activity of G.lucidum spores.[Conclusions]Molecular distillation technology can be applied to the refining of G.lucidum spore oil to improve product quality.

Bioactive components,pharmacological properties and underlying mechanism of Ganoderma lucidum spore oil:A review

Ganoderma lucidum is a Chinese medicinal fungus with a long history of use in healthcare and disease treatment.G.lucidum spores(GLS)are tiny germ cells released from the mushroom cap during the mature stage of growth.They contain all the genetic active substances of G.lucidum.G.lucidum spore oil(GLSO)is a lipid component extracted from broken-walled Ganoderma spores using supercritical CO_(2)extraction technology.GLSO contains fatty acids,Ganoderma triterpenes,sterols and other bioactive compounds.Previous studies have demonstrated that GLSO has a wide range of pharmacological properties,including anti-tumor,anti-aging,neuroprotection,immunomodulation,hepatoprotection and modulation of metabolic diseases.This review summarizes the research progress of GLSO over the past two decades in terms of its bioactive components,extraction and processing techniques,pharmacological effects and safety evaluation.This provides a solid foundation for further research and application of GLSO.

高压超临界CO_(2)萃取茶籽油、核桃油及灵芝孢子油及其对质量的影响研究

研究高压超临界CO_(2)萃取茶籽油、核桃油及灵芝孢子油萃取效率及其对产品质量的影响,并与常规萃取压力进行对比。在萃取温度40℃、分离压力11 MPa、分离温度50℃的萃取条件下,对比分析65、50、35 MPa的萃取压力条件对3种功能性油脂萃取效率的影响。通过GC-MS、HPLC法及相关理化指标测定,研究高压等不同萃取压力对3种油的脂肪酸组成、不皂化物成分、活性营养成分及理化指标等质量的影响。萃取压力对3种油脂的萃取效率有明显的差异,萃取压力越高,收率相应升高,油脂萃取效率也越高;高压等不同萃取压力对油脂脂肪酸组成几乎没有影响,但能显著提高角鲨烯等活性成分的萃取;从理化指标上看,高压萃取条件有助于降低食用油的酸值,提高油脂的品质。

灵芝孢子油缓解小鼠体力疲劳的作用及其机制研究

为了评价灵芝孢子油缓解小鼠体力疲劳的作用并探究其可能机制。将144只SPF级雄性KM小鼠随机分为4组,即溶剂对照组、灵芝孢子油低、中、高剂量组,每组36只,灌胃30 d。共分为4批,分别用于负重游泳实验(Ⅰ)、肝糖原(Ⅱ)、血乳酸(Ⅳ)以及血清尿素氮、肌糖原及其他指标(腓肠肌HE染色、PAS染色和TUNEL染色)测定(Ⅲ)。结果表明,与溶剂对照组相比,灵芝孢子油中剂量组小鼠负重游泳时间极显著延长(P<0.01);灵芝孢子油各剂量组小鼠的血清尿素氮水平均极显著降低(P<0.01);各组小鼠的肝糖原和肌糖原含量无显著差异(P>0.05);灵芝孢子油各剂量组小鼠的血乳酸曲线下面积均极显著降低(P<0.01)。腓肠肌HE染色结果显示各组均未见明显病理改变。PAS染色结果显示灵芝孢子油高剂量组肌糖原阳性面积显著增加(P<0.05)。TUNEL染色结果显示灵芝孢子油低剂量组凋亡细胞阳性率显著降低(P<0.05)。因此,在本实验条件下,灵芝孢子油具有缓解体力疲劳的作用,其机制可能与减少机体糖原消耗、减轻肌细胞凋亡有关。

灵芝孢子油的制备工艺研究

为探究灵芝孢子油制备工艺路线,考察了不同提取工艺影响,利用单因素及响应面试验优化超临界CO_(2)萃取工艺条件,研究分子蒸馏精制对灵芝孢子油质量的改善。结果表明,正己烷浸提与超临界CO_(2)萃取工艺所得灵芝孢子油提取率、三萜含量、酸价皆无显著差异;超临界CO_(2)萃取工艺中,前处理需进行制粒工艺,最佳萃取条件为温度50℃、压力28 MPa、时间3.5 h。此条件下小试灵芝孢子油得率为28.57%,中试得率为29.12%;经分子蒸馏后,灵芝孢子油的感观、酸价及塑化剂含量得到极大改善。

灵芝孢子油及添加维生素E灵芝孢子油对NRK-52E细胞氧化损伤的作用比较

灵芝孢子油是从灵芝孢子粉中提取的油状脂质物,其中的不饱和脂肪酸和三萜类灵芝酸是其主要活性成分。是由于其中的不饱和脂肪酸易氧化挥发,研究人员通过添加维生素E以求解决难题,但目前对添加维生素E的灵芝孢子油抗氧化应激活性的系统研究未见报道。因此选用灵芝孢子油(GLSO)及添加5%维生素E的灵芝孢子油(GLSO+VE)2种样品,作用于H2O2处理的大鼠肾小管上皮NRK-52E细胞,以评价、比较对氧化应激损伤的保护作用。结果表明,GLSO和GLSO+VE均能显著性增加NRK-52E细胞存活率,提高抗氧化酶的活性,降低氧化产物水平。比较可知添加维生素E可显著降低灵芝孢子油的细胞毒作用,并在一定程度上增加其抗氧化活性。此次试验初步证实了灵芝孢子油中添加维生素E对抗细胞氧化损伤的增强作用,为添加维生素E以增加灵芝孢子油稳定性的研究提供更多理论依据和支撑数据。

基于GC-Q-Exactive-MS的灵芝孢子油化学成分定性分析

目的:利用高分辨气相色谱-四级杆-静电轨道阱质谱法(GC-Q-Exactive-MS)定性分析灵芝孢子油的化学成分。方法:采用GC-Q-Exactive-MS,在电子轰击(EI)源下获取化合物的全扫描质谱数据,通过总结脂肪酸类、萜类、甾醇类及醛类化学成分的质谱裂解规律,并检索NIST、MassBank、HMDB、PubChem在线数据库及查阅相关文献,对灵芝孢子油的各类化学成分进行鉴定。结果:从灵芝孢子油中共鉴定了22个化学成分,包括3个脂肪酸类、4个萜类、4个甾醇类、4个醛类及7个其他类化合物。结论:研究结果为灵芝孢子油质量控制和中药弱极性化学成分定性分析提供了参考。

不同干燥方式对灵芝孢子粉中灵芝孢子油过氧化值的影响

目的:比较不同干燥方式对灵芝孢子粉中灵芝孢子油过氧化值的影响。方法:以西藏灵芝孢子粉为例,采用不同的干燥方式将灵芝孢子粉干燥至合格,然后进行破壁,用超临界CO_(2)萃取法提取灵芝孢子油,检测灵芝孢子油的过氧化值,并比较不同干燥方式对灵芝孢子油的过氧化值的影响。结果:微波干燥和真空干燥方式得到的灵芝孢子油过氧化值均合格,分别为0.13%,0.14%;热风干燥和晾晒干燥方式得到的灵芝孢子油过氧化值不合格,分别为0.16%、0.17%。结论:水分变化率可能是灵芝孢子粉干燥过程中的重要影响因素,微波干燥方式水分变化率远高于其他方式,干燥效率高,耗能少,且不影响孢子油过氧化值,适合干燥大规模样品;其它干燥方式相对比较费时耗能,且灵芝孢子粉存在变质的风险。

灵芝孢子油增强小鼠免疫功能及护肝作用的实验研究

[目的]探讨灵芝孢子油对小鼠免疫功能的影响及对肝脏的保护作用。[方法](1)免疫功能实验:昆明种小鼠经口连续分别给予0.17、0.33、1.00 g/kg BW的灵芝孢子油及粟米油(溶剂对照组)30 d,进行迟发型变态反应试验、淋巴细胞转化试验、NK细胞活性测定;(2)护肝作用实验:昆明种小鼠经口连续分别给予0.17、0.33、1.00g/kg BW的灵芝孢子油及粟米油(溶剂对照)30 d后,腹腔注射CCl4以诱发小鼠化学性肝损伤,测定谷丙转氨酶(ALT)和谷草转氨酶(AST)及观察肝脏病理组织学变化。[结果](1)免疫功能实验:与空白对照组比较,中、高剂量组迟发型变态反应能力,脾淋巴细胞转化能力及脾NK细胞活性均增强,差异有统计学意义(P﹤0.05);(2)护肝功能实验:与CCl4对照组比较,各剂量组血清谷丙转氨酶、谷草转氨酶及肝脏病理组织学变化均减轻,差异有统计学意义(P﹤0.05)。[结论]灵芝孢子油对小鼠细胞免疫功能和NK细胞活性有明显的促进作用,对CCl4诱导的化学性肝损伤具有辅助保护作用。

超临界CO2静态膨胀-动态循环萃取灵芝孢子油

为了直接从未破壁的灵芝孢子中萃取油脂,在超临界CO2动态循环萃取之前引入静态膨胀工艺,考察了各膨胀因素对灵芝孢子油萃取率的影响。试验结果表明,膨胀压力越高,膨胀时间越短,静态萃取时间越长,越有利于灵芝孢子油的萃取,而膨胀温度过高或过低均不利于灵芝孢子油的萃取。超临界CO2静态膨胀-动态循环萃取灵芝孢子油的优化工艺为:膨胀压力30MPa,膨胀时间30s,膨胀温度70℃,静态萃取时间20min,在此条件下灵芝孢子油的萃取率达94.3%。

灵芝孢子油化学成分研究

【目的】研究灵芝孢子油的化学成分。【方法】采用硅胶色谱技术、制备液相色谱技术和Sephadex LH-20色谱技术分离化学成分,核磁共振扫描(NMR)、质谱分析法(MS)、甲酯化气相色谱法等方法鉴定化合物。【结果】得到6个化合物,分别为1-0-十八碳烷酰-2-0-(9Z-十八碳烯酰)-3-0-(9Z-十八碳烯酰)甘油酯(1)、1-0-十六碳烷酰-2-0-(9Z-十八碳烯酰)-3-0-(9,12Z-十八碳二烯酰)甘油酯(2)、1-0-(9Z-十八碳烯酰)-2-0-(9Z-十八碳烯酰)-3-0-(9,12Z-十八碳二烯酰)甘油酯(3)、1-0-(11Z-十八碳烯酰)-2-0-(9Z-十八碳烯酰)-3-0-(9Z-十八碳烯酰)甘油酯(4)、1-0-(11Z-十八碳烯酰)-2-0-(9Z-十八碳烯酰)-3-0-(9,12Z-十八碳二烯酰)甘油酯(5)、十八碳烷酸(6)。【结论】化合物1～5为首次从该属中分离得到,化合物6为首次从灵芝孢子油中分离得到。

灵芝孢子油对小鼠血清SOD、CAT活性及C3、P21mRNA表达的影响

目的:探讨灵芝孢子油对D-半乳糖所致衰老模型小鼠抗衰老作用及其作用机理。方法:以D-半乳糖建立小鼠衰老模型,灌胃灵芝孢子油900mg/(kg.d)45d后,检测小鼠血清中血清超氧化物歧化酶(SOD)、过氧化氢酶(CAT)活性;检测脾脏指数、胸腺指数;半定量PCR检测脾脏、胸腺中C3、P21 mRNA表达。结果:DB组(D-半乳糖+灵芝孢子油)SOD、CAT的活性显著高于DY组(D-半乳糖+玉米油)(P≤0.01),DB组脾脏指数、胸腺指数显著高于DY组(P≤0.05)。C3mRNA在脾脏、胸腺中的表达DB组显著高于DY组(P≤0.05),C3mRNA在胸腺中的表达SB组(生理盐水+灵芝孢子油)高于SY组(生理盐水+玉米油)(P≤0.05);P21mRNA在脾脏中的表达DB组低于DY组(P≤0.05),SB组低于SY组(P≤0.05)。结论:灵芝孢子油可提高小鼠脾脏指数、胸腺指数、SO D、C AT活性,具有抗氧化功能;能促进C3 mR NA的表达,抑制P 21 mR NA的表达。

灵芝孢子油干预治疗6-羟多巴帕金森病大鼠模型的实验研究

【目的】研究灵芝孢子油对6-羟多巴(6-OHDA)帕金森病(PD)大鼠模型行为学及病理改变的影响,探讨该药对黑质多巴胺能神经元的保护作用。【方法】100只SD大鼠随机分为正常对照组20只、6-OHDA组40只、灵芝孢子油+6-OHDA组40只。通过脑部立体定向法将6-OHDA注射到SD大鼠一侧黑质致密部建立6-OHDA大鼠PD模型,灵芝孢子油+6-OHDA组在造模前3d开始给灵芝孢子油每天500mg/kg,连续10d。6-OHDA组喂食生理盐水做对照。造模后每周给予阿朴吗啡观察大鼠旋转行为的变化,4周后用高效液相色谱法检测大鼠纹状体多巴胺及其代谢物含量,免疫组织化学法检测黑质致密部酪氨酸羟化酶(TH)阳性细胞数量,westernblot法对TH蛋白进行半定量测定。【结果】①灵芝孢子油+6-OHDA组出现旋转行为的大鼠比例为10%,6-OHDA组为45%,两组比较有显著性差异。②纹状体多巴胺及其代谢物含量在两组间存在差异,多巴胺手术侧含量/手术对侧含量在灵芝孢子油+6-OHDA组为(60.12±7.5)%,在6-OHDA组为(38.58±7.26)%。③在黑质致密带区灵芝孢子油+6-OHDA组的TH免疫阳性细胞及TH蛋白表达量均较6-OHDA组显著增多。【结论】灵芝孢子油能明显改善6-OHDA大鼠模型行为学,增加纹状体多巴胺及其代谢物含量并提高黑质多巴胺能神经元的残存率,提示灵芝孢子油可能具有减缓PD病变进程的神经保护作用。

灵芝孢子油中脂溶性维生素含量及其体外抗氧化活性研究

采用超临界CO2流体萃取灵芝孢子油,在压力30 MPa和温度40℃条件下进行萃取(CO2流量25 L/h,时间2.0 h),在8 MPa和45℃条件下进行分离,灵芝孢子油的平均得率为24.35%,提取率达95.08%。高效液相色谱分析结果表明:灵芝孢子油中的脂溶性维生素D2、维生素D3、维生素E的含量分别为15.13、14.68、7.15μg/g。体外抗氧化活性检测结果表明:灵芝孢子油具有较强的DPPH自由基和超氧阴离子自由基清除能力,并且呈明显的剂量效应关系;当样品质量浓度达800μg/mL时,对DPPH自由基和超氧阴离子自由基的清除率可达89.1%和41.3%,较接近于抗氧化剂BHT和芦丁;但对ABTS自由基的清除作用较弱。

灵芝孢子油及灵芝提取物孢子油对乳腺癌血管生成调节因子的作用

目的探讨灵芝孢子油及灵芝提取物孢子油对人源高恶性乳腺癌血管生成调节因子的作用。方法不同剂量的灵芝孢子油、灵芝提取物孢子油分别刺激体外培养的人源高恶性乳腺癌细胞系MDA-MB-231细胞及MDA-MB-231细胞制作的荷廇小鼠,Western blotting检测表皮生长因子受体(EGFR)的蛋白表达变化,Real-time PCR检测肿瘤血管生成相关因子EGFR、血管内皮生长因子(VEGF)、基质金属蛋白酶(MMPs)、血小板反应素-1(TSP-1)、血小板衍生因子(PDGF)、成纤维细胞生长因子(FGF)转录水平的基因表达变化。结果灵芝孢子油、灵芝提取物孢子油均可在体内和体外抑制人源高恶性乳腺癌细胞MDA-MB-231的EGFR蛋白表达,且有剂量依赖性;均可在体内和体外抑制VEGF RNA表达,增强血管生成抑制因子TSP-1 RNA表达;灵芝提取物孢子油比灵芝孢子油的作用更为显著。结论灵芝孢子油、灵芝提取物孢子油均有抑制肿瘤血管生成因子表达和促进血管生成抑制因子表达的作用,其中灵芝提取物孢子油比灵芝孢子油的作用更为显著。

灵芝孢子油的研究进展

综述了近年来有关灵芝孢子油组成、提取、药理作用等方面的研究进展。

灵芝孢子油的提取及脂肪酸检测

采用索氏抽提法、超临界CO_2萃取法、微波提取法和超声波提取法对灵芝孢子油进行提取,提取率分别为33.15%、27.89%、27.23%和28.92%。采用超声波提取法得到的灵芝孢子油分别采用碱法、酸法和酸碱结合3种甲酯化方法处理后,用气相色谱-质谱联用仪进行分析。结果显示,酸碱结合甲酯化后得到的脂肪酸种类最多,达到19种。

不同破壁技术对灵芝孢子油提取的影响

通过比较酸热法、超声波冻融法和高能纳米冲击磨法对灵芝孢子粉破壁效果,找到适合工业化生产的孢子油提取的最佳破壁技术。结果显示:采用高能纳米冲击磨法可显著提高灵芝孢子的破壁率和孢子油得率,在球料比3∶1(质量比),球磨时间6 h的条件下,破壁率为90.36%,灵芝孢子油得率为30.79%。