Effect of coenzyme Q10 supplementation on post-vitrification mouse embryo development

Objective:To investigate the effects of coenzyme Q10(CoQ10)supplementation on post-vitrification embryo development and gross morphology.Methods:Balb/c mouse embryos were cultured in potassium simplex optimised medium(KSOM)with varying CoQ10 concentrations[0(control),20,40,and 60μM].The most effective CoQ10 concentration(40μM)was selected for subsequent post-vitrification morphology study.Embryos were randomly divided into four groups:Group A(non-vitrified without CoQ10),Group B(non-vitrified with CoQ10),Group C(vitrified without CoQ10),and Group D(vitrified with CoQ10),followed by vitrification at the 8-cell stage.Survival rates and development until the blastocyst stage were evaluated through morphological examinations using ASEBIR's system,distinguishing normal and abnormal embryos.Results:Supplementation of 40μM CoQ10 significantly increased blastocyst formation(95%)compared to the control group(92%),20μM(62%),and 60μM(56%)(P<0.001).Following vitrification,Group D exhibited a significant increase in blastocyst formation(92%)compared to Group C(82%)(P<0.05).Morphological assessments indicated superior embryo quality in Group B over Group D during the cleavage stage,morula,and blastocyst(P<0.05).Conclusions:CoQ10 supplementation exhibits promising potential to enhance preimplantation embryo development,increase blastocyst formation rates,and improve embryo quality post-vitrification.This offers a promising approach to mitigate oxidative stress on embryos,potentially improving overall assisted reproductive technology outcomes.

Effects of dietary coenzyme Q10 supplementation during gestation on the embryonic survival and reproductive performance of high‑parity sows

Background Fertility declines in high-parity sows.This study investigated whether parity-dependent declines in embryonic survival and reproductive performance could be restored by dietary coenzyme Q10(CoQ10)supplementation.Methods Two experiments were performed.In Exp.1,30 young sows that had completed their 2nd parity and 30 high-parity sows that had completed their 10^(th)parity,were fed either a control diet(CON)or a CON diet supple-mented with 1 g/kg CoQ10(+CoQ10)from mating until slaughter at day 28 of gestation.In Exp.2,a total of 314 post-weaning sows with two to nine parities were fed the CON or+CoQ10 diets from mating throughout gestation.Results In Exp.1,both young and high-parity sows had a similar number of corpora lutea,but high-parity sows had lower plasma CoQ10 concentrations,down-regulated genes involved with de novo CoQ10 synthesis in the endome-trium tissues,and greater levels of oxidative stress markers in plasma and endometrium tissues.High-parity sows had fewer total embryos and alive embryos,lower embryonic survival,and greater embryo mortality than young sows.Dietary CoQ10 supplementation increased the number of live embryos and the embryonic survival rate to levels simi-lar to those of young sows,as well as lowering the levels of oxidative stress markers.In Exp.2,sows showed a parity-dependent decline in plasma CoQ10 levels,and sows with more than four parities showed a progressive decline in the number of total births,live births,and piglets born effective.Dietary supplementation with CoQ10 increased the number of total births,live births,and born effective,and decreased the intra-litter covariation coefficients and the percentage of sows requiring farrowing assistance during parturition.Conclusions Dietary CoQ10 supplementation can improve the embryonic survival and reproductive performance of gestating sows with high parity,probably by improving the development of uterine function.

辅酶Q_(10)在卵母细胞衰老与辅助生殖领域的研究进展

辅酶Q_(10)是线粒体呼吸链中重要递氢体,其作为常见的抗氧化剂广泛应用于临床多个领域。氧化应激导致的线粒体功能障碍是造成卵母细胞衰老的重要原因,而卵母细胞衰老是生育能力下降的重要标志。辅助生殖技术作为治疗不孕症的主要手段,可大大提高低生育人群的妊娠率。辅酶Q_(10)能够延缓卵巢储备消耗,促进卵母细胞成熟,从而提高妊娠率。此外,辅酶Q_(10)能改善患者卵巢对刺激的反应,并改善卵母细胞和胚胎质量,有助于提高辅助生殖技术的成功率。

Advances in the Coenzyme Q10 Biosynthesis Pathway in Rhodobacter sphaeroides and the Enhancement of Coenzyme Q10 Production Based on Metabolic Engineering

Coenzyme Q10 is widely used in food,cosmetics and pharmaceuticals,possessing a broad market.Rhodobacter sphaeroides is enriched in natural coenzyme Q10 and is becoming an important microorganism for producing natural coenzyme Q10.The paper reviewed the biosynthesis pathways of coenzyme Q10 in R.sphaeroides and the advances in enhancement of coenzyme Q10 production in R.sphaeroides based on metabolic engineering.

Evidence on neuroprotective properties of coenzyme Q10 in the treatment of glaucoma

Glaucoma, the leading cause of visual impairment and irreversible blindness worldwide, is a multifactorial, progressive optic neuropathy characterized by loss of retinal ganglion cells, alterations of the optic nerve head, and specific visual field defects. Clinical evidence shows that intraocular pressure is the major risk factor of the treatable disease. However, in some patients, glaucoma develops and continues to progress despite normal intraocular pressure values, suggesting that other risk factors are involved in the disease. Consequently, neuroprotective treatments, focused on preventing retinal ganglion cells death by acting on different therapeutic strategies but not focused on intraocular pressure reduction, has therefore become of great interest. In this contest, coenzyme Q10, showing evidence in slowing or reversing pathological changes typical of the disease, has been proposed as a potential neuroprotective agent in glaucoma. In this review, we describe the possible mechanisms of action of coenzyme Q10 and the recent evidence in literature regarding the neuroprotective activity of the molecule.

Breeding of Coenzyme Q_(10) Produced Strain by Low-Energy Ion Implantation and Optimization of Coenzyme Q_(10) Fermentation

In order to increase the production efficiency of coenzyme Q10, the original strain Agrobacterium tumefaciens ATCC 4452 was mutated by means of Nitrogen ions implantation. A mutant strain, ATX 12, with high contents of coenzyme Q10 was selected. Subsequently, the conditions such as carbohydrate concentration, nitrogen source concentration, inoculum＇s size, seed age, aeration and temperature which might affect the production of CoQ10 were investigated in detail. Under optimal conditions, the maximum concentration of the intracellular CoQ10 reached 200.3 mg/L after 80 h fed-batch fermentation, about 245% increasing in CoQ10 production after ion implantation, compared to the original strain.

Plasma coenzyme Q10 levels in type 2 diabetic patients with retinopathy

AIMTo determine the relationship between proliferative diabetic retinopathy (PDRP) and plasma coenzyme Q10(CoQ10) concentration.

Validation and application of Vierordt’’s spectrophotometric method for simultaneous estimation of tamoxifen/coenzyme Q10 in their binary mixture and pharmaceutical dosage forms

For the sake of improving patient compliance and sustainability of chemotherapy healthcare system, both TC and CoQ10 were formulated as solid lipid nanoparticles (SLNs). The study was focused on establishing and validating a simple and reproducible spectrophotometric method for simultaneous determination of TC and CoQ10 in their binary mixture or pharmaceutical dosage forms. A new method based on simultaneous estimation of drug mixture without prior separation was developed. Validation parameters were checked with International Conference on Harmonization (ICH) guidelines. The accuracy and reproducibility of proposed method was statistically compared to HPLC. The TC and CoQ10 were quantified at absorptivity wavelengths of 236 nm and 275 nm, respectively. Calibration curves obeyed Beer’s law in range of 2–14 μg/ml with a correlation coefficient (R^2) of 0.999 in both methanol and simplified simulated intestinal fluid (SSIF). The %means recovery of TC and Co Q10 in pure state or binary mixture at various concentration levels were all around 100%.The low values of SD and %RSD (<2%) confirm high precision and accuracy of the proposed method. Formulated SLNs showed different %means recovery in range 81–92% for TC and 32–59% for CoQ10. The data obtained by applying simultaneous Vierordt’s equations showed no statistical significance in comparison to HPLC. Vierordt’s method was successfully applied as a simple, accurate, precise, and economical analysis method for estimating TC and CoQ10 concentrations in pure state, binary mixture and pharmaceutical dosage forms.

Coenzyme Q10 in neurodegenerative disorders: Potential benefit of Co Q10 supplementation for multiple system atrophy

Coenzyme Q10(Co Q10) is an essential cofactor in the mitochondrial respiratory pathway and also functions as a lipid-soluble antioxidant. Co Q10 deficiency has been implicated in many clinical disorders and aging. Primary Co Q10 deficiency is a group of recessively inherited diseases caused by mutations in any gene involved in the Co Q10 biosynthesis pathway. Although primary Co Q10 deficiency is rare, its diagnosis is important because it is potentially treatable with exogenous Co Q10. Multiple system atrophy(MSA) was recently shown to be linked to mutations in the COQ2 gene, one of the genes involved in the Co Q10 biosynthesis pathway. MSA is relatively common in adult-onset neurodegenerative diseases characterized by Parkinsonism, cerebellar ataxia and autonomic failures. Because COQ2 mutations are associated with an increased risk of MSA, oral Co Q10 supplementation may be beneficial for MSA, as for other primary Co Q10 deficiencies. Statins are 3-hydroxy-3-methylglutaryl coenzyme A inhibitors that inhibit the biosynthesis of cholesterol, as well as the synthesis of mevalonate, a critical intermediate in cholesterol synthesis. Statin therapy has been associ-ated with a variety of muscle complaints from myalgia to rhabdomyolysis. Statin treatment carries a potential risk of Co Q10 deficiency, although no definite evidence has implicated CQ10 deficiency as the cause of statinrelated myopathy.

Coenzyme Q10 as a therapeutic candidate for treating inherited photoreceptor degeneration

Inherited photoreceptor degeneration（IPD）：The human retina is a highly specialised tissue that enables the perception of light across a range of intensities and colours.It covers about65%of the inner surface of the eye and contains three layers of cells：the outer nuclear layer（ONL）containing the cell bodies and nuclei of the light-sensitive rod and cone photoreceptorswhose photopigment-containing outer segments form the photoreceptor layer; the inner nuclear layer （INL） containing bipolar, horizontal and amacrine cells; and the ganglion cell layer （GCL） from which the optic nerve arises. There are two layers of synaptic connections between these three layers： the photoreceptors synapse with second order neurons, mainly bi- polar cells, in the outer plexiform layer （OPL）, while in turn the bipolar cells form connections in the inner plexiform layer （IPL） with ganglion cells. The retinal pigment epithelium （RPE） lies directly behind the photoreceptor layer, is heavily pigmented to reduce scattering of light, and is essential for the nourishment, maintenance and metabolism of photoreceptors.

Effect of levocarnitine+coenzyme Q10 adjuvant therapy on vasoactive molecules,endothelial injury and oxidative stress in patients with chronic heart failure

Objective: To study the effect of levocarnitine + coenzyme Q10 adjuvant therapy on vasoactive molecules, endothelial injury and oxidative stress in patients with chronic heart failure. Methods: A total of 90 patients with chronic heart failure who were treated in the hospital between December 2014 and December 2016 were collected and divided into control group and observation group by random number table method, 45 cases in each group. Control group received conventional therapy, and observation group received levocarnitine + coenzyme Q10 adjuvant therapy on the basis of conventional therapy. The differences in vasoactive molecule, endothelial injury and oxidative stress levels were compared between the two groups before and after treatment. Results: Before treatment, the differences in vasoactive molecule, endothelial injury and oxidative stress levels were not statistically significant between the two groups of patients. After treatment, serum vasoactive molecules ET-1, AngⅡ and TXB2 contents of observation group were lower than those of control group while NO content was higher than that of control group;endothelial function indexes FMD level was higher than that of control group;serum oxidative stress indexes SOD and T-AOC contents were higher than those of control group while MDA and ROS contents were lower than those of control group. Conclusion: Levocarnitine + coenzyme Q10 adjuvant therapy can optimize the vascular activity, and reduce the endothelial injury and systemic oxidative stress response in patients with chronic heart failure.

辅酶Q_(10)联合牙周基础治疗对2型糖尿病伴发慢性牙周炎患者龈沟内炎症因子和糖代谢水平的影响

目的:针对罹患2型糖尿病的慢性牙周炎患者,开展牙周基础治疗后口服辅酶Q_(10)3个月,观察其牙周临床指数、龈沟内炎症因子及机体糖代谢水平的变化情况。方法:选取60例患有2型糖尿病的慢性牙周炎患者,随机将其分为观察组、对照组,每组30例。对照组仅实施常规牙周基础治疗,观察组在其基础上辅助口服辅酶Q_(10)3个月。两组均在完成各自治疗计划后第6个月复诊,比较牙周临床指数(PD、AL和SBI)、龈沟内炎症因子(IL-1β、IL-6)水平和糖代谢(FBG、HbA1c)水平。结果:(1)治疗前,两组PD、AL和SBI水平无统计学差异(P>0.05);复诊时,两组PD、AL、SBI均较治疗前显著降低(P<0.05),且观察组较对照组更低(P<0.05)。(2)治疗前,两组龈沟内IL-1β和IL-6的浓度无统计学差异(P>0.05);复诊时,两组IL-1β、IL-6均较治疗前降低(P<0.05),且观察组低于对照组(P<0.05)。(3)治疗前,两组FBG、HbA1c均无统计学差异(P>0.05);复诊时,两组FBG、HbA1c均显著低于治疗前(P<0.05),且观察组低于对照组(P<0.05)。结论:相较于单纯的牙周基础治疗,联合口服辅酶Q_(10)对于2型糖尿病的慢性牙周炎患者牙周临床指数、龈沟内炎症因子水平和机体糖代谢情况的控制和改善更显著有效。

辅酶Q-10对于抗精神病药物所致心电图异常的影响

此次研究主要试图利用辅酶Q - 10的改善心肌能量代谢及其功能的作用,对住院服用抗精神药物的患者同时投入辅酶Q - 10 ,并观察其心电图的情况,分析其在精神科临床的使用价值。

结直肠癌中辅酶Q_(10)的功能及分子机制探讨

目的:探索辅酶Q_(10)(coenzyme Q_(10),CoQ_(10))对结直肠癌细胞增殖和迁移能力的影响及潜在分子机制。方法:使用CoQ_(10)分别处理SW480细胞和RKO细胞后,采用细胞计数和细胞划痕实验探究CoQ_(10)对结直肠癌细胞增殖和迁移能力的影响;采用流式细胞术探究CoQ_(10)对结直肠癌SW480细胞周期和细胞凋亡的影响;采用RNA-seq测序分析CoQ_(10)对结直肠癌RKO细胞系基因表达谱的影响,将差异表达基因进行GO和KEGG通路分析,最后采用定量RT-PCR验证RNA-seq结果。结果:(1)CoQ_(10)对结直肠癌细胞系SW480的细胞增殖、细胞周期、细胞凋亡和细胞迁移均无明显影响,对结直肠癌细胞系RKO的细胞增殖也无明显影响,但可抑制RKO细胞迁移。(2)CoQ_(10)处理结直肠癌RKO细胞后的RNA-seq结果表明,差异表达基因明显富集于细胞黏附分子信号通路、细胞外基质受体信号通路和胆固醇信号通路等。定量RT-PCR验证结果表明,CoQ_(10)处理确实可导致胆固醇合成通路中的PCSK9、HMGCR、HMGCS1和DHCR7基因表达明显上调,提示CoQ_(10)可能通过调节这些基因的表达来抑制结直肠癌细胞RKO的迁移。结论:CoQ_(10)对结直肠癌细胞的增殖无明显影响,但可通过参与调节胆固醇代谢而抑制部分结直肠癌细胞的迁移能力。

软糖中辅酶Q_(10)含量检测方法研究

本研究采用HPLC法,测定软糖基质辅酶Q_(10)含量,通过筛选提取溶剂、溶解软糖的用水量、溶剂提取次数,确定检测软糖中辅酶Q_(10)含量测定的前处理方法,并进行相关的方法学验证。通过检测限、定量限、线性、精密度和准确度的试验,证明本研究所采用的方法能满足软糖中辅酶Q_(10)含量测定的要求。

前体物质对辅酶Q_(10)生物合成的影响

首次研究了以辅酶Q10 (CoQ10 )主要侧链供给前体物质———茄尼醇和醌环供给前体———羟基苯甲酸和辅酶Q0 对粟酒裂殖酵母(Schizosaccharomycespromb 2 1794 - 2 3) 生产CoQ10 产量的影响,并对前体的转化工艺进行了初步研究。确定了适宜于粟酒裂殖酵母生长及高转化前体生成CoQ10 的条件为:酵母在2 8℃下,2 2 0r/min于发酵培养基中培养18h后,加入0 5 g/L茄尼醇继续发酵培养18h ,进行前体转化反应。结果表明,单独添加茄尼醇能达到最大产量33 1mg/L ,比对照样品增加了91% ,任2种前体物质共同添加都要比单独添加茄尼醇时产量低。茄尼醇和CoQ0 共同添加时,单位细胞胞外辅酶CoQ10 的产量达到最高的1 35mg/g ,比对照样品增加了117%。

人血浆中辅酶Q_(10)的HPLC测定法及其动态研究

目的：建立人血浆中辅酶Ｑ１０的高效液相色谱检测法，以测定人体内辅酶Ｑ１０的经时变化过程。方法：血浆经无水乙醇沉淀蛋白后，以正己烷提取，进行高效液相色谱法检测。色谱柱为ＳｐｈｅｒｉｓｏｒｂＣ１８１０μｍ２５ｃｍ×４６ｍｍＩＤ，流动相为无水乙醇—水—冰醋酸（９８∶２∶０７），检测波长为２７５ｎｍ，内标为辅酶Ｑ９。结果：在０２～４０μｇ·ｍｌ－１浓度范围内峰面积比与浓度呈良好的线性关系，γ＝０９９９８，方法重现性好，提取回收率大于９０％；以本法测定了８名男性健康受试者服用辅酶Ｑ１０制剂前后血浆中辅酶Ｑ１０的浓度经时变化过程。结论：用本法测定人血浆中辅酶Ｑ１０浓度结果满意；人血浆中内源性辅酶Ｑ１０浓度为（７６３３±８６３）ｎｇ·ｍｌ－１。

利用广谱性和特异性组合诱变技术选育辅酶Q_(10)高产菌

为提高辅酶Q10产量,采用了对细胞进行全面的非特异性诱变和针对特定途径的特异性诱变相结合的育种策略.以放射型根瘤菌(Rhizobium radiobacter)WSH2601为出发菌株,选择UV射线和亚硝基胍作为诱变剂,在筛选获得放线菌素D抗性突变株的基础上,通过进一步的诱变处理,分别获得了放线菌素D和L-乙基硫氨酸双抗性突变株、放线菌素D和维生素K3双抗性突变株,以及抗放线菌素D和X-gal利用能力提高的突变株.与出发菌株相比,突变株辅酶Q10的产量提高幅度达25%～37%.其中一株放线菌素D和L-乙基硫氨酸双抗性突变株WSH-E25,胞内辅酶Q10含量和辅酶Q10总产量分别达到2.86 mg g DCW-1和40.0 mg L-1,均比出发菌株提高了37%,且遗传稳定性良好.