Gonadotropins

促性腺激素
  • 文章类型: Journal Article
    卵巢颗粒细胞对促性腺激素调节的雌激素产生至关重要,女性周期维持和生育能力。上皮Na+通道(ENaC)与女性生育能力有关;然而,它是否以及如何在卵巢细胞功能中发挥作用仍有待探索。这里,我们报道了人和小鼠卵巢颗粒细胞中ENaC表达和通道活性的膜片钳和Na+成像检测,由垂体促性腺激素促进,卵泡刺激素(FSH)或黄体生成素(LH)。小鼠中基于Cre重组酶和CRISPR-Cas9的颗粒特异性敲除ENaCα亚基(Scnn1a)导致早期发情时雌激素升高失败,黄体数量减少,异常延长的发情期,减少成年雌性小鼠的产仔数和低生育力。使用包括RNA测序和Ca2+成像在内的技术进行的进一步分析显示,基于shRNA的敲除或ENaC的敲除减少了自发或受刺激的Ca2振荡,降低了细胞内Ca2储存的能力,并损害了FSH/LH刺激的转录组变化,从而在小鼠和/或人颗粒细胞中产生雌激素。一起,这些结果揭示了ENaC在调节颗粒细胞中的促性腺激素信号以促进雌激素稳态和女性生育能力方面的作用。
    Ovarian granulosa cells are essential to gonadotrophin-regulated estrogen production, female cycle maintenance and fertility. The epithelial Na+ channel (ENaC) is associated with female fertility; however, whether and how it plays a role in ovarian cell function(s) remained unexplored. Here, we report patch-clamp and Na+ imaging detection of ENaC expression and channel activity in both human and mouse ovarian granulosa cells, which are promoted by pituitary gonadotrophins, follicle stimulating hormone (FSH) or luteinizing hormone (LH). Cre-recombinase- and CRISPR-Cas9-based granulosa-specific knockout of ENaC α subunit (Scnn1a) in mice resulted in failed estrogen elevation at early estrus, reduced number of corpus luteum, abnormally extended estrus phase, reduced litter size and subfertility in adult female mice. Further analysis using technologies including RNA sequencing and Ca2+ imaging revealed that pharmacological inhibition, shRNA-based knockdown or the knockout of ENaC diminished spontaneous or stimulated Ca2+ oscillations, lowered the capacity of intracellular Ca2+ stores and impaired FSH/LH-stimulated transcriptome changes for estrogen production in mouse and/or human granulosa cells. Together, these results have revealed a previously undefined role of ENaC in modulating gonadotrophin signaling in granulosa cells for estrogen homeostasis and thus female fertility.
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  • 文章类型: Journal Article
    背景:分泌型卷曲相关蛋白(SFRP)包含WNT信号拮抗剂家族,其在卵巢中的作用知之甚少。以前发现Sfrp4-null小鼠由于颗粒细胞对促性腺激素的反应增强而肥沃,导致窦卵泡闭锁减少和排卵率提高。本研究旨在阐明SFRP4拮抗FSH作用的机制。
    方法:用FSH和/或SFRP4处理来自野生型小鼠的颗粒细胞的原代培养物,并且通过RT-qPCR和RNAseq评价处理对基因表达的影响。进行生物信息学分析以分析SFRP4对转录组的影响,并将它们与FSH或FOXO1的组成型活性突变体进行比较。来自野生型或Sfrp4-null小鼠的其他颗粒细胞培养物,一些用特定信号效应物的药物抑制剂预处理,用于检查FSH和/或SFRP4对信号通路的影响,蛋白质印迹和TUNEL的自噬和凋亡。
    结果:发现用重组SFRP4处理培养的颗粒细胞可降低FSH靶基因的基础和FSH刺激的mRNA水平。出乎意料的是,发现这种效应既不通过规范(CTNNB1依赖性)也不通过规范的WNT信号机制发生,但被发现是GSK3β依赖性的。相反,发现SFRP4通过涉及AMPK的机制使AKT活性前变性。这导致FOXO1的低磷酸化和FSH和FOXO1转录组的一部分的表达减少。相反,FSH刺激的AMPK,发现相对于野生型对照,Sfrp4缺失小鼠的颗粒细胞中的AKT和FOXO1磷酸化水平增加。SFRP4处理颗粒细胞还通过经由AKT-mTORC1-ULK1的信号传导诱导自噬以及细胞凋亡。
    结论:本研究确定了一种新的GSK3β-AMPK-AKT信号机制,SFPR4通过该机制拮抗FSH作用,并进一步鉴定SFRP4为颗粒细胞自噬的新型调节因子。这些发现为先前在Sfrp4-null小鼠中观察到的表型变化提供了机制基础,并拓宽了我们对卵巢中WNT信号传导过程的生理作用的理解。
    BACKGROUND: Secreted frizzled-related proteins (SFRPs) comprise a family of WNT signaling antagonists whose roles in the ovary are poorly understood. Sfrp4-null mice were previously found to be hyperfertile due to an enhanced granulosa cell response to gonadotropins, leading to decreased antral follicle atresia and enhanced ovulation rates. The present study aimed to elucidate the mechanisms whereby SFRP4 antagonizes FSH action.
    METHODS: Primary cultures of granulosa cells from wild-type mice were treated with FSH and/or SFRP4, and effects of treatment on gene expression were evaluated by RT-qPCR and RNAseq. Bioinformatic analyses were conducted to analyse the effects of SFRP4 on the transcriptome, and compare them to those of FSH or a constitutively active mutant of FOXO1. Additional granulosa cell cultures from wild-type or Sfrp4-null mice, some pretreated with pharmacologic inhibitors of specific signaling effectors, were used to examine the effects of FSH and/or SFRP4 on signaling pathways, autophagy and apoptosis by western blotting and TUNEL.
    RESULTS: Treatment of cultured granulosa cells with recombinant SFRP4 was found to decrease basal and FSH-stimulated mRNA levels of FSH target genes. Unexpectedly, this effect was found to occur neither via a canonical (CTNNB1-dependent) nor non-canonical WNT signaling mechanism, but was found to be GSK3β-dependent. Rather, SFRP4 was found to antognize AKT activity via a mechanism involving AMPK. This lead to the hypophosphorylation of FOXO1 and a decrease in the expression of a portion of the FSH and FOXO1 transcriptomes. Conversely, FSH-stimulated AMPK, AKT and FOXO1 phosphorylation levels were found to be increased in the granulosa cells of Sfrp4-null mice relative to wild-type controls. SFRP4 treatement of granulosa cells also induced autophagy by signaling via AKT-mTORC1-ULK1, as well as apoptosis.
    CONCLUSIONS: This study identifies a novel GSK3β-AMPK-AKT signaling mechanism through which SFPR4 antagonizes FSH action, and further identifies SFRP4 as a novel regulator of granulosa cell autophagy. These findings provide a mechanistic basis for the phenotypic changes previously observed in Sfrp4-null mice, and broaden our understanding of the physiological roles of WNT signaling processes in the ovary.
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  • 文章类型: Journal Article
    女性的生育能力取决于卵泡的卵巢储备,这是在出生时决定的。原始卵泡发育和卵母细胞成熟受多种因素和途径调节,分为促性腺激素依赖性和促性腺激素依赖性阶段。根据对促性腺激素的反应。毛囊发生一直被认为是促性腺激素依赖性仅从窦阶段开始,但文献中的证据强调了促卵泡激素(FSH)和黄体生成素(LH)在早期卵泡形成过程中的作用,在原始卵泡池的进展中具有潜在的作用.在卵泡发生的最早期阶段,激素和分子途径的改变可能是多囊卵巢综合征(PCOS)和与抗癫痫治疗相关的PCOS样表型的无排卵的根本原因。过度诱导原始卵泡激活也可导致卵巢早衰(POI),一种以40岁以前妇女更年期为特征的疾病。未来旨在抑制初始募集或防止静止卵泡生长的治疗方法可能有助于延长女性生育能力,尤其是患有PCOS或POI的女性。本文将简要介绍促性腺激素对早期卵泡发育的影响。我们将讨论LH对卵巢储备的影响及其在PCOS和POI不孕症中的潜在作用。
    Female fertility depends on the ovarian reserve of follicles, which is determined at birth. Primordial follicle development and oocyte maturation are regulated by multiple factors and pathways and classified into gonadotropin-independent and gonadotropin-dependent phases, according to the response to gonadotropins. Folliculogenesis has always been considered to be gonadotropin-dependent only from the antral stage, but evidence from the literature highlights the role of follicle-stimulating hormone (FSH) and luteinizing hormone (LH) during early folliculogenesis with a potential role in the progression of the pool of primordial follicles. Hormonal and molecular pathway alterations during the very earliest stages of folliculogenesis may be the root cause of anovulation in polycystic ovary syndrome (PCOS) and in PCOS-like phenotypes related to antiepileptic treatment. Excessive induction of primordial follicle activation can also lead to premature ovarian insufficiency (POI), a condition characterized by menopause in women before 40 years of age. Future treatments aiming to suppress initial recruitment or prevent the growth of resting follicles could help in prolonging female fertility, especially in women with PCOS or POI. This review will briefly introduce the impact of gonadotropins on early folliculogenesis. We will discuss the influence of LH on ovarian reserve and its potential role in PCOS and POI infertility.
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  • 文章类型: Journal Article
    卵泡刺激素(FSH)和黄体生成素(LH)通过调节几个过程来控制窦卵泡的生长,比如激素和信号分子的合成,扩散,生存,凋亡,黄体化,和排卵。为了发挥这些作用,促性腺激素与它们各自的Gs蛋白偶联受体结合,激活蛋白激酶A(PKA)途径或募集Gq蛋白以激活蛋白激酶C(PKC)信号。虽然FSH和LH的作用机制是明确的,最近,已经表明,两种促性腺激素通过激活鞘氨醇激酶1促进颗粒细胞和卵泡膜细胞中1-磷酸鞘氨醇(S1P)的合成。此外,抑制SPHKs减少S1P合成,细胞活力,以及卵泡细胞对促性腺激素的反应增殖,在培养基中添加S1P可增加颗粒细胞和卵泡膜细胞的增殖,而对性类固醇的合成没有明显影响。因此,我们认为S1P是一个重要的信号分子,它补充了经典的促性腺激素途径,以促进颗粒细胞和卵泡膜细胞的增殖和活力。
    Follicle-stimulating hormone (FSH) and luteinizing hormone (LH) control antral follicular growth by regulating several processes, such as the synthesis of hormones and signaling molecules, proliferation, survival, apoptosis, luteinization, and ovulation. To exert these effects, gonadotropins bind to their respective Gs protein-coupled receptors, activating the protein kinase A (PKA) pathway or recruiting Gq proteins to activate protein kinase C (PKC) signaling. Although the action mechanism of FSH and LH is clear, recently, it has been shown that both gonadotropins promote the synthesis of sphingosine-1-phosphate (S1P) in granulosa and theca cells through the activation of sphingosine kinase 1. Moreover, the inhibition of SPHKs reduces S1P synthesis, cell viability, and the proliferation of follicular cells in response to gonadotropins, and the addition of S1P to the culture medium increases the proliferation of granulosa and theca cells without apparent effects on sexual steroid synthesis. Therefore, we consider that S1P is a crucial signaling molecule that complements the canonical gonadotropin pathway to promote the proliferation and viability of granulosa and theca cells.
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  • 文章类型: Letter
    暂无摘要。
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  • 文章类型: Journal Article
    为了确定子宫内膜厚度(EMT)在i)柠檬酸克罗米芬(CC)和促性腺激素(Gn)之间是否不同,使用患者作为自己的对照,和ii)受孕CC和未受孕CC的患者。此外,研究晚期卵泡EMT与妊娠结局之间的关系,在CC和Gn周期。
    回顾性研究。为了本研究的目的,分别进行了三组分析。在分析1中,我们纳入了最初接受CC/IUI(CC1,n=1252)的女性的所有周期,其次是Gn/IUI(Gn1,n=1307),要比较CC/IUI和Gn/IUI之间的EMT差异,利用女性作为自己的控制。在分析2中,我们纳入了所有CC/IUI周期(CC2,n=686),这些周期来自在同一研究期间最终受孕CC的女性,评估受孕CC(CC2)和未受孕CC(CC1)的患者之间的EMT差异。在分析3中,在CC/IUI和Gn/IUI周期中评估了不同EMT四分位数之间的妊娠结局,分开,探讨EMT与妊娠结局之间的潜在关联。
    在分析1中,当CC1与Gn1循环进行比较时,EMT明显变薄[中位数(IQR):6.8(5.5-8.0)与8.3(7.0-10.0)mm,p<0.001]。患者内,CC1与Gn1EMT相比平均薄1.7mm。广义线性混合模型,针对混杂因素进行了调整,结果相似(系数:1.69,95%CI:1.52-1.85,CC1为参考。).在分析2中,将CC1与CC2EMT进行了比较,前者在[中位数(IQR):6.8(5.5-8.0)与7.2(6.0-8.9)mm,p<0.001]和调整后(系数:0.59,95CI:0.34-0.85,CC1为参考。).在分析3中,随着CC周期中EMT四分位数的增加(Q1至Q4),临床妊娠率(CPRs)和持续妊娠率(OPR)得到改善(分别为p<0.001,p<0.001),而在Gn周期中没有观察到这种趋势(分别为p=0.94,p=0.68)。广义估计方程模型,针对混杂因素进行了调整,提示在CC周期中EMT与CPR和OPR呈正相关,但不是在Gn周期。
    患者内部,与Gn相比,CC通常导致更薄的EMT。子宫内膜变薄与CC周期中OPR降低有关,而在Gn周期中未检测到这种关联。
    UNASSIGNED: To determine whether endometrial thickness (EMT) differs between i) clomiphene citrate (CC) and gonadotropin (Gn) utilizing patients as their own controls, and ii) patients who conceived with CC and those who did not. Furthermore, to investigate the association between late-follicular EMT and pregnancy outcomes, in CC and Gn cycles.
    UNASSIGNED: Retrospective study. Three sets of analyses were conducted separately for the purpose of this study. In analysis 1, we included all cycles from women who initially underwent CC/IUI (CC1, n=1252), followed by Gn/IUI (Gn1, n=1307), to compare EMT differences between CC/IUI and Gn/IUI, utilizing women as their own controls. In analysis 2, we included all CC/IUI cycles (CC2, n=686) from women who eventually conceived with CC during the same study period, to evaluate EMT differences between patients who conceived with CC (CC2) and those who did not (CC1). In analysis 3, pregnancy outcomes among different EMT quartiles were evaluated in CC/IUI and Gn/IUI cycles, separately, to investigate the potential association between EMT and pregnancy outcomes.
    UNASSIGNED: In analysis 1, when CC1 was compared to Gn1 cycles, EMT was noted to be significantly thinner [Median (IQR): 6.8 (5.5-8.0) vs. 8.3 (7.0-10.0) mm, p<0.001]. Within-patient, CC1 compared to Gn1 EMT was on average 1.7mm thinner. Generalized linear mixed models, adjusted for confounders, revealed similar results (coefficient: 1.69, 95% CI: 1.52-1.85, CC1 as ref.). In analysis 2, CC1 was compared to CC2 EMT, the former being thinner both before [Median (IQR): 6.8 (5.5-8.0) vs. 7.2 (6.0-8.9) mm, p<0.001] and after adjustment (coefficient: 0.59, 95%CI: 0.34-0.85, CC1 as ref.). In analysis 3, clinical pregnancy rates (CPRs) and ongoing pregnancy rates (OPRs) improved as EMT quartiles increased (Q1 to Q4) among CC cycles (p<0.001, p<0.001, respectively), while no such trend was observed among Gn cycles (p=0.94, p=0.68, respectively). Generalized estimating equations models, adjusted for confounders, suggested that EMT was positively associated with CPR and OPR in CC cycles, but not in Gn cycles.
    UNASSIGNED: Within-patient, CC generally resulted in thinner EMT compared to Gn. Thinner endometrium was associated with decreased OPR in CC cycles, while no such association was detected in Gn cycles.
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  • 文章类型: Journal Article
    出生时患有下丘脑-垂体-性腺轴严重中枢紊乱导致促性腺激素缺乏的婴儿不仅在青春期缺乏青春期发育,但也缺乏婴儿迷你青春期。这个时期的小青春期,婴儿的促性腺激素和性类固醇浓度达到成人范围,对未来的生殖能力至关重要,尤其是男孩。目前,对于先天性低促性腺激素性腺功能减退症或多发性垂体激素缺乏症导致的促性腺激素缺乏症婴儿的诊断或治疗尚无共识。病例系列表明,在缺乏小青春期的男性婴儿中,促性腺激素治疗可有效促进睾丸未降的人的睾丸下降,并促进阴茎大小增加。此外,用促卵泡激素替代可增加睾丸支持细胞群,可测量为睾丸体积和抑制素B的增加,因此,假设增加这些患者的成年期精子发生能力。然而,对于与生育力和非生殖后遗症有关的结果,长期随访数据有限,包括神经发育和心理健康。对促性腺激素缺乏症患者使用国际登记册是收集高质量、地理上广泛的数据,以告知从出生到成年的最佳实践管理。
    Infants born with severe central disorders of the hypothalamic-pituitary-gonadal axis leading to gonadotropin deficiency not only lack pubertal development in adolescence, but also lack infantile mini-puberty. This period of mini-puberty, where infants have gonadotropin and sex steroid concentrations up into the adult range, is vital for future reproductive capacity, particularly in boys. At present, there is no consensus on the diagnosis or management of infants with gonadotropin deficiency due to congenital hypogonadotropic hypogonadism or multiple pituitary hormone deficiency. Case series suggest that gonadotropin treatment in male infants with absent mini-puberty is effective in promoting both testicular descent in those with undescended testes and also facilitating increased penile size. Moreover, replacement with follicle-stimulating hormone increases the testicular Sertoli cell population, measurable as an increase in testicular volume and inhibin B, thus hypothetically increasing the capacity for spermatogenesis in adult life for these patients. However, long-term follow-up data is limited for both outcomes pertaining to fertility and nonreproductive sequelae, including neurodevelopment and psychological well-being. The use of international registries for patients with gonadotropin deficiency is a key element in the collection of high-quality, geographically widespread data to inform best-practice management from birth to adulthood.
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  • 文章类型: Journal Article
    生殖激素对交配系统至关重要,行为,生育力,妊娠,分娩,和哺乳动物的泌乳以及了解激素在这些过程中的作用对于物种保护至关重要。Sirenia是一种独特的海洋哺乳动物,包括海牛,儒艮和已灭绝的斯特勒海牛。由于栖息地的丧失,现存的Sirenian物种都被列为脆弱物种,寒冷的压力,船撞击创伤,有害的藻类水华毒性,纠缠,非法狩猎因此,成功的繁殖对于维持和增加Sirenian种群至关重要。了解Sirenian的生殖行为,内分泌学,交配策略将有助于保护和管理努力,以保护并为成功繁殖提供适当的条件。这篇评论的目的是综合有关Sirenians生殖周期和内分泌学的当前知识,并确定知识差距,以供将来进行调查。当前有关Sirenian生殖生理学的文献报道了生殖季节性,性成熟,发情周期性和无环性,怀孕,和性别差异。然而,关于促性腺激素的周期性和脉冲释放仍然存在显著的知识空白,成熟的女性,和整个妊娠期妊娠激素谱的表征。迄今为止,没有解释卵巢非周期性疾病的确认模式,也不了解海牛中描述的众多附属黄体的功能。重要的第一步是研究,包括对更广泛的野生海牛种群进行更多的纵向和事后研究。一起来看,了解这些脆弱和受威胁物种的生殖内分泌学对于政策和管理决策至关重要,以更好地为保护计划提供信息。
    Reproductive hormones are essential to mating systems, behavior, fertility, gestation, parturition, and lactation in mammals and understanding the role of hormones in these processes is essential for species conservation. Sirenia is a unique order of marine mammals that include manatees, dugongs, and the extinct Steller\'s sea cow. Extant Sirenian species are all listed as vulnerable due to habitat loss, cold stress, boat strike trauma, harmful algal bloom toxicity, entanglements, and illegal hunting. Therefore, successful reproduction is essential to maintaining and increasing Sirenian populations. Understanding Sirenian reproductive behavior, endocrinology, and mating strategies will aid conservation and management efforts to protect and provide the proper conditions for successful reproduction. The objectives of this review were to synthesize the current knowledge regarding reproductive cycles and endocrinology of Sirenians and identify knowledge gaps for future investigation. The current literature on Sirenian reproductive physiology reports reproductive seasonality, sexual maturation, estrous cyclicity and acyclicity, pregnancy, and sex differences. However, there remain significant knowledge gaps on the cyclicity and pulsatile release of gonadotropins, maturation in females, and characterization of pregnancy hormone profiles throughout gestation. To date, there is no explanation for confirmed pattern for ovarian acyclicity, nor understanding of the function of the numerous accessory corpus luteum described in manatees. Research including a greater number of longitudinal and postmortem studies on a wider variety of wild manatee populations are important first steps. Taken together, understanding the reproductive endocrinology of these vulnerable and threatened species is critical for policy and management decisions to better inform protection initiatives.
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  • 文章类型: Journal Article
    本研究描述了条纹蛇头的产卵诱导,使用鲤鱼垂体提取物(CPE)和LH-RH激动剂即Buserelin(Glp-His-Trp-Ser-Tyr-Ser-tBu-Leu-Arg-Pro-NHEt)。在两种激素试验下设计共四种治疗方法,并作为对照组,T1、T2和T3,每种处理重复三次。虽然在所有激素处理下的育种者都表现出产卵性能,对照组未观察到产卵性能。在CPE的情况下,激素治疗后的等待时间(20-24小时)比Buserelin(25-30小时)最低。关于CPE,产卵,在不同处理中,随着CPE剂量的增加,受精和孵化率均较高。最高平均值±标准差产卵,受精率和孵化率为85.60±8.58%,在CPE剂量为80mgkg-1的T3中,分别为79.38±4.89%和64.33±6.60%。同样,在Buserelin激素的情况下,T3的产卵率最高(80.61±5.59),其中Buserelin的剂量为0.80µgkg-1体重。T1、T2和T3的受精率分别为48.57±5.99、70.62±5.33和90.32±4.79。同时,T1,T2和T3处理的孵化率分别为20.81±4.91、37.11±4.50和61.33±6.61。然而,T3表现出关于产卵的最佳性能,受精率和孵化率均显著高于其他两种处理。目前的研究表明,使用鲤鱼垂体提取物和Buserelin进行产卵诱导是有效的,可能对Channastriata的人工育种有用。关于剂量应用,即80mgkg-1的CPE和0.80μgkg-1的Buserelin可以成功地应用于Channa纹状体的排卵刺激。
    Present study describes the spawning induction of striped Snakehead, Channa striata using carp pituitary extract (CPE) and LH-RH agonist i.e. Buserelin (Glp-His-Trp-Ser-Tyr-Ser-tBu-Leu-Arg-Pro-NHEt). Total four treatments were designed under both hormones trail and treated as control group, T1, T2, and T3 with three replications of each treatment. While breeders under all hormone treatments showed spawning performances, no spawning performance was observed in control group. Latency time after hormonal treatment was lowest (20-24 hrs) in case of CPE than Buserelin (25-30 hrs). Regarding to CPE, spawning, fertilization and hatching rate were higher with the increasing doses of CPE in different treatments. The highest mean ± Standard deviation spawning, fertilization and hatching rate were 85.60±8.58 %, 79.38±4.89 % and 64.33±6.60 % respectively in T3 where dose of CPE was 80 mg kg-1. Similarly, in case of Buserelin hormone highest spawning rate was found in T3 (80.61±5.59) where dose of Buserelin was 0.80 µg kg-1 body weight. Fertilization rate was on the level 48.57±5.99, 70.62±5.33 and 90.32±4.79 respectively for T1, T2, and T3.Whilst, hatching rate was found 20.81±4.91, 37.11±4.50 and 61.33±6.61 in T1, T2, and T3 treatments respectively. However, T3 exhibited best performance regarding spawning, fertilization and hatching rate which were significantly higher than other two treatments.The current study revealed that spawning induction using carp pituitary extract and Buserelin is effective and might be useful for artificial breeding of Channa striata. Regarding to dose application i.e. 80 mg kg-1 of CPE and 0.80 µg kg-1 of Buserelin may be successfully applied to ovulation stimulation of Channa striata.
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  • 文章类型: Journal Article
    人类促性腺激素是一种具有高度复杂结构的糖蛋白激素,这需要应用复杂的分析方法来评估它们的质量。这项研究的主要目的是对两种尿液来源的质量研究的凝胶电泳技术和基于质谱的方法进行比较评估,高度纯化,人类更年期促性腺激素制剂,Menopur75/75I.U.和Meriofert75I.U.分子量(先生),等电点(pI),通过SDS-PAGE和2D凝胶电泳估计研究化合物的同工型模式,而基质辅助激光解吸/电离飞行时间质谱(MALDI-TOFMS)用于在凝胶内胰蛋白酶消化选定蛋白质斑点后获得的肽的下游表征。此外,为了估计这些生物制品的糖基化模式,进行低聚糖的酶促释放,并研究了同工型模式。凝胶电泳显示了蛋白质生物治疗药物的典型电泳行为,其中包括以不同质量和pI迁移的极其复杂的斑点模式。MS分析被证明是鉴定和详细表征促性腺激素的强大工具,并以高序列覆盖率鉴定了相关肽。这项研究的结果不仅可用于此类复杂生物药物的质量评估,而且还可以作为基于糖基化模式调节以增强功效或减少副作用的生物药物进一步开发的支持平台。
    Human gonadotropins are glycoprotein hormones with a highly complex structure, which demands the application of sophisticated analytical methodologies to assess their quality. The principal objective of this study was a comparative evaluation of gel electrophoretic techniques and mass spectrometry-based methods for the quality study of the two urinary-derived, highly purified, human menopausal gonadotropin preparations, Menopur 75/75 I. U. and Meriofert 75 I. U. Molecular mass (Mr), isoelectric point (pI), and isoform pattern of studied compounds were estimated via SDS-PAGE and 2D gel electrophoresis, whereas matrix-assisted laser desorption/ionization time-of-flight mass spectrometry (MALDI-TOF MS) was used for the downstream characterization of peptides obtained after in-gel tryptic digestion of selected protein spots. Additionally, for the estimation of the glycosylation pattern of these biologics, the enzymatic release of oligosaccharides was performed, and the isoform pattern was studied. Gel electrophoresis showed a typical electrophoretic behaviour for protein biotherapeutics medicines consisting of extremely complex spot patterns migrating at different masses and pIs. MS analysis proved to be a powerful tool for the identification and detailed characterization of the gonadotropins and the relevant peptides were identified with high sequence coverages. The results of this study are not only useful for the quality assessment of this class of complex biopharmaceuticals but may also serve as a supporting platform for further development of biopharmaceuticals based on modulation of the glycosylation pattern to enhance efficacy or reduce side effects.
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