Taste Buds

味蕾
  • 文章类型: Journal Article
    强烈的环境压力可以通过复杂的进化机制产生回归和建设性特征。虽然回归研究得很好,构造特征的生物学基础不太清楚。居住在洞穴中的Astyanax鱼头上有丰富的口外味蕾,在同种表面居民中不存在。这里,我们提供了新的个体发育数据,表明口外味蕾在生活史上逐渐和晚期出现。在不同的洞穴鱼种群中,这种外观相似但不相同,图案已经演变为允许在内胚层-外胚层胚层边界上重新指定味蕾。定量遗传分析显示,头部空间上不同的味蕾主要由两个不同的洞穴优势基因座介导。虽然这种晚期扩展到头部的确切功能是未知的,口外味蕾的出现与从活食到蝙蝠鸟粪的饮食转变相吻合,提出了一种适应性机制来检测食物匮乏的洞穴中的营养。这项工作为建设性的进化特征提供了基本的见解,出现在生活史的后期,有望为脊椎动物感觉器官发育的未解决特征提供新窗口。
    Intense environmental pressures can yield both regressive and constructive traits through complex evolutionary mechanisms. Although regression is well-studied, the biological bases of constructive features are less well understood. Cave-dwelling Astyanax fish harbor prolific extraoral taste buds on their heads, which are absent in conspecific surface-dwellers. Here, we present novel ontogenetic data demonstrating extraoral taste buds appear gradually and late in life history. This appearance is similar but non-identical in different cavefish populations, where patterning has evolved to permit taste bud re-specification across the endoderm-ectoderm germ layer boundary. Quantitative genetic analyses revealed that spatially distinct taste buds on the head are primarily mediated by two different cave-dominant loci. While the precise function of this late expansion on to the head is unknown, the appearance of extraoral taste buds coincides with a dietary shift from live-foods to bat guano, suggesting an adaptive mechanism to detect nutrition in food-starved caves. This work provides fundamental insight to a constructive evolutionary feature, arising late in life history, promising a new window into unresolved features of vertebrate sensory organ development.
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  • 文章类型: Journal Article
    哺乳动物味蕾是高度再生的,可以在舌上皮的正常磨损或包括烧伤在内的物理和化学损伤后恢复自身,化疗,和神经损伤。这是由于持续的扩散,分化,和味觉祖细胞的成熟,然后必须与外周味觉神经元重新连接以将味觉信号传递给大脑。外周味觉突触的更新和重建对于维持这种复杂的感觉系统至关重要。在过去的几十年里,已经很好地描述了味觉细胞内的信号转导和神经递质释放机制。然而,舌头中突触伙伴(味觉细胞和味觉神经元)之间的复杂动力学仅被部分理解。在这次审查中,我们强调了最近的发现,这些发现提高了我们对味蕾内连接和信号传导机制的理解,以及关于味觉细胞和味觉神经元之间复杂相互作用的仍未解决的问题。
    Mammalian taste buds are highly regenerative and can restore themselves after normal wear and tear of the lingual epithelium or following physical and chemical insults, including burns, chemotherapy, and nerve injury. This is due to the continual proliferation, differentiation, and maturation of taste progenitor cells, which then must reconnect with peripheral gustatory neurons to relay taste signals to the brain. The turnover and re-establishment of peripheral taste synapses are vital to maintain this complex sensory system. Over the past several decades, the signal transduction and neurotransmitter release mechanisms within taste cells have been well delineated. However, the complex dynamics between synaptic partners in the tongue (taste cell and gustatory neuron) are only partially understood. In this review, we highlight recent findings that have improved our understanding of the mechanisms governing connectivity and signaling within the taste bud and the still-unresolved questions regarding the complex interactions between taste cells and gustatory neurons.
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  • 文章类型: Journal Article
    人们对海鸥味觉的化学感觉系统知之甚少,基部无颚脊椎动物,以活食为食。这项研究的目的是研究海七匙咽部沿咽部长度的味蕾分布和化学感应反应。扫描电子显微镜和免疫细胞化学显示,在七对内部g孔之间的所有六个侧咽部位置都有味蕾和相关轴突。最前端的咽部区域比最尾部区域包含更多和更大的味蕾。记录味觉受体细胞对甜味的反应,苦涩,氨基酸和胆汁酸牛磺胆酸,以及三磷酸腺苷。在所有六个具有味蕾的咽部位置观察到类似的化学感应反应。总的来说,这项研究表明,在海洋七叶鱼的七个咽区,有明显的味蕾和味觉感受器细胞活性。
    Little is known about the chemosensory system of gustation in sea lampreys, basal jawless vertebrates that feed voraciously on live prey. The objective of this study was to investigate taste bud distribution and chemosensory responses along the length of the pharynx in the sea lamprey. Scanning electron microscopy and immunocytochemistry revealed taste buds and associated axons at all six lateral pharyngeal locations between the seven pairs of internal gill pores. The most rostral pharyngeal region contained more and larger taste buds than the most caudal region. Taste receptor cell responses were recorded to sweet, bitter, amino acids and the bile acid taurocholic acid, as well as to adenosine triphosphate. Similar chemosensory responses were observed at all six pharyngeal locations with taste buds. Overall, this study shows prominent taste buds and taste receptor cell activity in the seven pharyngeal regions of the sea lamprey.
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  • 文章类型: Journal Article
    离子通道Piezo1和Piezo2已被鉴定为膜机械蛋白。研究化学感觉器官中的机械敏感通道可以帮助理解这些通道的作用机制,为各种疾病提供新的治疗靶点。本研究调查了斑马鱼化学感觉器官中Piezo蛋白的表达模式。第一次,据报道,成年斑马鱼化学感觉器官中的压电蛋白表达。在嗅觉上皮中,Piezo1免疫标记kappe神经元,微绒毛细胞,和隐窝神经元,而Calretinin在纤毛感觉细胞中表达。Piezo1和Calretinin之间缺乏重叠,证实了Piezo1对kappe神经元的特异性,微绒毛细胞,和隐窝神经元。Piezo2在kappe神经元中显示出强烈的免疫反应性,单纤毛感觉细胞,和多纤毛感觉细胞,具有重叠的Calretinin表达,显示其嗅觉神经元的性质。在味蕾中,Piezo1免疫标记皮肤和咽部味蕾基部的默克尔样细胞以及皮肤和口腔味蕾的明暗细胞。它还标记了咽部味蕾的暗细胞和口腔味蕾中的支持细胞。在皮肤和口腔味蕾的浅色和深色细胞以及分离的化学感应细胞中发现了压电2。这些发现为斑马鱼化学感觉器官中压电通道的分布提供了新的见解,增强我们对其感官处理和潜在治疗应用的理解。
    The ion channels Piezo 1 and Piezo 2 have been identified as membrane mechano-proteins. Studying mechanosensitive channels in chemosensory organs could help in understanding the mechanisms by which these channels operate, offering new therapeutic targets for various disorders. This study investigates the expression patterns of Piezo proteins in zebrafish chemosensory organs. For the first time, Piezo protein expression in adult zebrafish chemosensory organs is reported. In the olfactory epithelium, Piezo 1 immunolabels kappe neurons, microvillous cells, and crypt neurons, while Calretinin is expressed in ciliated sensory cells. The lack of overlap between Piezo 1 and Calretinin confirms Piezo 1\'s specificity for kappe neurons, microvillous cells, and crypt neurons. Piezo 2 shows intense immunoreactivity in kappe neurons, one-ciliated sensory cells, and multi-ciliated sensory cells, with overlapping Calretinin expression, indicating its olfactory neuron nature. In taste buds, Piezo 1 immunolabels Merkel-like cells at the bases of cutaneous and pharyngeal taste buds and the light and dark cells of cutaneous and oral taste buds. It also marks the dark cells of pharyngeal taste buds and support cells in oral taste buds. Piezo 2 is found in the light and dark cells of cutaneous and oral taste buds and isolated chemosensory cells. These findings provide new insights into the distribution of Piezo channels in zebrafish chemosensory organs, enhancing our understanding of their sensory processing and potential therapeutic applications.
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  • 文章类型: Journal Article
    糖的口服检测依赖于两种类型的受体系统。第一个是G蛋白偶联受体TAS1R2/TAS1R3。激活时,这个受体触发了一个下游的信号级联反应,磷脂酶Cβ2(PLCβ2),和瞬时受体电位通道M5(TRPM5)。第二种类型的受体是葡萄糖转运蛋白。当葡萄糖通过这种转运蛋白进入细胞时,代谢产生ATP。这种ATP抑制KATP通道的开放,导致细胞去极化。除了这些受体系统,对甜味敏感的味觉细胞具有基于身体内部和外部状态调节其对甜味物质的敏感性的机制。甜味受体不限于口腔;它们也存在于口腔外器官,如胃肠道,胰腺,和大脑。这些口外甜味受体参与各种功能,包括葡萄糖吸收,胰岛素释放,糖偏好,和食物摄入,有助于维持能量稳态。此外,甜味受体可能在某些器官如气管和骨骼中具有独特的作用。这篇综述总结了过去和最近对甜味受体系统的研究,探索口腔和口外器官中甜味(糖)检测的分子机制和生理功能。
    The oral detection of sugars relies on two types of receptor systems. The first is the G-protein-coupled receptor TAS1R2/TAS1R3. When activated, this receptor triggers a downstream signaling cascade involving gustducin, phospholipase Cβ2 (PLCβ2), and transient receptor potential channel M5 (TRPM5). The second type of receptor is the glucose transporter. When glucose enters the cell via this transporter, it is metabolized to produce ATP. This ATP inhibits the opening of KATP channels, leading to cell depolarization. Beside these receptor systems, sweet-sensitive taste cells have mechanisms to regulate their sensitivity to sweet substances based on internal and external states of the body. Sweet taste receptors are not limited to the oral cavity; they are also present in extraoral organs such as the gastrointestinal tract, pancreas, and brain. These extraoral sweet receptors are involved in various functions, including glucose absorption, insulin release, sugar preference, and food intake, contributing to the maintenance of energy homeostasis. Additionally, sweet receptors may have unique roles in certain organs like the trachea and bone. This review summarizes past and recent studies on sweet receptor systems, exploring the molecular mechanisms and physiological functions of sweet (sugar) detection in both oral and extraoral organs.
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  • 文章类型: Journal Article
    自2019年以来,2019年冠状病毒病(COVID-19)已经影响到全球数百万人。除急性呼吸窘迫综合征外,病态也是COVID-19的常见症状,会给患者带来数周或永久性的负担。然而,味觉功能障碍的潜在机制仍不清楚。这里,我们对5例死于COVID-19的患者进行了完整的尸检.综合舌头样本,包括许多味蕾,唾液腺,船只,收集神经来绘制病理学图,分布,细胞嗜性,和严重急性呼吸综合征冠状病毒2(SARS-CoV-2)在舌中的受体分布。我们的结果显示,所有患者在唾液腺周围和粘膜附近的固有层中都有中度淋巴细胞浸润,味蕾和唾液腺上皮中的固缩。这可能是因为严重的acini,唾液腺管,味蕾是SARS-CoV-2感染的主要部位。多色免疫荧光显示SARS-CoV-2容易感染味蕾中的角蛋白(KRT)7味觉受体细胞,浆液性腺分泌细胞,和导管中的内部上皮细胞。主要受体,血管紧张素转换酶2(ACE2)和跨膜蛋白酶丝氨酸亚型2(TMPRSS2),都在这些细胞中大量表达。在血管和神经中很少检测到病毒抗原和受体。这表明SARS-CoV-2感染会引发舌头的病理损伤,并且这种畸形可能与病毒感染和细胞损伤直接相关。
    Since 2019, Coronavirus Disease 2019(COVID-19) has affected millions of people worldwide. Except for acute respiratory distress syndrome, dysgeusis is also a common symptom of COVID-19 that burdens patients for weeks or permanently. However, the mechanisms underlying taste dysfunctions remain unclear. Here, we performed complete autopsies of five patients who died of COVID-19. Integrated tongue samples, including numerous taste buds, salivary glands, vessels, and nerves were collected to map the pathology, distribution, cell tropism, and receptor distribution of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) in the tongue. Our results revealed that all patients had moderate lymphocyte infiltration around the salivary glands and in the lamina propria adjacent to the mucosa, and pyknosis in the epithelia of taste buds and salivary glands. This may be because the serous acini, salivary gland ducts, and taste buds are the primary sites of SARS-CoV-2 infection. Multicolor immunofluorescence showed that SARS-CoV-2 readily infects Keratin (KRT)7+ taste receptor cells in taste buds, secretory cells in serous acini, and inner epithelial cells in the ducts. The major receptors, angiotensin-converting enzyme 2 (ACE2) and transmembrane protease serine subtype 2 (TMPRSS2), were both abundantly expressed in these cells. Viral antigens and receptor were both rarely detected in vessels and nerves. This indicates that SARS-CoV-2 infection triggers pathological injury in the tongue, and that dysgeusis may be directly related to viral infection and cellular damage.
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  • 文章类型: Journal Article
    化学感觉障碍是SARS-CoV-2感染的突出症状。我们假设测量的感觉障碍伴随着舌头叶状乳头区域的转录组变化。具有已知SARS-CoV-2免疫球蛋白G(IgG)状态的医院人员完成了感官知觉问卷(n=158)。n=141的亚组参加了强制选择味觉测试,n=43参与者同意捐赠叶状乳头区域的舌拭子用于整个转录组分析。该研究包括四组不同IgG水平的参与者(≥10AU/mL=IgG;<10AU/mL=IgG-)和自我报告的感觉障碍(SSI±)。未检测到金属味道的IgG+受试者的IgG+水平高于检测到葡萄糖酸铁的IgG+参与者(p=0.03)。气味感知是来自进行基因本体论富集的IgG+/SSI+参与者的转录组数据中最受损的生物学过程。IgG/SSI受试者显示出166种嗅觉受体(OR)和9种味觉相关受体(TAS)的较低表达水平,其中OR1A2,OR2J2,OR1A1,OR5K1和OR1G1以及TAS2R7与金属感知有关。这项研究提出的问题是,舌头上的气味受体(i)是否可能在金属感觉中起作用,和(ii)是病毒引发的感觉障碍的潜在目标,这需要在未来的功能研究中进行研究。
    Chemosensory impairment is an outstanding symptom of SARS-CoV-2 infections. We hypothesized that measured sensory impairments are accompanied by transcriptomic changes in the foliate papillae area of the tongue. Hospital personnel with known SARS-CoV-2 immunoglobulin G (IgG) status completed questionnaires on sensory perception (n = 158). A subcohort of n = 141 participated in forced choice taste tests, and n = 43 participants consented to donate tongue swabs of the foliate papillae area for whole transcriptome analysis. The study included four groups of participants differing in IgG levels (≥ 10 AU/mL = IgG+; < 10 AU/mL = IgG-) and self-reported sensory impairment (SSI±). IgG+ subjects not detecting metallic taste had higher IgG+ levels than IgG+ participants detecting iron gluconate (p = 0.03). Smell perception was the most impaired biological process in the transcriptome data from IgG+/SSI+ participants subjected to gene ontology enrichment. IgG+/SSI+ subjects demonstrated lower expression levels of 166 olfactory receptors (OR) and 9 taste associated receptors (TAS) of which OR1A2, OR2J2, OR1A1, OR5K1 and OR1G1, as well as TAS2R7 are linked to metallic perception. The question raised by this study is whether odorant receptors on the tongue (i) might play a role in metal sensation, and (ii) are potential targets for virus-initiated sensory impairments, which needs to be investigated in future functional studies.
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  • 文章类型: Journal Article
    已经相对于各种甜味剂的已知感官特性评估了微流体片上舌平台。人类小组报告的典型感官特征的类似指标,如甜味阈值,发病,挥之不去,从味觉受体激活曲线推导出苦味和阻断相互作用,然后进行比较。为此,将包含带有甜味和六种苦味受体的受体细胞阵列的流动池瞬时暴露于纯的和混合的甜味剂样品。通过注射荧光素染料来分别表征样品随时间的浓度梯度。随后,细胞钙对不同剂量的优势的反应,阿斯巴甜,糖精,和蔗糖用浓度梯度覆盖。定量描述与梯度相比的响应动力学的参数。与100mM的蔗糖相比,15μM的Advantame记录到5±2s的甜味起效明显更快,39s的滞留时间更长,起效时间为13±2s,滞留时间为6s。糖精被证明可以激活苦味受体TAS2R8,TAS2R31和TAS2R43,证实其已知的异味,而加入甜蜜素减少或阻断了这种糖精苦味反应。讨论了使用这种芯片上的舌头与体外测定和味觉小组弥合差距的潜力。
    A microfluidic tongue-on-a-chip platform has been evaluated relative to the known sensory properties of various sweeteners. Analogous metrics of typical sensory features reported by human panels such as sweet taste thresholds, onset, and lingering, as well as bitter off-flavor and blocking interactions were deduced from the taste receptor activation curves and then compared. To this end, a flow cell containing a receptor cell array bearing the sweet and six bitter taste receptors was transiently exposed to pure and mixed sweetener samples. The sample concentration gradient across time was separately characterized by the injection of fluorescein dye. Subsequently, cellular calcium responses to different doses of advantame, aspartame, saccharine, and sucrose were overlaid with the concentration gradient. Parameters describing the response kinetics compared to the gradient were quantified. Advantame at 15 μM recorded a significantly faster sweetness onset of 5 ± 2 s and a longer lingering time of 39 s relative to sucrose at 100 mM with an onset of 13 ± 2 s and a lingering time of 6 s. Saccharine was shown to activate the bitter receptors TAS2R8, TAS2R31, and TAS2R43, confirming its known off-flavor, whereas addition of cyclamate reduced or blocked this saccharine bitter response. The potential of using this tongue-on-a-chip to bridge the gap with in vitro assays and taste panels is discussed.
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  • 文章类型: Journal Article
    N-琥珀酰氨基酸(N-Suc-AAs)因其作为味觉活性化合物的潜力而备受关注。复杂的N-Suc-AA在鉴定具有味道活性的那些方面提出了相当大的挑战。因此,我们采用基于结构的虚拟筛选来精确定位味觉活性N-Suc-AAs,揭示N-琥珀酰-L-色氨酸(ST)作为对不同味觉受体具有高亲和力的化合物。在这一发现之后,ST是通过酶促过程合成的,达到40.2%的收率,其结构通过核磁共振波谱验证。感官评估以及电子舌头评估表明,浓度为1mg/L的ST显着增强鲜味,kokumi,和咸味强度,同时减轻各种苦味化合物的苦味,而自己却保持无味。此外,时间强度(TI)结果表明,注入1mg/LST的溶液的鲜味持续时间显着增加,苦味持续时间显着减少。分子对接研究表明ST作为激动剂或拮抗剂与多种味觉受体相互作用,主要通过氢键和疏水相互作用。这项研究标志着ST的酶合成及其在改善口味特性方面的功效的首次报道,强调ST在提高食品感官品质和促进调味品行业创新方面的重要性。
    N-Succinyl amino acids (N-Suc-AAs) are garnering attention for their potential as taste-active compounds. The intricate variety of N-Suc-AAs presented considerable challenges in identifying those with taste-active properties. Consequently, we employed structure-based virtual screening to pinpoint taste-active N-Suc-AAs, revealing N-succinyl-L-tryptophan (ST) as a compound with high affinity for different taste receptors. Following this discovery, ST was synthesized through an enzymatic process, achieving a yield of 40.2%, with its structure verified via NMR spectroscopy. Sensory evaluation alongside electronic tongue assessments indicated that ST at a concentration of 1 mg/L significantly enhances umami, kokumi, and saltiness intensities, while concurrently mitigating bitterness from various bitter compounds, whilst itself remaining tasteless. Additionally, time-intensity (TI) results elucidated a marked augmentation in umami duration and a notable diminution in bitterness duration for solutions imbued with 1 mg/L ST. Molecular docking study suggested ST interacted with diverse taste receptors as an agonist or antagonist, primarily through hydrogen bonds and hydrophobic interactions. This study marked the inaugural report on the enzymatic synthesis of ST and its efficacy in improving taste characteristics, underscoring the importance of ST in improving sensory qualities of food products and fostering innovation within the seasoning industry.
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  • 文章类型: Journal Article
    人类的苦味感对于识别食物中潜在的有害物质很重要。多年来,研究重点是鉴定25种人类苦味受体的激活剂。拮抗剂的发现以及关于不同功效的激动剂的知识的增加基本上增加了苦味感知的复杂性。本文旨在提高人们对复合混合物甚至整个食品的苦味进行评估时被低估的新复杂性的认识。
    Human bitter perception is important for the identification of potentially harmful substances in food. For quite some years, research focused on the identification of activators for ∼25 human bitter taste receptors. The discovery of antagonists as well as increasing knowledge about agonists of different efficacies has substantially added to the intricacy of bitter taste perception. This article seeks to raise awareness for an underestimated new level of complexity when compound mixtures or even whole food items are assessed for their bitter taste.
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