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Variation in branchial expression among insulin-like growth-factor binding proteins (igfbps) during Atlantic salmon smoltification and seawater exposure 大西洋鲑鱼闷烧和海水暴露过程中胰岛素样生长因子结合蛋白(igfbps)鳃表达的变化
Q1 Biochemistry, Genetics and Molecular Biology Pub Date : 2017-01-18 DOI: 10.1186/s12899-017-0028-5
J. Breves, Chelsea K. Fujimoto, Silas K. Phipps-Costin, I. Einarsdóttir, B. Björnsson, S. McCormick
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引用次数: 24
Small interfering RNA targeting NF-κB attenuates lipopolysaccharide-induced acute lung injury in rats 靶向NF-κB的小干扰RNA减轻脂多糖诱导的大鼠急性肺损伤
Q1 Biochemistry, Genetics and Molecular Biology Pub Date : 2016-12-28 DOI: 10.1186/s12899-016-0027-y
Ning Li, Yuanbin Song, Wei Zhao, Ting-ting Han, Shuhui Lin, Oscar Ramirez, Li Liang
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引用次数: 36
Ryanodine-induced vasoconstriction of the gerbil spiral modiolar artery depends on the Ca2+ sensitivity but not on Ca2+ sparks or BK channels ryanoine诱导的沙鼠螺旋臼齿动脉血管收缩取决于Ca2+敏感性,而不取决于Ca2+火花或BK通道
Q1 Biochemistry, Genetics and Molecular Biology Pub Date : 2016-11-02 DOI: 10.1186/s12899-016-0026-z
G. Krishnamoorthy, K. Reimann, P. Wangemann
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引用次数: 3
Trimester-specific thyroid hormone reference ranges in Sudanese women 苏丹妇女妊娠特异性甲状腺激素参考范围
Q1 Biochemistry, Genetics and Molecular Biology Pub Date : 2016-10-31 DOI: 10.1186/s12899-016-0025-0
Enaam T. Elhaj, I. Adam, M. Ahmed, Mohamed Faisal Lutfi
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引用次数: 15
The gastric H,K-ATPase in stria vascularis contributes to pH regulation of cochlear endolymph but not to K secretion. 血管纹中的胃H,K-ATP酶有助于调节耳蜗内淋巴的pH值,但与K的分泌无关。
Q1 Biochemistry, Genetics and Molecular Biology Pub Date : 2016-08-11 DOI: 10.1186/s12899-016-0024-1
Hiromitsu Miyazaki, Philine Wangemann, Daniel C Marcus

Background: Disturbance of acid-base balance in the inner ear is known to be associated with hearing loss in a number of conditions including genetic mutations and pharmacologic interventions. Several previous physiologic and immunohistochemical observations lead to proposals of the involvement of acid-base transporters in stria vascularis.

Results: We directly measured acid flux in vitro from the apical side of isolated stria vascularis from adult C57Bl/6 mice with a novel constant-perfusion pH-selective self-referencing probe. Acid efflux that depended on metabolism and ion transport was observed from the apical side of stria vascularis. The acid flux was decreased to about 40 % of control by removal of the metabolic substrate (glucose-free) and by inhibition of the sodium pump (ouabain). The flux was also decreased a) by inhibition of Na,H-exchangers by amiloride, dimethylamiloride (DMA), S3226 and Hoe694, b) by inhibition of Na,2Cl,K-cotransporter (NKCC1) by bumetanide, and c) by the likely inhibition of HCO3/anion exchange by DIDS. By contrast, the acid flux was increased by inhibition of gastric H,K-ATPase (SCH28080) but was not affected by an inhibitor of vH-ATPase (bafilomycin).  K flux from stria vascularis was reduced less than 5 % by SCH28080.

Conclusions: These observations suggest that stria vascularis may be an important site of control of cochlear acid-base balance and demonstrate a functional role of several acid-base transporters in stria vascularis, including basolateral H,K-ATPase and apical Na,H-exchange. Previous suggestions that H secretion is mediated by an apical vH-ATPase and that basolateral H,K-ATPase contributes importantly to K secretion in stria vascularis are not supported. These results advance our understanding of inner ear acid-base balance and provide a stronger basis to interpret the etiology of genetic and pharmacologic cochlear dysfunctions that are influenced by endolymphatic pH.

背景:众所周知,内耳酸碱平衡失调与多种情况下的听力损失有关,包括基因突变和药物干预。之前的一些生理和免疫组化观察结果表明,血管横纹中存在酸碱转运体:结果:我们使用新型恒定灌注 pH 选择性自参照探针直接测量了体外从成年 C57Bl/6 小鼠离体血管纹顶端侧流出的酸量。从血管纹顶部观察到的酸流出取决于新陈代谢和离子转运。通过移除代谢底物(无葡萄糖)和抑制钠泵(乌阿巴因),酸流出量降至对照组的 40%左右。a) 阿米洛利、二甲基阿米洛利(DMA)、S3226 和 Hoe694 对 Na、H 交换的抑制,b) 布美他尼对 Na、2Cl、K 共转运体(NKCC1)的抑制,以及 c) DIDS 对 HCO3/阴离子交换的可能抑制,也会降低酸通量。相比之下,抑制胃 H、K-ATP 酶(SCH28080)会增加酸通量,但 vH-ATP 酶抑制剂(巴非罗霉素)不会影响酸通量。 血管横纹的 K 通量在 SCH28080 的作用下减少不到 5%:这些观察结果表明,血管横纹可能是控制耳蜗酸碱平衡的重要部位,并证明了血管横纹中几种酸碱转运体的功能作用,包括基底侧的 H、K-ATP 酶和顶端的 Na、H 交换。以前有人认为血管横纹中 H 的分泌是由顶端的 vH-ATPase 介导的,而基底侧的 H、K-ATPase 对 K 的分泌有重要作用,但这些观点都不成立。这些结果加深了我们对内耳酸碱平衡的理解,为解释受内耳pH影响的遗传和药物耳蜗功能障碍的病因提供了更坚实的基础。
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引用次数: 0
The novel in vitro reanimation of isolated human and large mammalian heart-lung blocs. 分离的人类和大型哺乳动物心肺块的新颖体外再生。
Q1 Biochemistry, Genetics and Molecular Biology Pub Date : 2016-06-04 DOI: 10.1186/s12899-016-0023-2
Ryan P Goff, Brian T Howard, Stephen G Quallich, Tinen L Iles, Paul A Iaizzo

Background: In vitro isolated heart preparations are valuable tools for the study of cardiac anatomy and physiology, as well as for preclinical device testing. Such preparations afford investigators a high level of hemodynamic control, independent of host or systemic interactions. Here we hypothesize that recovered human and swine heart-lung blocs can be reanimated using a clear perfusate and elicit viable cardiodynamic and pulmonic function. Further, this approach will facilitate multimodal imaging, which is particularly valuable for the study of both functional anatomy and device-tissue interactions. Five human and 18 swine heart-lung preparations were procured using techniques analogous to those for cardiac transplant. Specimens were then rewarmed and reperfused using modifications of a closed circuit, isolated, beating and ventilated heart-lung preparation. Positive pressure mechanical ventilation was also employed, and epicardial defibrillation was applied to elicit native cardiac sinus rhythm. Videoscopy, fluoroscopy, ultrasound, and infrared imaging were performed for anatomical and experimental study.

Results: Systolic and diastolic left ventricular pressures observed for human and swine specimens were 68/2 ± 11/7 and 74/3 ± 17/5 mmHg, respectively, with associated native heart rates of 80 ± 7 and 96 ± 16 beats per minute. High-resolution imaging within functioning human pulmonary vasculature was obtained among other anatomies of interest. Note that one human specimen elicited poor cardiac performance post defibrillation.

Conclusions: We report the first dynamic videoscopic images of the pulmonary vasculature during viable cardiopulmonary function in isolated reanimated heart-lung blocs. This experimental approach provides unique in vitro opportunities for the study of novel medical therapeutics applied to large mammalian, including human, heart-lung specimens.

背景:体外分离心脏制剂是心脏解剖学和生理学研究以及临床前设备测试的重要工具。这些制剂为研究人员提供了高水平的血流动力学控制,独立于宿主或系统相互作用。在这里,我们假设恢复的人和猪心肺块可以通过清晰的灌注重新激活,并引发可行的心脏动力学和肺功能。此外,这种方法将促进多模态成像,这对于功能解剖学和设备-组织相互作用的研究特别有价值。使用类似于心脏移植的技术,获得了5个人和18个猪的心肺制剂。然后使用改良的闭路、分离、跳动和通气心肺准备物对标本进行再加热和再灌注。同时采用正压机械通气,心外膜除颤以诱发原生心脏窦性心律。采用视频、透视、超声和红外成像进行解剖和实验研究。结果:人类和猪的左心室收缩压和舒张压分别为68/2±11/7和74/3±17/5 mmHg,相应的自然心率为80±7和96±16次/分钟。高分辨率成像功能的人肺血管系统中获得其他解剖感兴趣。注意,一个人体标本在除颤后表现不佳。结论:我们首次报道了在孤立的复苏心肺块存活的心肺功能期间肺血管的动态视频图像。这种实验方法为研究适用于大型哺乳动物(包括人类)心肺标本的新型医学疗法提供了独特的体外机会。
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引用次数: 7
Renal effects of angiotensin II in the newborn period: role of type 1 and type 2 receptors. 新生儿期血管紧张素 II 对肾脏的影响:1 型和 2 型受体的作用。
Q1 Biochemistry, Genetics and Molecular Biology Pub Date : 2016-04-18 DOI: 10.1186/s12899-016-0022-3
Angela E Vinturache, Francine G Smith

Background: Evidence suggests a critical role for the renin-angiotensin system in regulating renal function during postnatal development. However, the physiological relevance of a highly elevated renin-angiotensin system early in life is not well understood, nor which angiotensin receptors might be involved. This study was designed to investigate the roles of angiotensin receptors type 1 (AT1R) and type 2 (AT2R) in regulating glomerular and tubular function during postnatal development.

Methods: The renal effects of the selective antagonist to AT1R, ZD 7155 and to AT2R, PD 1233319 were evaluated in two groups of conscious chronically instrumented lambs aged ~ one week (N = 8) and ~ six weeks (N = 10). Two experiments were carried out in each animal and consisted of the assessment of renal variables including glomerular and tubular function, for 30 min before (Control) and 60 min after infusion of ZD 7155 and PD 123319, respectively. Statistical significance was determined using parametric testing (Student t-test, analysis of variance ANOVA) as appropriate.

Results: ZD 7155 infusion was associated with a significant decrease in glomerular filtration rate and filtration fraction at one but not six weeks; urinary flow rate decreased significantly in older animals, whereas sodium excretion and free water clearance were not altered. There was an age-dependent effect on potassium handling along the nephron, potassium excretion decreasing after ZD 7155 infusion in younger but not in older lambs. PD 123319 had no significant effects on glomerular filtration rate and tubular function in either age group.

Conclusions: These results provide evidence to support an important role for AT1Rs in mediating the renal effects of angiotensin II during postnatal maturation in conscious developing animals. In contrast to a role for AT2Rs later in life, there appears to be no role for AT2Rs in influencing the renal effects of Angiotensin II in the postnatal period.

背景:有证据表明,肾素-血管紧张素系统在出生后的发育过程中对肾功能的调节起着至关重要的作用。然而,人们对生命早期肾素-血管紧张素系统高度升高的生理相关性以及哪些血管紧张素受体可能参与其中并不十分清楚。本研究旨在探讨 1 型(AT1R)和 2 型(AT2R)血管紧张素受体在调节出生后发育过程中肾小球和肾小管功能中的作用:方法:在两组年龄约为一周(N = 8)和约为六周(N = 10)的有意识的慢性器械麻醉羔羊中评估 AT1R 选择性拮抗剂 ZD 7155 和 AT2R 选择性拮抗剂 PD 1233319 对肾脏的影响。每只动物分别在输注 ZD 7155(对照组)前 30 分钟和输注 PD 123319 后 60 分钟进行了两次实验,评估肾脏变量,包括肾小球和肾小管功能。统计意义酌情采用参数检验(学生 t 检验、方差分析 ANOVA)来确定:输注 ZD 7155 会导致肾小球滤过率和滤过率在一周内显著下降,但在六周内不会;年龄较大的动物尿流率显著下降,而钠排泄和自由水清除率没有变化。对肾小球钾处理的影响与年龄有关,输注 ZD 7155 后,年龄较小的羔羊钾排泄量减少,而年龄较大的羔羊则没有减少。PD 123319 对两个年龄组的肾小球滤过率和肾小管功能均无明显影响:这些结果提供了证据,支持 AT1R 在有意识的发育中动物出生后成熟过程中介导血管紧张素 II 对肾脏影响的重要作用。与 AT2R 在生命后期的作用不同,AT2R 在影响血管紧张素 II 在出生后对肾脏的影响方面似乎没有作用。
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引用次数: 0
Subcellular dissemination of prothymosin alpha at normal physiology: immunohistochemical vis-a-vis western blotting perspective 正常生理下胸腺素α原的亚细胞散布:免疫组织化学相对于免疫印迹的观点
Q1 Biochemistry, Genetics and Molecular Biology Pub Date : 2016-03-01 DOI: 10.1186/s12899-016-0021-4
C. Kijogi, C. Khayeka–Wandabwa, K. Sasaki, Yoshimasa Tanaka, H. Kurosu, H. Matsunaga, H. Ueda
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引用次数: 16
Hypoxia mediated pulmonary edema: potential influence of oxidative stress, sympathetic activation and cerebral blood flow. 缺氧介导的肺水肿:氧化应激、交感神经激活和脑血流的潜在影响。
Q1 Biochemistry, Genetics and Molecular Biology Pub Date : 2015-10-09 DOI: 10.1186/s12899-015-0018-4
Shadi Khademi, Melinda A Frye, Kimberly M Jeckel, Thies Schroeder, Eric Monnet, Dave C Irwin, Patricia A Cole, Christopher Bell, Benjamin F Miller, Karyn L Hamilton

Background: Neurogenic pulmonary edema (NPE) is a non-cardiogenic form of pulmonary edema that can occur consequent to central neurologic insults including stroke, traumatic brain injury, and seizure. NPE is a public health concern due to high morbidity and mortality, yet the mechanism(s) are unknown. We hypothesized that NPE, evoked by cerebral hypoxia in the presence of systemic normoxia, would be accompanied by sympathetic activation, oxidative stress, and compensatory antioxidant mechanisms.

Methods: Thirteen Walker hounds were assigned to cerebral hypoxia (SaO2 ~ 55 %) with systemic normoxia (SaO2 ~ 90 %) (CH; n = 6), cerebral and systemic (global) hypoxia (SaO2 ~ 60 %) (GH; n = 4), or cerebral and systemic normoxia (SaO2 ~ 90 %) (CON; n = 3). Femoral venous (CH and CON) perfusate was delivered via cardiopulmonary bypass to the brain and GH was induced by FiO2 = 10 % to maintain the SaO2 at ~60 %. Lung wet to lung dry weight ratios (LWW/LDW) were assessed as an index of pulmonary edema in addition to hemodynamic measurements. Plasma catecholamines were measured as markers of sympathetic nervous system (SNS) activity. Total glutathione, protein carbonyls, and malondialdehyde were assessed as indicators of oxidative stress. Brain and lung compensatory antioxidants were measured with immunoblotting.

Results: Compared to CON, LWW/LDW and pulmonary artery pressure were greater in CH and GH. Expression of hemeoxygenase-1 in brain was higher in CH compared to GH and CON, despite no group differences in oxidative damage in any tissue. Catecholamines tended to be higher in CH and GH.

Conclusion: Cerebral hypoxia, with systemic normoxia, is not systematically associated with an increase in oxidative stress and compensatory antioxidant enzymes in lung, suggesting oxidative stress did not contribute to NPE in lung. However, increased SNS activity may play a role in the induction of NPE during hypoxia.

背景:神经源性肺水肿(NPE)是一种非心源性肺水肿,可发生于中枢神经损伤,包括中风、外伤性脑损伤和癫痫发作。由于发病率和死亡率高,非肺栓塞是一个令人关注的公共卫生问题,但其机制尚不清楚。我们假设NPE是在全身缺氧的情况下由大脑缺氧引起的,并伴有交感神经激活、氧化应激和代偿性抗氧化机制。方法:将13只沃克犬分为脑缺氧组(SaO2 ~ 55%)和全身缺氧组(SaO2 ~ 90%) (CH;n = 6),脑及全身(全身)缺氧(SaO2 ~ 60%) (GH;n = 4),或脑及全身缺氧(SaO2 ~ 90%) (CON;n = 3)。体外循环将股静脉(CH)和股静脉(CON)灌注至脑,FiO2 = 10%诱导GH,使SaO2维持在~ 60%。除血流动力学测量外,还评估肺湿重比和肺干重比(LWW/LDW)作为肺水肿指标。测定血浆儿茶酚胺作为交感神经系统(SNS)活性的标志物。总谷胱甘肽、蛋白羰基和丙二醛被评估为氧化应激的指标。用免疫印迹法测定脑和肺代偿性抗氧化剂。结果:与对照组相比,chh和GH组LWW/LDW和肺动脉压升高。CH脑组织中血红素加氧酶-1的表达高于GH和CON,尽管任何组织的氧化损伤均无组间差异。儿茶酚胺在CH和GH中趋于较高。结论:脑缺氧伴全身性缺氧与肺氧化应激和代偿性抗氧化酶升高无系统性关联,提示氧化应激与肺NPE无关。然而,SNS活动的增加可能在缺氧时NPE的诱导中起作用。
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引用次数: 11
Effects of postnatal growth restriction and subsequent catch-up growth on neurodevelopment and glucose homeostasis in rats. 出生后生长限制和随后的追赶生长对大鼠神经发育和葡萄糖稳态的影响。
Q1 Biochemistry, Genetics and Molecular Biology Pub Date : 2015-06-05 DOI: 10.1186/s12899-015-0017-5
Erica E Alexeev, Bo Lönnerdal, Ian J Griffin

Background: There is increasing evidence that poor growth of preterm infants is a risk factor for poor long-term development, while the effects of early postnatal growth restriction are not well known. We utilized a rat model to examine the consequences of different patterns of postnatal growth and hypothesized that early growth failure leads to impaired development and insulin resistance. Rat pups were separated at birth into normal (N, n = 10) or restricted intake (R, n = 16) litters. At d11, R pups were re-randomized into litters of 6 (R-6), 10 (R-10) or 16 (R-16) pups/dam. N pups remained in litters of 10 pups/dam (N-10). Memory and learning were examined through T-maze test. Insulin sensitivity was measured by i.p. insulin tolerance test and glucose tolerance test.

Results: By d10, N pups weighed 20% more than R pups (p < 0.001). By d15, the R-6 group caught up to the N-10 group in weight, the R-10 group showed partial catch-up growth and the R-16 group showed no catch-up growth. All R groups showed poorer scores in developmental testing when compared with the N-10 group during T-Maze test (p < 0.05). Although R-16 were more insulin sensitive than R-6 and R-10, all R groups were more glucose tolerant than N-10.

Conclusion: In rats, differences in postnatal growth restriction leads to changes in development and in insulin sensitivity. These results may contribute to better elucidating the causes of poor developmental outcomes in human preterm infants.

背景:越来越多的证据表明,早产婴儿生长不良是长期发育不良的危险因素,而出生后早期生长限制的影响尚不清楚。我们利用一个大鼠模型来检查不同的出生后生长模式的后果,并假设早期生长失败导致发育受损和胰岛素抵抗。大鼠幼仔在出生时被分为正常(N, N = 10)窝和限制摄食(R, N = 16)窝。11 d时,将R只幼崽重新随机分为6只(R-6)、10只(R-10)和16只(R-16) /只的窝。N只幼崽,每胎10只(N-10)。通过t -迷宫测试记忆和学习能力。胰岛素敏感性采用胰岛素耐量试验和葡萄糖耐量试验。结果:到第10天,N组幼鼠的体重比R组幼鼠重20% (p)。结论:出生后生长限制的差异导致大鼠发育和胰岛素敏感性的变化。这些结果可能有助于更好地阐明人类早产儿发育不良的原因。
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引用次数: 17
期刊
BMC Physiology
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