947 resultados para BOMBINA-MAXIMA SKIN


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In mammals, trefoil factor family (TFF) proteins are involved in mucosal maintenance and repair, and they are also implicated in tumor suppression and cancer progression. A novel two domain TFF protein from frog Bombina maxima skin secretions (Bm-TFF2) has been purified and cloned. It activated human platelets in a dose-dependent manner and activation of integrin a(11b)beta(3) was involved. Aspirin and apyrase did not largely reduce platelet response to Bm-TFF2 (a 30% inhibition), indicating that the aggregation is not substantially dependent on ADP and thromboxane A2 autocrine feedback. Elimination of external Ca2+ with EGTA did not influence the platelet aggregation induced by Bm-TFF2, meanwhile a strong calcium signal (cytoplasmic Ca2+ release) was detected, suggesting that activation of phospholipase C (PLC) is involved. Subsequent immunoblotting revealed that, unlike in platelets activated by stejnulxin (a glycoprotein VI agonist), PLC gamma 2 was not phosphorylated in platelets activated by Bm-TFF2. FITC-labeled Bm-TFF2 bound to platelet membranes. Bm-TFF2 is the first TFF protein reported to possess human platelet activation activity. (c) 2005 Elsevier Inc. All rights reserved.

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Albumin, the most abundant protein components of blood plasma, is synthesized and secreted by liver cells in vertebrates. Recently, it was demonstrated that frog Bombina maxima albumin is also expressed in skin. Both B. maxima albumins from skin and serum

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In vertebrates, non-lens beta gamma-crystallins are widely expressed in various tissues but their functions are unknown. The molecular mechanisms of trefoil factors, initiators of mucosal healing and being greatly involved in tumorigenesis, have remained

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In vertebrates, non-lens beta gamma-crystallins are widely expressed in various tissues, but their functions are unknown. The molecular mechanisms of trefoil factors, initiators of mucosal healing and being greatly involved in tumorigenesis, have remained

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Albumin, the most abundant protein components of blood plasma, is synthesized and secreted by liver cells in vertebrates. Recently, it was demonstrated that frog Bombina maxima albumin is also expressed in skin. Both B. maxima albumins from skin and serum (BmA-skin and BmAserum) have similar biochemical characteristics except that the former contains haem b. Present studies showed that BmA-skin exhibited cytotoxic activity on H9 and C8166 cells. Pretreated with hemin to induce erythroid differentiation, K562 cells lost their resistance to cytotoxicity of BmAskin. After treating cells with BmA-skin for 48 h, 50 percentage cytotoxic concentrations (CC50) of BmA-skin on H9, C8166 and hemin-treated K562 cells were 1.31±0.09, 1.59±0.08 and 2.28±0.06 μM, respectively. The cell death induced by BmA-skin was mediated by apoptosis of the tested cell lines, as demonstrated by nuclear morphological changes, DNA fragmentation and DNA hypodiploidy of apoptosis cells. At BmA-skin concentration of 2 μM, 27.3%, 19.7% and 17.8% of H9, C8166 and hemin-treated K562 cells were found to be apoptotic. In contrast, BmA-serum possessed no cytotoxic and apoptosis-inducing activity on all the cell lines tested, even with concentration used up to 15 μM. These results indicated that bound haem b in BmA-skin contributed significantly to its cytotoxic and apoptosis-inducing activity on the cell lines assayed.

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Amphibian skin secretions are rich in antimicrobial peptides acting as important components of innate defense system against invading microorganisms. A novel type of peptide, designated as maximin S, was deduced by random sequencing of 793 clones from a constructed Bombina maxima skin cDNA library. The putative primary structures of maximin S peptides can be grouped into five species, in which maximin S I has 14 amino acid residues and the rest of maximin S peptides (S2-S5) all have 18 amino acid residues. Unlike most of the amphibian antimicrobial peptides so far identified, the newly characterized four maximin S precursors are composed of maximin S I and different combinations of tandem repeated maximin S2-S5 linked by internal peptides. Except maximin S I, the predicted secondary structures of maximin S2-S5 show a similar amphipathic alpha-helical structure. MALDI-TOF mass spectrometry analysis of partially isolated skin secretions of the toad indicates that most of the deduced maximin S peptides are expressed. Two deduced maximin S peptides (S1, S4) were synthesized and their antimicrobial activities were tested. Maximin S4 only had an antibiotic activity against mycoplasma and had no antibacterial or antifungal activity toward tested strains. Maximin S1 had no activity under the same conditions. (C) 2004 Elsevier Inc. All rights reserved.

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非晶状体-晶状体蛋白质(non-lens -crystallins)在脊椎动物中以一簇的基 因家族的形式存在,在各种上皮细胞中广泛表达,但对其在体内承担的功能,人 们几乎一无所知。三叶因子蛋白(trefoil factors, TFFs)主要分布在胃肠道上皮和两 栖动物皮肤表面,许多研究表明该家族的蛋白质,在粘膜保护,损伤修复和肿瘤 抑制中具有重要的作用;但是自发现以来,TFFs 一直作为孤儿配基存在,对于 其作用的机制了解得很少。人们从来没有把两个家族的蛋白质联系在一起来考虑 过。 本实验室从中国特有的两栖动物大蹼铃蟾(Bombina maxima)皮肤分泌物中, 分离到这两个家族的蛋白质的天然结合在一起的复合物,并命名为:非晶状体- 晶状体蛋白和三叶因子蛋白复合物(non-lens -crystallin and treifol factor complex, -CAT)。尽管在低剂量下,-CAT 已对小鼠,大鼠和兔有致死活性, 但其结构与人源的non-lens -crystallins 和TFFs 的同源性,提示了它可能在正 常的生理功能中起到重要作用,也为揭示两类重要的蛋白质的功能和作用机制提 供了可能性。本研究工作,在多种细胞株中,对-CAT 的生物学活性作了详细 的研究,并对其作用机制进行了进一步深入的探讨。 我们原代培养了人脐静脉血管内皮细胞(HUVEC) ,兔主动脉内皮细胞 (RAEC),兔心内皮细胞(REEC);培养了多种肿瘤细胞株。-CAT 能够引起多种 贴壁细胞的脱落。-CAT 在高剂量下能够引起这些细胞的凋亡;但是在不同的 细胞株中,发生凋亡的通路可能是不同的。在低剂量下,-CAT 能够促进细胞 的迁移,对HUVEC 具有诱导伤口修复的活性。 以HUVEC 细胞为模型,我们探讨了-CAT 的作用机制。在激光共聚焦显 微镜下,观察到-CAT 诱导HUVEC 发生囊泡化,这个效应是剂量依赖的;囊 泡化的发生不依赖于NH4Cl 的存在,但是NH4Cl 能够增大囊泡化的效应。在荧 光染料Cy3 直接标记-CAT 时,观察到-CAT 被定向运输到细胞核上。荧光染 料FITC 分别标记-CAT 的轻链和重链的多克隆抗体,免疫荧光染色发现,在较 短的时间(5 min)内, -CAT 已经进入细胞,并有部分分子被运输到细胞核上。随 着时间增加到30 min,轻链和重链在核上的比例也渐增加;到2 小时,-CAT的重链全部集中在细胞核上,而-CAT 的轻链则退出核外,主要聚集在细胞核 周围。核定位显示-CAT 分子进入HUVEC 细胞核,可能在基因的转录调节中 发挥作用。我们运用基因芯片检测了加药处理前后细胞蛋白质表达水平的变化。 在四组重复实验中均显示,加入-CAT 处理后,有121 个基因发生上调,这些 基因在调节细胞的生存和死亡中具有复杂的功能。其中核受体蛋白质家族 (NR4A1 等)的变化最为明显。而其他的基因包括调节细胞早期生长,凋亡, 炎症反应的相关基因和金属蛋白酶。同时,加入-CAT 处理后,仅有2 个基因 发生下调,包括胶原I,这为解释细胞发生脱落和调亡提供了分子基础。 本研究工作揭示了非晶状体-晶状体蛋白和三叶因子蛋白的相互作用,共 同定位到细胞核上,并调节基因的转录,首次提示非晶状体-晶状体蛋白可能 参与一条全新的细胞信号调节途径,在组织平衡,肿瘤发生和胚胎发育中起到重 要的作用;同时也为三叶因子蛋白的分子作用机制的解析提供了一种新的可能 性。

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通过对两栖类动物大蹼铃蟾(B朋b了na勿日对朋)皮肤分泌物及匀浆物的分离,纯化,从其碱性组分中得到了全新的三叶因子多肤(BIn--TFFZ)和膜联蛋白H相关蛋白(BAIIRP),它们分别具有诱导或抑制人血小板活化的全新功能。以血小板膜糖蛋白GPVI受体激动剂stejnulxin为对照,研究了Bm一TFFZ活化人血小板的信号传导途径。哺乳动物的三叶因子(TFF)蛋白的主要功能在于通过修复粘膜损伤,维持粘膜层的完整。它们在肿瘤抑制及癌症侵润方面也有一定程度的作用。我们从两栖类动物大蹼铃蟾皮肤分泌物分离,纯化而得到了一个全新的三叶因子多肤(Bm一TFFZ)。它是单亚基蛋白,表观分子量为13000,并具有全新的诱导人血小板活化的功能,我们研究了其诱导人血小板活化的活性的量效关系。它对血小板的激活涉及血小板整合素a:Ibp3的活化,Bm一TFFZ可诱导经阿斯匹林及三磷酸腺昔"双磷酸酶(Apyrase)处理的血小板的聚集,表明B,TFFZ的活性不依赖于血小板的ADP及血栓嗯烷A2(TXAZ)的自泌正反馈。F工TC标记的B爪一TFFZ蛋白能与血小板膜结合。通过专一性药理学抑制剂的研究,我们初步排除了Bm一TFFZ蛋白作用于血小板膜已知的G一蛋白偶联受体(如ADP,TXAZ及血小板活化因子受体)的可能性。以血小板GPVI激动剂stejnulxin为对照,我们仔细研究了Bm一TFFZ蛋白刺激血小板后的信号传导分子事件,发现其酪氨酸磷酸化图谱明显不同于血小板GPVI激动剂5tejnu1X如,尤其是磷脂酶CYZ并不磷酸化。因此,我们认为Bm一TFFZ蛋白激活血小板的信号传导通路是活化磷脂酶C,并刺激胞内钙离子的释放,活化血小板伪:。p3,进而导致血小板的聚集。从Bm--TFFZ蛋白的cDNA克隆序列推知它由104个氨基酸组成,含有两个三叶因子结构域,与人TFFZ和非洲爪蟾xPZ序列中相同的氨基酸分别占28%及34%。为了确定两栖类的三叶因子蛋白具有诱导人血小板活化的功能,我们仔细地研究了整个分离纯化过程中所有组份的血小板聚集活性并比较了它们的相对活性差异。Bm一TFFZ是第一个来自两栖类动物的血小板激动剂,也是我们第一个报道的具有诱导血小板聚集活性的三叶因子多肤。·我们还通过阴离子交换,凝胶过滤和阳离子交换层析,从大蹼铃蟾皮肤匀浆物中纯化了一个表观分子量为33kD。的单链蛋白。N一末端序列比较分析显示,该·蛋白与来自非洲爪蟾、红色原鸡和人膜联蛋白H的N一末端序列相同的氨基酸分别占70%、64%和56%。该蛋白具有以钙依赖的方式抑制专一性血小板膜糖蛋白VI(GPVI)受体激动剂-Stejnu1Xin诱导洗涤人血小板聚集的生物学功能,最大抑制率达48%。结合其N一末端序列搜索结果及其活性的钙依赖性,推测该蛋白是与膜联蛋白H相关的一类蛋白质。

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Amphibian skin contains rich bradykinin-related peptides, but the mode of biosynthesis of these peptides is unknown. In the present study, a novel bradykinin-related peptide, termed bombinakinin M, was purified from skin secretions of the Chinese red bell

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Two groups of antimicrobial peptides have been isolated from skin secretions of Bombina maxima. Peptides in the first group, named maximins 1, 2, 3, 4 and 5, are structurally related to bombinin-like peptides (BLPs). Unlike BLPs, sequence variations in maximins occurred all through the molecules. In addition to the potent antimicrobial activity, cytotoxicity against tumor cells and spermicidal action of maximins, maximin 3 possessed a significant anti-HIV activity. Maximins 1 and 3 were toxic to mice with LD50 values of 8.2 and 4.3 mg/kg, respectively. Peptides in the second group, termed maximins H1, H2, H3 and H4, are homologous with bombinin H peptides. cDNA sequences revealed that one maximin peptide plus one maximin H peptide derived from a common larger protein. (C) 2002 Elsevier Science Inc. All rights reserved.

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A novel trypsin inhibitor was identified and purified from skin secretions of Chinese red-belly toad Bombina maxima. The partial N-terminal 29 amino acid residues of the peptide, named BMTI, were determined by automated Edman degradation. This allowed the cloning of a full-length cDNA encoding BMTI from a cDNA library prepared from the toad skin. The deduced complete amino acid sequence of BMTI indicates that mature BMTI is composed of 60 amino acids. A FASTA search in the databanks revealed that BMTI exhibits 81.7% sequence identity with BSTI, a trypsin/thrombin inhibitor from European toad Bombina bombina skin secretions. Sequence differences between BMTI and BSTI were due to 11 substitutions at positions 2, 9, 25, 27, 36-37, 39, 41-42, 50 and 56. BMTI potently inhibited trypsin with a K-i value of 0.06 muM, similar to that of BSTI. However, unlike BSTI, which also inhibited thrombin with a K-i value of 1 muM, no inhibitory effect of BMTI on thrombin was observed under the assay conditions. (C) 2002 Elsevier Science Inc. All rights reserved.

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A novel 28-amino acid peptide, termed bombinakinin-GAP, was purified and characterized from skin secretions of the toad Bombina maxima. Its primary structure was established as DMYEIKQYKTAHGRPPICAPGEQCPIWV-NH2, in which two cysteines form a disulfide bond. A FASTA search of SWISS-PROT databank detected a 32% sequence identity between the sequences of the peptide and a segment of rat cocaine- and amphetamine-regulated transcript (CART). Intracerebroventricular (i.c.v.) administration of the peptide induced a significant decrease in food intake in rats, suggesting that it played a role in the control of feeding by brain. Analysis of its cDNA structure revealed that this peptide is coexpressed with bombinakinin M, a bradykinin-related peptide from the same toad. Bombinakinin-GAP appears to be the first example of a novel class of bioactive peptides from amphibian skin, which may be implicated in feeding behavior. (C) 2003 Elsevier Science Inc. All rights reserved.

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Amphibian skin is a rich resource of bioactive peptides like proline-rich bombesin from frog Bombina maxima. A novel cDNA clone encoding a precursor protein that comprises proline-rich bombesin and a novel peptide, designated as bombestatin, was isolated from a skin cDNA library of B. maxima. The predicted primary structure of the novel peptide is WEVLLNVALIRLELLSCRSSKDQDQKESCGMHSW, in which two cysteines form a disulfide bond. A BLAST search of databases did not detect sequences with significant similarity. Bombestatin possesses dose-dependent contractile activity on rat stomach strips. The differences between cDNAs encoding PR-bombesin plus bombestatin and PR-bombesin alone are due to fragment insertions located in 3'-coding region and 3'-untranslational region, respectively. (c) 2005 Elsevier B.V. All rights reserved.

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Amphibian skin contains rich neuropeptides. In the present study, a novel neuromedin U (NmU) analog was isolated from skin secretions of Chinese red belly Load Bombina maxima. Being 17-amino acids long, its primary structure was established as DSSGIVGRPFFLFRPRN-NH2, in which the C-terminal 8-residue segment (FFLFRPRN) is the same as that of rat NmU, while the N-terminal part DSSGIVGRP shows a great sequence variation compared with those of NmU peptides from different resources. The peptide, named Bm-NmU-17, was found to elicit concentration-dependent contractile effects on smooth muscle of rat uterus horns. The cDNA Structure of the peptide, as obtained by a 3'-RACE strategy and subsequently cloning from a skin cDNA library, was found to contain a coding region of 438 nucleotides. The encoded precursor is composed of 145 amino acids with a single copy of Bm-NmU-17 located towards the C-terminus. The sequence of the peptide is preceded by a dibasic site (Lys-Arg) and followed by the sequence of Gly-Arg-Lys, providing the sites of cleavage and releasing of the mature peptide. (c) 2005 Elsevier B.V. All rights reserved.