降钙素基因相关肽肽段的抗原性和免疫原性

用固相合成法合成了有关降钙素基因相关肽ＣＧＲＰ五个肽段。它们的氨基酸顺序分别为：ＣＧＲＰ－１（２４－３７）;ＣＧＲＰ－２（１４－３７）;ＣＧＲＰ－３（９－２３）;ＣＧＲＰ－４（１－２３）和ＣＧＲＰ－５（１－１３）。用酶标方法测定了它们的抗原性,发现ＣＧＲＰ－２和ＣＧＲＰ－１能够很好地与抗ＣＧＲＰ抗血清结合。将ＣＧＲＰ－１;ＣＧＲＰ－３和ＣＧＲＰ－５分别免疫兔子,获得的抗血清分别与ＣＧＲＰ进行反应,发现只有抗ＣＧＲＰ－１的抗血清能够与ＣＧＲＰ很好地结合。因此,可以推测ＣＧＲＰ的羧端部分是其免疫活性部位。     

降钙素基因相关肽肽段的抗原性和免疫原性

用固相合成法合成了有关降钙素基因相关肽ＣＧＲＰ五个肽段。它们的氨基酸顺序分别为：ＣＧＲＰ－１（２４－３７）;ＣＧＲＰ－２（１４－３７）;ＣＧＲＰ－３（９－２３）;ＣＧＲＰ－４（１－２３）和ＣＧＲＰ－５（１－１３）。用酶标方法测定了它们的抗原性,发现ＣＧＲＰ－２和ＣＧＲＰ－１能够很好地与抗ＣＧＲＰ抗血清结合。将ＣＧＲＰ－１;ＣＧＲＰ－３和ＣＧＲＰ－５分别免疫兔子,获得的抗血清分别与ＣＧＲＰ进行反应,     

降钙素的基因结构与表达调控

降钙素与降钙素基因相关肽（ＣＴ／ＣＧＲＰ）基因编码一组多肽,即降钙素（ＣＴ）、降钙素的Ｎ端肽和Ｃ端肽、降钙素基因相关肽（ＣＧＲＰ）及淀粉不溶素（Ａｍｙｌｉｎ）。ＣＴ／ＣＧＲＰ基因转录而成的ｍＲＮＡ前体,在不同组分中通过选择性加工形成ＣＴ ｍＲＮＡ或ＣＧＲＰｍＲＮＡ,再通过翻译及蛋白质加工,最后形成成熟的降钙素或降钙素基因相关肽。本简单介绍一下降钙素的基因结构及表达调控方面的研究进展。     

大鼠内毒素血症不同时期血CGRP和背根神经节CGRP mRNA水平的变化

本文采用逆转录聚合酶链反应（ＲＴ－ＰＣＲ）方法测定大鼠内毒素血症不同时期胸腰段背根神经节降钙素基因相关肽（ＣＧＲＰ）ｍＲＮＡ水平的改变,结合血浆ＣＧＲＰ水平的改变,以期全面了解大鼠内毒不血症不同时期ＣＧＲＰ释放与合成的变化。结果显示：注射内毒素（５ｍｇ／ｋｇ）后３０ｍｉｎ时,大鼠血浆ＣＧＲＰ开始增高,而背根神经节ＣＧＲＰ ｍＲＮＡ水平无明显变化;注射内毒素后３ｈ时,血浆ＣＧＲＰ及背根神经节ＣＧＲＰ     

降钙素基因相关肽和心房肽对犬冠脉的舒张作用

本实验利用冠脉内给药和离体血管灌流等方法观察比较了降钙素基因相关肽（ＣＧＲＰ）和心房肽（ＡＮＰ）对犬冠脉循环的影响及其对犬大小冠状动脉的舒张作用。结果显示,ＣＧＲＰ和ＡＮＰ均能明显增加冠脉血流量、降低大小冠脉阻力,两者均呈剂量依赖性舒张大小脉冠脉血管。ＡＮＰ的作用显著小于ＣＧＲＰ,其中大冠脉对两者的反应性显著小于小冠脉,ＣＧＲＰ和ＡＮＰ对冠脉的舒张作用均无内皮依赖性。结果提示,ＣＧＲＰ和ＡＮＰ直接     

降钙素基因相关肽对家兔离体窦房结电生理活动的影响

用常规微电极方法研究了降钙素基因相关肽（ＣＧＲＰ）对家兔窦房结起搏细胞的电生理作用,并进一步探讨这种作用与钙电流的关系。结果：⑴低浓度ＣＧＲＰ（１ｎｍｏｌ／Ｌ）对窦房结动作电位各参数无显著影响;中等浓度ＣＧＲＰ（１０ｎｍｏｌ／Ｌ）可增加最大舒张期电位、动作电位幅度、０期最大除极化速率和４期自动除极速率,缩短窦性周期、动作电位复极化５０％和９０％时间,这些作用经２０ｍｉｎ达到高峰;高浓度ＣＧＲＰ（２     

恒河猴肺内CGRP及CGRP mRNA免疫组织化学和原位杂交的研究

本实验采用免疫组织化学ＡＢＣ－ＧＤＮ法和地高辛标记寡核苷酸探针原位杂交技术,研究了降钙素基因相关肽（ＣＧＲＰ）及其ｍＲＮＡ在恒河猴内的表达。结果显示ＣＧＲＰ分布于恒河猴肺内各级支气管粘膜上皮的神经内分泌细胞（ＮＥＣ）和神经上皮样小体（ＮＥＢ）中。ＣＧＲＰ杂交阳性细胞的分布与免疫组织化学的结果相同。ＣＧＲＰ ｍＲＮＡ杂交信号均匀分布于整个细胞质,而ＣＧＲＰ免疫反应物仅在神经内分泌细胞的基部更明显,说     

降钙素基因相关肽对小鼠肠道集合淋巴结T细胞及腹腔巨噬细…

本工作观察了降钙素基因相关肽（ＣＧＲＰ）对小鼠肠集合淋巴小结（ＰＰ结）Ｔ细胞和小鼠腹腔巨噬细胞功能的影响。结果表明：ＣＧＲＰ能明显抑制ＰＰ结Ｔ淋巴细胞的转化,并且这种作用与Ｔ细胞的分化增殖状态有明显关系。此外ＣＧＲＰ对腹腔巨噬细胞ＤＮＡ和蛋白质的合成也有明显的抑制作用。以上结果提示ＣＧＲＰ可能作为一种抑制型的神经内分泌免疫调节肽而对肠道免疫功能发挥着重要的调节作用。     

糖尿病大鼠肠系膜动脉降钙素基因相关肽释放减少以及一氧化氮的作用

我们以前的工作已表明,内毒素可引起降钙素基因相关肽（ＣＧＲＰ）从大鼠肠系膜动脉床释放,此作用部分是通过一氧化氮介导的。我们在离体肠系膜动脉床研究了内毒素引起糖尿病大鼠ＣＣＲＰ释放的改变以及一氧化氮所起的作用。采用ＣＣＲＰ放射免疫分析法测定灌流液中ＣＣＲＰ含量,ＲＴ－ＰＣＲ法测定背根神经节ＣＧＲＰｍＲＮＡ水平。结果显示：内毒素累积灌流引起ＣＧＲＰ浓度依赖性地释放增多,此作用在糖尿病大鼠系膜动脉术明显     

脑室内注射降钙素基因相关肽对压力感受性反射的抑制

脑室内注射降钙素基因相关肽对压力感受性反射的抑制张继峰唐朝枢１（廊坊师范专科学校生物系,廊坊１０２８４９;１北京医科大学心血管研究所）降钙素基因相关肽（Ｃａｌｃｉｔｏｎｉｎｇｅｎｅｒｅｌａｔｅｄｐｅｐｔｉｄｅ,ＣＧＲＰ）是１９８３年Ｒｏｓｅｎｆｅｌ...     

降钙素基因相关肽与动脉粥样硬化

动脉粥样硬化是心血管疾病中最常见的一种血管病变,影响着血管、免疫、代谢等系统。动脉粥样硬化发生发展是一个复杂的过程,它损伤血管内皮,平滑肌等细胞,涉及到多种细胞因子的相互作用。而CGRP具有抑制血管平滑肌增值作用,对预防血管术后再狭窄有重要意义,CGRP能舒张血管,对防治氧化应激引起的内皮损伤具有保护作用,但其机制还不完全清楚。     

降钙素基因相关肽与动脉粥样硬化

动脉粥样硬化是心血管疾病中最常见的一种血管病变,影响着血管、免疫、代谢等系统。动脉粥样硬化发生发展是一个复杂的过程,它损伤血管内皮,平滑肌等细胞,涉及到多种细胞因子的相互作用。而CGRP具有抑制血管平滑肌增值作用,对预防血管术后再狭窄有重要意义,CGRP能舒张血管,对防治氧化应激引起的内皮损伤具有保护作用,但其机制还不完全清楚。     

Calcitonin gene-related peptide: Brain and spinal action on intestinal motility

The effects of intracerebroventricular (ICV) and intrathecal (IT) administration of calcitonin gene-related peptide (CGRP) on intestinal motility were examined in conscious rats chronically fitted with intraparietal electrodes in the duodeno-jejunum and a cannula in a cerebral lateral ventricle or catheter in the subarachnoid space. ICV administration of CGRP (0.5–10 μg) restores the fasted pattern of intestinal motility in fed rats in a dose-related manner. Intrathecal administration of CGRP or calcitonin also induces fasted pattern but after a 30 min delay. These effects persisted after transection of the spinal cord and no change in intestinal motility appeared after intravenous administration of CGRP at a dose effective when given IT. This study suggests that CGRP, as calcitonin, has a neuromodulatory role in the control of intestinal motility at both brain and spinal cord levels.     

Calcitonin receptor-stimulating peptide: Its evolutionary and functional relationship with calcitonin/calcitonin gene-related peptide based on gene structure

This review focuses on the evolutionary and functional relationship of calcitonin receptor-stimulating peptide (CRSP) with calcitonin (CT)/calcitonin gene-related peptide (CGRP) in mammals. CRSP shows high sequence identity with CGRP, but distinct biological properties. CRSP genes (CRSPs) have been identified in mammals such as pigs and dogs of the Laurasiatheria, but not in primates and rodents of the Euarchontoglires or in non-placental mammals. CRSPs have genomic organizations highly similar to those of CT/CGRP genes (CT/CGRPs), which are located along with CGRPs in a locus between CYP2R1 and INSC, while the other members of the CGRP superfamily, adrenomedullin and amylin, show genomic organizations and locations distinct from CT, CGRP, and CRSP. Thus, we categorized these three peptides into the CT/CGRP/CRSP family. Non-placental mammals having one and placental mammals having multiple CT/CGRP/CRSP family genes suggests that multiplicity of CT/CGRP started at an early stage of mammalian evolution. In the placental mammals, Laurasiatheria generally possesses multiple CRSPs and only one CT/CGRP, while Euarchontoglires possesses CT/CGRP and CGRPβ but no CRSP, indicating an increase in the diversity and multiplicity of this family of genes in mammalian evolution. Phylogenetic analysis suggests that some CRSPs have been generated very recently in mammalian evolution. Taken together, the increase in the number and complexity of the CT/CGRP/CRSP family genes may have due to evolutionary pressure to facilitate adaptation during mammalian evolution. In this regard, it is important to elucidate the physiological roles of CT, CGRP and CRSP from the viewpoint of the CT/CGRP/CRSP family even in Euarchontoglires.     

Calcitonin gene-related peptide coexists with substance P in capsaicin sensitive neurons and sensory ganglia of the rat

Immunohistochemical and radioimmunoassay studies revealed that both CGRP- and SP-like immunoreactivity in the caudal spinal trigeminal nucleus and tract, the substantia gelatinosa and the dorsal cervical spinal cord as well as in cell bodies of the trigeminal ganglion and the spinal dorsal root ganglion is markedly depleted by capsaicin which is known to cause degeneration of a certain number of primary sensory neurons. Higher brain areas and the ventral spinal cord were not affected by capsaicin treatment. Furthermore CGRP and substance P-like immunoreactivity were shown to be colocalized in the above areas and to coexist in cell bodies of the trigeminal ganglion and the spinal dorsal root ganglia. It is suggested that CGRP, like substance P, may have a neuromodulatory role on nociception and peripheral cardiovascular reflexes.     

Distinct hemodynamic and gastric effects of human CGRP I and II in man

The human calcitonin gene-related peptides I and II (or and β) (CGRP I and II) are encoded by two different genes, but they have 34 of the 37 amino acid residues in common. Human CGRP I more potently stimulated blood flow through the skin and carotid artery (p<0.01), and the heart rate (p<0.05), and plasma renin activity and aldosterone secretion than human CGRP II (p<0.02). Inhibition of pentagastrin-stimulated gastric acid output, on the other hand, was only obtained with CGRP II. The separate effects of human CGRP I and II on the cardiovascular and gastric systems are presumably mediated by different receptors or receptor pathways recognized by the two closely related neuropeptides.     

降钙素基因相关肽家族受体及其受体活性修饰蛋白

降钙素基因相关肽家族是一类多功能的激素家族 ,参与人体的多种生物学功能 ,与多种疾病有关。降钙素基因相关肽受体包括降钙素受体 (CTR)和降钙素受体样受体 (CRLR) ,CTR可以独自与降钙素结合 ,而CRLR必须与一组称作受体活性修饰蛋白 (RAMPs)的蛋白质共同作用才能发挥生物学功能。综述CTR的研究概况及CRLR与RAMPs相互作用的机制和表达调控 ,以期为人们设计新型药物提供参考。     

Calcitonin gene-related peptide and its receptor in the thymus

Calcitonin gene-related peptide (CGRP), a 37-amino acid residue neuropeptide, was immunostained in rat thymus at two sites: a subpopulation of thymic epithelial cells, namely subcapsular/perivascular cells, were heavily stained besides some nerve fibers surrounding arteries and arterioles. The administration of nanomolar concentrations of rat -CGRP dose-dependently raised intracellular cyclic adenosine monophosphate (cAMP) levels in isolated rat thymocytes (half-maximum stimulation 1 nM) but not in cultured rat thymic epithelial cells. Peptides structurally related to CGRP (i.e., rat calcitonin or amylin) had no effect. CGRP(8–37), an N-terminally truncated form, acted as an antagonist. Peripheral blood lymphocytes did not respond to CGRP, suggesting that receptors are present only on a subpopulation of thymocytes but not on mature T cells. This was substantiated by visualization of CGRP receptors on single cells by use of CGRP-gold and -biotin conjugates of established biological activity: only a small proportion of isolated thymocytes was surface labeled. In situ, the CGRP conjugates labeled receptors on large thymocytes residing in the outer cortical region of rat thymus pseudolobules. Thus, immunoreactive CGRP is found in subcapsular/perivascular thymic epithelial cells and acts via specific CGRP receptors on thymocytes by raising their intracellular cAMP level. It is suggested that CGRP is a paracrine thymic mediator that might influence the differentiation, maturation, and proliferation of thymocytes.     

Inhibition of vascular smooth muscle cell proliferation in vitro by genetically engineered marrow stromal cells secreting calcitonin gene-related peptide

Calcitonin gene-related peptide (CGRP) has a beneficial effect in pulmonary hypertension and is a target for cardiovascular gene therapy. Marrow stromal cells (MSCs), also known as mesenchymal stem cells, hold promise for use in adult stem cell-based ex vivo gene therapy. To test the hypothesis that genetically engineered MSCs secreting CGRP can inhibit vascular smooth muscle cell proliferation, rat MSCs were isolated, ex vivo expanded, and transduced with adenovirus containing CGRP. Immunocytochemical analysis demonstrated that wild type rat MSCs express markers specific for stem cells, endothelial cells, and smooth muscle cells including Thy-1, c-Kit, von Willebrand Factor and alpha-smooth muscle actin. Immunocytochemistry confirmed the expression of CGRP by the transduced rat MSCs. The transduced rat MSCs released 10.3+/-1.3 pmol CGRP/1 x 10(6) cells/48 h (mean+/-S.E.M., n=3) into culture medium at MOI 300 and the CGRP-containing culture supernatant from the transduced cells inhibited the proliferation of rat pulmonary artery smooth muscle cells (PASMCs) and rat aortic smooth muscle cells (ASMCs) in culture. Co-culture of the transduced rat MSCs with rat PASMCs or rat ASMCs also inhibited smooth muscle cell proliferation. These findings suggest that this novel adult stem cell-based CGRP gene therapy has potential for the treatment of cardiovascular diseases including pulmonary hypertension.