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Triplex-DNA stabilization by hydralazine and the presence of anti-(triplex DNA) antibodies in patients treated with hydralazine.

机译:肼苯哒嗪对三联体DNA的稳定作用以及接受肼苯哒嗪治疗的患者中抗(三联体DNA)抗体的存在。

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摘要

Hydralazine is an antihypertensive drug that elicits andti-nuclear antibodies in patients as an adverse effect. We investigated the ability of hydralazine to promote/stabilize the triplex DNA form of poly(dA).2poly(dT). Under conditions of low ionic strength, the polynucleotide melted as a double helix with a melting temperature (Tm) of 55.3 degrees C. Hydralazine destabilized this duplex form by reducing its Tm to 52.5 degrees C. Spermidine (2.5 microM), a natural polyamine, provoked the triplex form of poly(dA)-.2poly(dT) with two melting transitions, Tm1 of 42.8 degrees C corresponding to triplex-->duplex+single-stranded DNA and Tm2 of 65.4 degrees C, corresponding to duplex melting. Triplex DNA thus formed in the presence of spermidine was further stabilized by hydralazine (250 microM) with a Tm1 of 53.6 degrees C. A similar stabilization effect of hydralazine was found on triplex DNA formed in the presence of 5 mM Mg2+. CD spectra revealed conformational perturbations of DNA in the presence of spermidine and hydralazine. These results support the hypothesis that hydralazine is capable of stabilizing unusual forms of DNA. In contrast with the weak immunogenicity of DNA in its right-handed B-DNA conformation, these unusual forms are immunogenic and have the potential to elicit anti-DNA antibodies. To test this possibility, we analysed sera from a panel of 25 hydralazine-treated patients for anti-(triplex DNA) antibodies using an ELISA. Our results showed that 72% of sera from hydralazine-treated patients contained antibodies reacting toward the triplex DNA. In contrast, there was no significant binding of normal human sera to triplex DNA. Taken together our data indicate that hydralazine and related drugs might exert their action by interacting with DNA and stabilizing higher-order structures such as the triplex DNA.
机译:肼屈嗪是一种降压药,在患者中会引起对地核抗体的副作用。我们研究了肼苯哒嗪促进/稳定poly(dA).2poly(dT)的三链体DNA形式的能力。在低离子强度的条件下,多核苷酸以55.3摄氏度的熔融温度(Tm)熔化为双螺旋。肼屈嗪通过将其Tm降低至52.5摄氏度而使该双链体形式不稳定。亚精胺(2.5 microM),一种天然多胺,激发了具有两个熔解转变的poly(dA)-。2poly(dT)的三链体形式,Tm1为42.8摄氏度,对应于三链->双链体+单链DNA,Tm2为65.4摄氏度,对应于双链融解。因此,在亚精胺存在下形成的三链体DNA通过肼苯甲醛(250 microM)在53.6摄氏度的Tm1下进一步稳定。发现肼苯哒嗪对在5 mM Mg2 +存在下形成的三链DNA具有类似的稳定作用。 CD光谱揭示了在亚精胺和肼苯哒嗪存在下DNA的构象扰动。这些结果支持了肼苯哒嗪能够稳定异常形式的DNA的假设。与右旋B-DNA构型的DNA免疫原性弱相反,这些异常形式具有免疫原性,并具有引发抗DNA抗体的潜力。为了测试这种可能性,我们使用ELISA分析了一组25例接受肼屈嗪治疗的患者的血清中的抗(三重DNA)抗体。我们的结果表明,接受肼屈嗪治疗的患者血清中有72%含有对三链DNA发生反应的抗体。相反,正常人血清与三链DNA没有明显的结合。综上所述,我们的数据表明肼苯哒嗪和相关药物可能通过与DNA相互作用并稳定三联DNA等更高阶结构而发挥作用。

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