首页> 外文期刊>Investigative ophthalmology & visual science >Functional Role of hCNGB3 in Regulation of Human Cone CNG Channel: Effect of Rod Monochromacy-Associated Mutations in hCNGB3 on Channel Function.
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Functional Role of hCNGB3 in Regulation of Human Cone CNG Channel: Effect of Rod Monochromacy-Associated Mutations in hCNGB3 on Channel Function.

机译:hCNGB3在调节人锥CNG通道中的功能作用:hCNGB3中杆单色性相关突变对通道功能的影响。

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PURPOSE. The human cone photoreceptor cyclic nucleotide-gated (CNG) channel comprises alpha- and beta-subunits, which are respectively encoded by hCNGA3 and hCNGB3. The purpose was to examine the functional role of hCNGB3 in modulation of human cone CNG channels and to characterize functional consequences of rod monochromacy-associated mutations in hCNGB3 (S435F and D633G). METHODS. Macroscopic patch currents were recorded from human embryonic kidney (HEK) 293 cells expressing homomeric (hCNGA3 and hCNGB3) and heteromeric (hCNGA3/hCNGB3, hCNGA3/hCNGB3-S435F, and hCNGA3/hCNGB3-D633G) channels using inside-out patch-clamp technique. RESULTS. Both hCNGA3 homomeric and hCNGA3/hCNGB3 heteromeric channels were activated by cGMP, with half-maximally activating concentration (K(1/2)) of 11.1 +/- 1.0 and 26.2 +/- 1.9 micro M, respectively. The hCNGA3 channels appeared to be more sensitive to inhibition by extracellular Ca(2+) compared with hCNGA3/hCNGB3 channels, when assessed by the degree of outward rectification. Coexpression of either of rod monochromacy-associated mutants of hCNGB3 with hCNGA3 significantly reduced K(1/2) value for cGMP but little affected the sensitivity to extracellular Ca(2+), compared with wild-type heteromeric channels. The selectivity of hCNGA3, hCNGA3/hCNGB3, hCNGA3/hCNGB3-S435F, and hCNGA3/hCNGB3-D633G channels for monovalent cations were largely similar. Immunoprecipitation experiments showed association of hCNGA3 subunit with both of wild-type and mutant hCNGB3 subunits. CONCLUSIONS. The hCNGB3 plays an important modulatory role in the function of human cone CNG channels with respect to cGMP and extracellular Ca(2+) sensitivities. The rod monochromacy-associated S435F and D633G mutations in hCNGB3 evokes a significant increase in the apparent affinity for cGMP, which should alter cone function and thereby contribute at least partly to pathogenesis of the disease.
机译:目的。人视锥细胞受体环状核苷酸门控(CNG)通道包含分别由hCNGA3和hCNGB3编码的α和β亚基。目的是检查hCNGB3在调节人锥状CNG通道中的功能作用,并表征hCNGB3中杆单色性相关突变(S435F和D633G)的功能后果。方法。使用内-外膜片钳技术从表达同源(hCNGA3和hCNGB3)和异聚(hCNGA3 / hCNGB3,hCNGA3 / hCNGB3-S435F和hCNGA3 / hCNGB3-D633G)通道的人胚胎肾(HEK)293细胞中记录宏观的膜片电流。结果。 hCNGA3同源和hCNGA3 / hCNGB3异源通道均被cGMP激活,最大半数激活浓度(K(1/2))分别为11.1 +/- 1.0和26.2 +/- 1.9 microM。通过向外整流的程度进行评估时,与hCNGA3 / hCNGB3通道相比,hCNGA3通道似乎对细胞外Ca(2+)的抑制作用更为敏感。与hCNGA3的hCNGB3杆单色性相关的任何突变体的共表达显着降低了cGMP的K(1/2)值,但与野生型异聚通道相比,对细胞外Ca(2+)的敏感性影响很小。 hCNGA3,hCNGA3 / hCNGB3,hCNGA3 / hCNGB3-S435F和hCNGA3 / hCNGB3-D633G通道对单价阳离子的选择性非常相似。免疫沉淀实验表明,hCNGA3亚基与野生型和突变型hCNGB3亚基均相关。结论。 hCNGB3在人类锥状CNG通道功能方面对cGMP和细胞外Ca(2+)敏感性起重要的调节作用。 hCNGB3中与杆单色性相关的S435F和D633G突变引起对cGMP的表观亲和力的显着增加,这将改变视锥细胞的功能,从而至少部分地导致疾病的发病。

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