{"title":"作为平衡调节传感器的呼吸复合体 II","authors":"Muhammad Hagras","doi":"10.1039/d4cp03552f","DOIUrl":null,"url":null,"abstract":"The succinate-ubiquinone oxidoreductase (SQR) complex connects two of the cell's most vital energy-producing metabolic processes: the tricarboxylic acid cycle and the electron transport chain. Hence, the SQR complex is essential in cell metabolism, and its malfunction leads to the progression of multiple metabolic disorders and other diseases, such as cancer. In the current study, we calculated the electron tunneling (ET) pathways between the different redox systems in the SQR complex, including the SQR ligands and the distant heme b redox center, using the broken-symmetry semi-empirical ZINDO method. Interestingly, we discovered a water channel running from the mitochondrial matrix, filling the space between Fe3S4 and heme b redox centers. To investigate the physiological function of the water channel, we performed extensive MD simulations of membrane-embedded SQR complex in small and large water boxes, representing regular (MDA) and extended (MDB) volume states, respectively. We found that under regular volume conditions (MDA), the ET reaction is conducted through both the iron-sulfur cluster chain (i.e., pathway A) and through heme b (i.e., pathway B). Hence, the SQR complex encompasses an internal interferometer similar to the Mach-Zender interferometer, such that tunneling electron experiences a self-interference effect through pathways A and B, enhancing the SQR complex's overall ET thermodynamics and favoring the forward ET direction of oxidizing succinate to fumarate and reducing ubiquinone to ubiquinol. On the other hand, we found that under extended volume conditions (MDB), the internal water channel of the SQR complex \"senses\" the expansion in the mitochondrial volume, pushing the heme b and Fe4S3 redox centers apart and hence lowering the SQR equilibrium constant to almost unity. Therefore, the SQR complex could be driven to work in the reverse direction, catalyzing the production of ubiquinone molecules essential for the physiological function of respiratory complexes I and III and restoring the inner-mitochondrial membrane potential, which leads to restoring the function of the H-K anti-porter, pumping K+ outward from the matrix and restoring the regular mitochondrial volume.","PeriodicalId":99,"journal":{"name":"Physical Chemistry Chemical Physics","volume":"61 1","pages":""},"PeriodicalIF":2.9000,"publicationDate":"2024-11-22","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":"{\"title\":\"Respiratory Complex II Acting as a Homeostatic Regulatory Sensor\",\"authors\":\"Muhammad Hagras\",\"doi\":\"10.1039/d4cp03552f\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"The succinate-ubiquinone oxidoreductase (SQR) complex connects two of the cell's most vital energy-producing metabolic processes: the tricarboxylic acid cycle and the electron transport chain. Hence, the SQR complex is essential in cell metabolism, and its malfunction leads to the progression of multiple metabolic disorders and other diseases, such as cancer. In the current study, we calculated the electron tunneling (ET) pathways between the different redox systems in the SQR complex, including the SQR ligands and the distant heme b redox center, using the broken-symmetry semi-empirical ZINDO method. Interestingly, we discovered a water channel running from the mitochondrial matrix, filling the space between Fe3S4 and heme b redox centers. To investigate the physiological function of the water channel, we performed extensive MD simulations of membrane-embedded SQR complex in small and large water boxes, representing regular (MDA) and extended (MDB) volume states, respectively. We found that under regular volume conditions (MDA), the ET reaction is conducted through both the iron-sulfur cluster chain (i.e., pathway A) and through heme b (i.e., pathway B). Hence, the SQR complex encompasses an internal interferometer similar to the Mach-Zender interferometer, such that tunneling electron experiences a self-interference effect through pathways A and B, enhancing the SQR complex's overall ET thermodynamics and favoring the forward ET direction of oxidizing succinate to fumarate and reducing ubiquinone to ubiquinol. On the other hand, we found that under extended volume conditions (MDB), the internal water channel of the SQR complex \\\"senses\\\" the expansion in the mitochondrial volume, pushing the heme b and Fe4S3 redox centers apart and hence lowering the SQR equilibrium constant to almost unity. 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引用次数: 0
摘要
琥珀酸-泛醌氧化还原酶(SQR)复合体连接着细胞中两个最重要的能量代谢过程:三羧酸循环和电子传递链。因此,SQR 复合物在细胞代谢中至关重要,其功能失常会导致多种代谢紊乱和癌症等其他疾病的发展。在目前的研究中,我们利用破对称半经验 ZINDO 方法计算了 SQR 复合物中不同氧化还原系统(包括 SQR 配体和远处的血红素 b 氧化还原中心)之间的电子隧道(ET)通路。有趣的是,我们发现了一条从线粒体基质流出的水通道,填充了 Fe3S4 和血红素 b 氧化还原中心之间的空间。为了研究水通道的生理功能,我们在小水盒和大水盒(分别代表常规体积状态(MDA)和扩展体积状态(MDB))中对膜包埋 SQR 复合物进行了大量 MD 模拟。我们发现,在常规体积条件(MDA)下,ET 反应通过铁硫簇链(即途径 A)和血红素 b(即途径 B)进行。因此,SQR 复合物包含一个类似于马赫-曾德干涉仪的内部干涉仪,这样,隧道电子通过途径 A 和途径 B 时会产生自干涉效应,从而增强 SQR 复合物的整体 ET 热力学,并有利于将琥珀酸氧化成富马酸并将泛醌还原成泛醇的正向 ET 方向。另一方面,我们发现在扩展容积条件(MDB)下,SQR 复合物的内部水通道会 "感知 "线粒体容积的扩大,将血红素 b 和 Fe4S3 氧化还原中心推开,从而将 SQR 平衡常数降至几乎为一。因此,SQR 复合物可能被驱动反向工作,催化产生呼吸复合物 I 和 III 生理功能所必需的泛醌分子,并恢复线粒体内膜电位,从而恢复 H-K 反孔器的功能,从基质中向外泵送 K+,恢复线粒体的正常体积。
Respiratory Complex II Acting as a Homeostatic Regulatory Sensor
The succinate-ubiquinone oxidoreductase (SQR) complex connects two of the cell's most vital energy-producing metabolic processes: the tricarboxylic acid cycle and the electron transport chain. Hence, the SQR complex is essential in cell metabolism, and its malfunction leads to the progression of multiple metabolic disorders and other diseases, such as cancer. In the current study, we calculated the electron tunneling (ET) pathways between the different redox systems in the SQR complex, including the SQR ligands and the distant heme b redox center, using the broken-symmetry semi-empirical ZINDO method. Interestingly, we discovered a water channel running from the mitochondrial matrix, filling the space between Fe3S4 and heme b redox centers. To investigate the physiological function of the water channel, we performed extensive MD simulations of membrane-embedded SQR complex in small and large water boxes, representing regular (MDA) and extended (MDB) volume states, respectively. We found that under regular volume conditions (MDA), the ET reaction is conducted through both the iron-sulfur cluster chain (i.e., pathway A) and through heme b (i.e., pathway B). Hence, the SQR complex encompasses an internal interferometer similar to the Mach-Zender interferometer, such that tunneling electron experiences a self-interference effect through pathways A and B, enhancing the SQR complex's overall ET thermodynamics and favoring the forward ET direction of oxidizing succinate to fumarate and reducing ubiquinone to ubiquinol. On the other hand, we found that under extended volume conditions (MDB), the internal water channel of the SQR complex "senses" the expansion in the mitochondrial volume, pushing the heme b and Fe4S3 redox centers apart and hence lowering the SQR equilibrium constant to almost unity. Therefore, the SQR complex could be driven to work in the reverse direction, catalyzing the production of ubiquinone molecules essential for the physiological function of respiratory complexes I and III and restoring the inner-mitochondrial membrane potential, which leads to restoring the function of the H-K anti-porter, pumping K+ outward from the matrix and restoring the regular mitochondrial volume.
期刊介绍:
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