Your search keyword '"YA-JING PENG"' showing total 15 results

1. The molecular basis of the genesis of basal tone in internal anal sphincter

Author

Cheng-Hai Zhang, Pei Wang, Dong-Hai Liu, Cai-Ping Chen, Wei Zhao, Xin Chen, Chen Chen, Wei-Qi He, Yan-Ning Qiao, Tao Tao, Jie Sun, Ya-Jing Peng, Ping Lu, Kaizhi Zheng, Siobhan M. Craige, Lawrence M. Lifshitz, John F. Keaney Jr, Kevin E. Fogarty, Ronghua ZhuGe, and Min-Sheng Zhu

Subjects

Science

Abstract

The molecular basis of the basal tone generated by internal anal sphincters (IAS) is largely unknown. Here, the authors show that the tone arises from a global rise in intracellular Ca2+ in smooth muscle cells via a Ryanodine receptor-TMEM16A-L-type Ca2+channel-MLC kinase pathway, suggesting a potential therapy for IAS motility disorders.

Published

2016

2. Myosin light-chain kinase is necessary for membrane homeostasis in cochlear inner hair cells.

Author

Guang-Jie Zhu, Fang Wang, Chen Chen, Lin Xu, Wen-Cheng Zhang, Chi Fan, Ya-Jing Peng, Jie Chen, Wei-Qi He, Shi-Ying Guo, Jian Zuo, Xia Gao, and Min-Sheng Zhu

Subjects

Medicine, Science

Abstract

The structural homeostasis of the cochlear hair cell membrane is critical for all aspects of sensory transduction, but the regulation of its maintenance is not well understood. In this report, we analyzed the cochlear hair cells of mice with specific deletion of myosin light chain kinase (MLCK) in inner hair cells. MLCK-deficient mice showed impaired hearing, with a 5- to 14-dB rise in the auditory brainstem response (ABR) thresholds to clicks and tones of different frequencies and a significant decrease in the amplitude of the ABR waves. The mutant inner hair cells produced several ball-like structures around the hair bundles in vivo, indicating impaired membrane stability. Inner hair cells isolated from the knockout mice consistently displayed less resistance to hypoosmotic solution and less membrane F-actin. Myosin light-chain phosphorylation was also reduced in the mutated inner hair cells. Our results suggest that MLCK is necessary for maintaining the membrane stability of inner hair cells.

Published

2012

3. Excited-state intramolecular proton transfer with and without the assistance of vibronic-transition-induced skeletal deformation in phenol–quinoline

Author

Ya-Jing Peng, Sheng Hsien Lin, Shi-Bo Yu, Chaoyuan Zhu, Yu-Hui Liu, and Chen-Wen Wang

Subjects

Materials science, Proton, Hydrogen bond, General Chemical Engineering, Intramolecular force, Potential energy surface, Vibronic spectroscopy, Molecule, Density functional theory, General Chemistry, Photochemistry, Excitation

Abstract

The excited-state intramolecular proton transfer (ESIPT) reaction of two phenol-quinoline molecules (namely PQ-1 and PQ-2) were investigated using time-dependent density functional theory. The five-(six-) membered-ring carbocycle between the phenol and quinolone moieties in PQ-1 (PQ-2) actually causes a relatively loose (tight) hydrogen bond, which results in a small-barrier (barrier-less) on an excited-state potential energy surface with a slow (fast) ESIPT process with (without) involving the skeletal deformation motion up to the electronic excitation. The skeletal deformation motion that is induced from the largest vibronic excitation with low frequency can assist in decreasing the donor-acceptor distance and lowering the reaction barrier in the excited-state potential energy surface, and thus effectively enhance the ESIPT reaction for PQ-1. The Franck-Condon simulation indicated that the low-frequency mode with vibronic excitation 0 → 1' is an original source of the skeletal deformation vibration. The present simulation presents physical insights for phenol-quinoline molecules in which relatively tight or loose hydrogen bonds can influence the ESIPT reaction process with and without the assistance of the skeletal deformation motion.

Published

2021

4. The absorption and fluorescence spectra of 4-(3-methoxybenzylidene)-2-methyl-oxazalone interpreted by Franck–Condon simulation in various pH solvent environments

Author

Hang Su, Chaoyuan Zhu, Sheng Hsien Lin, Yu-Hui Liu, and Ya-Jing Peng

Subjects

Solvent, Chemistry, Excited state, Analytical chemistry, Cationic polymerization, General Physics and Astronomy, Molecule, Emission spectrum, Time-dependent density functional theory, Physical and Theoretical Chemistry, Absorption (chemistry), Fluorescence

Abstract

The absorption and fluorescence spectra of 4-(3-methoxybenzylidene)-2-methyl-oxazalone (m-MeOBDI) dissolved in neutral, acidic, and basic solvent environments have been investigated and assigned by using Franck–Condon (FC) simulations at the quantum TDDFT level. Four different structures of m-MeOBDI in the ground and excited states are optimized and are found to be responsible for the observed absorption and fluorescence spectra. The (absorption) fluorescence of m-MeOBDI in pure methanol and neutral/basic methanol/water (1/9 vol) mixed solvent is found to arise from the (ground neutral N-I) excited neutral N-I* and cationic C-III* species, respectively. In acidic solvent, the absorption is found to arise from ground acidic C-II species, and the excited divalent cation DC-IV* is found to be formed in its excited state due to the excess H+ in the solution, and then it emits ∼560 nm fluorescence. FC simulations have also been employed to confirm our assignments as well as interpret the vibronic band profiles. As expected, the simulated emission spectrum of the divalent cationic species is in good agreement with the experimental observation. Therefore, within the present FC simulation, the observed absorption and fluorescence spectra have been reasonably interpreted and novel fluorescence mechanisms of m-MeOBDI in various pH solvent environments have been proposed.

Published

2020

5. Deletion of myosin light chain kinase in endothelial cells has a minor effect on the lipopolysaccharide-induced increase in microvascular endothelium permeability in mice

Author

Yang, Yu, Ning, Lv, Zheng, Lu, Yan-Yan, Zheng, Wen-Cheng, Zhang, Chen, Chen, Ya-Jing, Peng, Wei-Qi, He, Fan-Qing, Meng, Min-Sheng, Zhu, and Hua-Qun, Chen

Subjects

Inflammation, Lipopolysaccharides, Male, Mice, Knockout, Integrases, Receptor Protein-Tyrosine Kinases, Mice, Transgenic, Eye, Receptor, TIE-2, Capillary Permeability, Mice, Inbred C57BL, Survival Rate, Mice, Esophagus, Animals, Female, Endothelium, Vascular, Myosin-Light-Chain Kinase

Abstract

There is a current view that myosin light chain kinase (MLCK) plays a critical role in endothelial permeability. To investigate the functions of MLCK in endothelial cells in vivo, we generated a mouse model in which MLCK was selectively deleted by crossing Mylk1 floxed mice with Tie2/cre transgenic mice. Knocking out Mylk1 from endothelial cells had no effect on the global phenotype of the mice, including body weight and blood pressure. Lipopolysaccharide (LPS)-mediated septic death was also not altered in the knockout (KO) mice. Consistently, LPS-induced inflammatory injury and the increase in microvascular permeability in the main organs, including the lung and the kidney, was not significantly attenuated in KO mice as compared with wild-type mice. However, the LPS-induced microvascular hyperpermeability of the esophagus and the eyeballs was attenuated in KO mice. We also found that the LPS-mediated increase in the number of caveolae in the endothelial cells of the esophagus was significantly reduced in KO mice. Our results do not support a role for endothelial cell MLCK in the pathogenesis of inflammatory diseases.

Published

2012

6. Quantum interference effect in electron tunneling through a quantum-dot-ring spin valve

Author

Jia Zhao, Kai-Cheng Zhang, Feng Chi, Ya-Jing Peng, and Jing-Min Ma

Subjects

Physics, Condensed matter physics, Spin polarization, Magnetic moment, Nano Idea, Spin valve, Coulomb blockade, General Medicine, Condensed Matter Physics, Condensed Matter::Mesoscopic Systems and Quantum Hall Effect, Magnetization, Tunnel magnetoresistance, Materials Science(all), lcsh:TA401-492, lcsh:Materials of engineering and construction. Mechanics of materials, Direct coupling, Quantum tunnelling

Abstract

Spin-dependent transport through a quantum-dot (QD) ring coupled to ferromagnetic leads with noncollinear magnetizations is studied theoretically. Tunneling current, current spin polarization and tunnel magnetoresistance (TMR) as functions of the bias voltage and the direct coupling strength between the two leads are analyzed by the nonequilibrium Green's function technique. It is shown that the magnitudes of these quantities are sensitive to the relative angle between the leads' magnetic moments and the quantum interference effect originated from the inter-lead coupling. We pay particular attention on the Coulomb blockade regime and find the relative current magnitudes of different magnetization angles can be reversed by tuning the inter-lead coupling strength, resulting in sign change of the TMR. For large enough inter-lead coupling strength, the current spin polarizations for parallel and antiparallel magnetic configurations will approach to unit and zero, respectively.PACS numbers

Published

2011

7. Identification and functional characterization of an aggregation domain in long myosin light chain kinase

Author

Wen-Cheng, Zhang, Ya-Jing, Peng, Wei-Qi, He, Ning, Lv, Chen, Chen, Gang, Zhi, Hua-Qun, Chen, and Min-Sheng, Zhu

Subjects

Male, Recombinant Fusion Proteins, Diaphragm, Molecular Sequence Data, Myosin Subfragments, Mice, Transgenic, Cell Line, Mitochondria, Protein Structure, Tertiary, Mice, Sequence Analysis, Protein, Muscle Fatigue, Animals, Humans, Female, Amino Acid Sequence, Chickens, Myosin-Light-Chain Kinase, Muscle Contraction

Abstract

The functions of long smooth muscle myosin light chain kinase (L-MLCK), a molecule with multiple domains, are poorly understood. To examine the existence of further potentially functional domains in this molecule, we analyzed its amino acid sequence with a tango program and found a putative aggregation domain located at the 4Ig domain of the N-terminal extension. To verify its aggregation capability in vitro, expressible truncated L-MLCK variants driven by a cytomegalovirus promoter were transfected into cells. As anticipated, only the overexpression of the 4Ig fragment led to particle formation in Colon26 cells. These particles contained 4Ig polymers and actin. Analysis with detergents demonstrated that the particles shared features in common with aggregates. Thus, we conclude that the 4Ig domain has a potent aggregation ability. To further examine this aggregation domain in vivo, eight transgenic mouse lines expressing the 4Ig domain (4Ig lines) were generated. The results showed that the transgenic mice had typical aggregation in the thigh and diaphragm muscles. Histological examination showed that 7.70 +/- 1.86% of extensor digitorum longus myofibrils displayed aggregates with a 36.44% reduction in myofibril diameter, whereas 65.13 +/- 3.42% of diaphragm myofibrils displayed aggregates and the myofibril diameter was reduced by 43.08%. Electron microscopy examination suggested that the aggregates were deposited at the mitochondria, resulting in structural impairment. As a consequence, the oxygen consumption of mitochondria in the affected muscles was also reduced. Macrophenotypic analysis showed the presence of muscular degeneration characterized by a reduction in force development, faster fatigue, decreased myofibril diameters, and structural alterations. In summary, our study revealed the existence of a novel aggregation domain in L-MLCK and provided a direct link between L-MLCK and aggregation. The possible significance and mechanism underlying the aggregation-based pathological processes mediated by L-MLCK are also discussed.

Published

2008

8. Ultrafast multiplex CARS investigation of vibrational characteristics in chloroform and PMMA

Author

Ying-Hui, Wang, primary, Ya-Jing, Peng, additional, Xing, He, additional, Yun-Fei, Song, additional, and Yan-Qiang, Yang, additional

Published

2009

9. Theoretical investigation on near-infrared and visible absorption spectra of nanometallic aluminium with oxide coating in nanoenergetic materials: size and shape effects

Author

Ya-Jing, Peng, primary, Shu-Ping, Zhang, additional, Ying-Hui, Wang, additional, and Yan-Qiang, Yang, additional

Published

2008

10. Analysis on the mechanism of photoluminescence quenching in π-conjugated polymers in photo-oxidation process with broadband transient grating

Author

Yue-qi Mo, Ya-jing Peng, Xian-xu Zheng, Yinghui Wang, and Yanqiang Yang

Subjects

chemistry.chemical_classification, Organic semiconductor, Photoluminescence, Materials science, Physics and Astronomy (miscellaneous), chemistry, Energy level, Polymer, Transient (oscillation), Conjugated system, Grating, Photochemistry, Luminescence

Abstract

Photoinduced oxidation process of poly[2-methoxy-5-(2′-ethyl-hexyloxy)-1,4-phenylene vinylene] is probed by using broadband transient grating technique. The results suggest that the damage of bonds in the side and main chains leads to the line shape variation and efficiency decreasing of luminescence in photoluminescence quenching, and their temporal evolution and damage rates are found to vary with molecular energy states.

Published

2008

11. Altered Contractile Phenotypes of Intestinal Smooth Muscle in Mice Deficient in Myosin Phosphatase Target Subunit 1.

Author

WEI-QI HE, YAN-NING QIAO, YA-JING PENG, JUAN-MIN ZHA, CHENG-HAI ZHANG, CHEN CHEN, CAI-PING CHEN, PEI WANG, XIAO YANG, CHAO-JUN LI, KAMM, KRISTINE E., STULL, JAMES T., and MIN-SHENG ZHU

Abstract

BACKGROUND & AIMS: The regulatory subunit of myosin light chain phosphatase, MYPT1, has been proposed to control smooth muscle contractility by regulating phosphorylation of the Ca2+-dependent myosin regulatory light chain. We generated mice with a smooth muscle-specific deletion of MYPT1 to investigate its physiologic role in intestinal smooth muscle contraction. METHODS: We used the CreloxP system to establish Mypt1-floxed mice, with the promoter region and exon 1 of Myptl flanked by 2 loxP sites. These mice were crossed with SMA-Cre transgenic mice to generate mice with smooth muscle-specific deletion of MYPT1 (Mypt1SMKO mice). The phenotype was assessed by histologic, biochemical, molecular, and physiologic analyses. RESULTS: Young adult Mypt1SMKO mice had normal intestinal motility in vivo, with no histologic abnormalities. On stimulation with KC1 or acetylcholine, intestinal smooth muscles isolated from Mypt1SMKO mice produced robust and increased sustained force due to increased phosphorylation of the myosin regulatory light chain compared with muscle from control mice. Additional analyses of contractile properties showed reduced rates of force development and relaxation, and decreased shortening velocity, compared with muscle from control mice. Permeable smooth muscle fibers from Mypt1SMKO mice had increased sensitivity and contraction in response to Ca2+. Ca2+. CONCLUSIONS: MYPT1 is not essential for smooth muscle function in mice but regulates the Ca2+ sensitivity of force development and contributes to intestinal phasic contractile phenotype. Altered contractile responses in isolated tissues could be compensated by adaptive physiologic responses in vivo, where gut motility is affected by lower intensifies of smooth muscle stimulation for myosin phosphorylation and force development. [ABSTRACT FROM AUTHOR]

Published

2013

12. Role of myosin light chain kinase in regulation of basal blood pressure and maintenance of salt-induced hypertensiion.

Author

Wei-Qi He, Yan-Ning Qiao, Cheng-Hai Zhang, Ya-Jing Peng, Chen Chen, Pei Wang, Yun-Qian Gao, Caiping Chen, Xin Chen, Tao Tao, Xiao-Hong Su, Chao-Jun Li, Kamm, Kristine E., James T. Stull, and Min-Sheng Zhu

Subjects

MYOSIN, BLOOD pressure, VASCULAR smooth muscle, PHOSPHORYLATION, MICE, VASOCONSTRICTORS

Abstract

Vascular tone, an important determinant of systemic vascular resistance and thus blood pressure, is affected by vascular smooth muscle (VSM) contraction. Key signaling pathways for VSM contraction converge on phosphorylation of the regulatory light chain (RLC) of smooth muscle myosin. This phosphorylation is mediated by Ca2+/calmodulin-dependent myosin light chain kinase (MLCK) but Ca2+-independent kinases may also contribute, particularly in sustained contractions. Signaling through MLCK has been indirectly implicated in maintenance of basal blood pressure, whereas signaling through RhoA has been implicated in salt-induced hypertension. In this report, we analyzed mice with smooth muscle-specific knockout of MLCK. Mesenteric artery segments isolated from smooth muscle-specific MLCK knockout mice (MLCKSMKO) had a significantly reduced contractile response to KCl and vasoconstrictors. The kinase knockout also markedly reduced RLC phosphorylation and developed force. We suggest that MLCK and its phosphorylation of RLC are required for tonic VSM contraction. MLCKSMKO mice exhibit significantly lower basal blood pressure and weaker responses to vasopressors. The elevated blood pressure in salt-induced hypertension is reduced below normotensive levels after MLCK attenuation. These results suggest that MLCK is necessary for both physiological and pathological blood pressure. MLCKSMKO mice may be a useful model of vascular failure and hypotension. [ABSTRACT FROM AUTHOR]

Published

2011

13. Trio Is a Key Guanine Nucleotide Exchange Factor Coordinating Regulation of the Migration and Morphogenesis of Granule Cells in the Developing Cerebellum.

Author

Ya-Jing Peng, Wei-Qi He, Jing Tang, Tao Tao, Chen Chen, Yun-Qian Gao, Wen-Cheng Zhang, Xue-Yan He, Yu-Yuan Dai, Nian-Chun Zhu, Ning Lv, Cheng-Hai Zhang, Yan-Ning Qiao, Li-Ping Zhao, Xiang Gao, and Min-Sheng Zhu

Subjects

*G proteins, *NEURONS, *CELLS, *CEREBELLUM, *CYTOSKELETON, *GUANOSINE triphosphatase

Abstract

Orchestrated regulation of neuronal migration and morphogenesis is critical for neuronal development and establishment of functional circuits, but its regulatory mechanism is incompletely defined. We established and analyzed mice with neural-specific knock-out of Trio, a guanine nucleotide exchange factor with multiple guanine nucleotide exchange factor domains. Knock-out mice showed defective cerebella and severe signs ataxia. Mutant cerebella had no granule cells in the internal granule cell layer due to aberrant granule cell migration as well as abnormal neurite growth. Trio-deficient granule cells showed reduced extension of neurites and highly branched and misguided processes with perturbed stabilization of actin microtubules. Trio deletion caused down-regulation of the activation of Rac1, RhoA, and Cdc42, and mutant granule appeared to be unresponsive to neurite growth-promoting molecules such as Netrin-1 and Semaphorin 6A. These results suggest that Trio may be a key signal module for the orchestrated regulation of neuronal migration and morphogenesis during cerebellar development. Trio may serve as a signal integrator decoding extrinsic signals to Rho GTPases for cytoskeleton organization. [ABSTRACT FROM AUTHOR]

Published

2010

14. Myosin Light Chain Kinase Is Necessary for Tonic Airway Smooth Muscle Contraction.

Author

Wen-Cheng Zhang, Ya-Jing Peng, Gen-Sheng Zhang, Wei-Qi He, Yan-Ning Qiao, Ying-Ying Dong, Yun-Qian Gao, Chen Chen, Cheng-Hai Zhang, Wen Li, Hua-Hao Shen, Wen Ning, Kamm, Kristine E., Stull, James T., Xiang Gao, and Min-Sheng Zhu

Subjects

*MYOSIN, *CALMODULIN, *PHOSPHORYLATION, *MUSCLE contraction, *LABORATORY mice

Abstract

Different interacting signaling modules involving Ca2+/calmodulin-dependent myosin light chain kinase, Ca2+-independent regulatory light chain phosphorylation, myosin phosphatase inhibition, and actin filament-based proteins are proposed as specific cellular mechanisms involved in the regulation of smooth muscle contraction. However, the relative importance of specific modules is not well defined. By using tamoxifen-activated and smooth muscle-specific knock-out of myosin light chain kinase in mice, we analyzed its role in tonic airway smooth muscle contraction. Knock-out of the kinase in both tracheal and bronchial smooth muscle significantly reduced contraction and myosin phosphorylation responses to K+-depolarization and acetylcholine. Kinase-deficient mice lacked bronchial constrictions in normal and asthmatic airways, whereas the asthmatic inflammation response was not affected. These results indicate that myosin light chain kinase acts as a central participant in the contractile signaling module of tonic smooth muscle. Importantly, contractile airway smooth muscles are necessary for physiological and asthmatic airway resistance. [ABSTRACT FROM AUTHOR]

Published

2010

15. Myosin Phosphatase Target Subunit 1 (MYPT1) Regulates the Contraction and Relaxation of Vascular Smooth Muscle and Maintains Blood Pressure.

Author

Yan-Ning Qiao, Wei-Qi He, Cai-Ping Chen, Cheng-Hai Zhang, Wei Zhao, Pei Wang, Lin Zhang, Yan-Ze Wu, Xiao Yang, Ya-Jing Peng, Ji-Min Gao, Kamm, Kristine E., Stull, James T., and Min-Sheng Zhu

Subjects

*MYOSIN, *SMOOTH muscle proteins, *BLOOD pressure, *PROTEIN kinase C, *NORADRENALINE, *PHOSPHORYLATION

Abstract

Myosin light chain phosphatase with its regulatory subunit, myosin phosphatase target subunit 1 (MYPT1) modulates Ca2+- dependent phosphorylation of myosin light chain by myosin light chain kinase, which is essential for smooth muscle contraction. The role of MYPT1 in vascular smooth muscle was investigated in adultMYPT1smooth muscle specific knock-out mice. MYPT1 deletion enhanced phosphorylation of myosin regulatory light chain and contractile force in isolated mesenteric arteries treated with KCl and various vascular agonists. The contractile responses of arteries from knock-out mice to norepinephrine were inhibited by Rho-associated kinase (ROCK) and protein kinase C inhibitors and were associated with inhibition of phosphorylation of the myosin light chain phosphatase inhibitor CPI-17. Additionally, stimulation of the NO/cGMP/protein kinase G (PKG) signaling pathway still resulted in relaxation of MYPT1-deficient mesenteric arteries, indicating phosphorylation of MYPT1 by PKG is not a major contributor to the relaxation response. Thus, MYPT1 enhances myosin light chain phosphatase activity sufficient for blood pressure maintenance. Rho-associated kinase phosphorylation of CPI-17 plays a significant role in enhancing vascular contractile responses, whereas phosphorylation of MYPT1 in the NO/cGMP/PKG signaling module is not necessary for relaxation. [ABSTRACT FROM AUTHOR]

Published

2014