Your search keyword '"Leon, Leonardo J."' showing total 4 results

1. Staying young at heart: autophagy and adaptation to cardiac aging.

Author

Leon, Leonardo J. and Gustafsson, Åsa B.

Subjects

*AUTOPHAGY, *BIOLOGICAL adaptation, *CARDIOVASCULAR diseases risk factors, *HOMEOSTASIS, *ORGANELLES, HEART aging

Abstract

Aging is a predominant risk factor for developing cardiovascular disease. Therefore, the cellular processes that contribute to aging are attractive targets for therapeutic interventions that can delay or prevent the development of age-related diseases. Our understanding of the underlying mechanisms that contribute to the decline in cell and tissue functions with age has greatly advanced over the past decade. Classical hallmarks of aging cells include increased levels of reactive oxygen species, DNA damage, accumulation of dysfunctional organelles, oxidized proteins and lipids. These all contribute to a progressive decline in the normal physiological function of the cell and to the onset of age-related conditions. A major cause of the aging process is progressive loss of cellular quality control. Autophagy is an important quality control pathway and is necessary to maintain cardiac homeostasis and to adapt to stress. A reduction in autophagy has been observed in a number of aging models and there is compelling evidence that enhanced autophagy delays aging and extends life span. Enhancing autophagy counteracts age-associated accumulation of protein aggregates and damaged organelles in cells. In this review, we discuss the functional role of autophagy in maintaining homeostasis in the heart, and how a decline is associated with accelerated cardiac aging. We also evaluate therapeutic approaches being researched in an effort to maintain a healthy young heart. [ABSTRACT FROM AUTHOR]

Published

2016

2. Apolipophorin III: Lipopolysaccharide binding requires helix bundle opening

Author

Leon, Leonardo J., Idangodage, Hasitha, Wan, Chung-Ping L., and Weers, Paul M.M.

Subjects

*ENDOTOXINS, *NATURAL immunity, *BACTERIAL cell walls, *IMMUNE response, *GENETIC mutation

Abstract

Abstract: Apolipophorin III (apoLp-III) is a prototypical apolipoprotein used for structure–function studies. Besides its crucial role in lipid transport, apoLp-III is able to associate with fungal and bacterial membranes and stimulate cellular immune responses. We recently demonstrated binding interaction of apoLp-III of the greater wax moth, Galleria mellonella, with lipopolysaccharides (LPS). In the present study, the requirement of helix bundle opening for LPS binding interaction was investigated. Using site-directed mutagenesis, two cysteine residues were introduced in close spatial proximity (P5C/A135C). When the helix bundle was locked by disulfide bond formation, the tethered helix bundle failed to associate with LPS. In contrast, the mutant protein regained its ability to bind upon reduction with dithiothreitol. Thus, helix bundle opening is a critical event in apoLp-III binding interaction with LPS. This mechanism implies that the hydrophobic interior of the protein interacts directly with LPS, analogous to that observed for lipid interaction. [Copyright &y& Elsevier]

Published

2006

3. Tyrosine fluorescence analysis of apolipophorin III–lipopolysaccharide interaction

Author

Leon, Leonardo J., Pratt, Cindy C., Vasquez, Lesley J., and Weers, Paul M.M.

Subjects

*TYROSINE, *AMINO acids, *GEL electrophoresis, *POLYACRYLAMIDE

Abstract

Abstract: Apolipophorin III (apoLp-III) is an exchangeable apolipoprotein that binds to lipopolysaccharides (LPS). Polyacrylamide gel electrophoresis analysis demonstrated that apoLp-III from Galleria mellonella associated with various truncated LPS variants, including lipid A. Subsequent binding studies were performed employing the intrinsic tyrosine fluorescence properties of apoLp-III, which is highly quenched in the unbound state. A marked increase in tyrosine fluorescence intensity was observed upon binding to LPS or detoxified LPS, indicating a new microenvironment for Tyr-142. This also implies that the LPS carbohydrate region is involved in LPS binding. Dissociation constants (K d) measured by apoLp-III titration were estimated at ∼1μM. Increasing the ionic strength did not decrease the K d, neither did LPS phosphate removal. In addition, truncation apoLp-III mutants, lacking two complete helices, were still able to associate with LPS. This indicates that the association of apoLp-III with LPS may not be governed by charge but by hydrophobic interactions. [Copyright &y& Elsevier]

Published

2006

4. Mcl-1-mediated mitochondrial fission protects against stress but impairs cardiac adaptation to exercise.

Author

Moyzis, Alexandra G., Lally, Navraj S., Liang, Wenjing, Leon, Leonardo J., Najor, Rita H., Orogo, Amabel M., and Gustafsson, Åsa B.

Subjects

*DRUG resistance in cancer cells, *MITOCHONDRIAL membranes, *HEART diseases, *BCL-2 proteins, *CELL death

Abstract

Myeloid cell leukemia-1 (Mcl-1) is a structurally and functionally unique anti-apoptotic Bcl-2 protein. While elevated levels of Mcl-1 contribute to tumor cell survival and drug resistance, loss of Mcl-1 in cardiac myocytes leads to rapid mitochondrial dysfunction and heart failure development. Although Mcl-1 is an anti-apoptotic protein, previous studies indicate that its functions extend beyond regulating apoptosis. Mcl-1 is localized to both the mitochondrial outer membrane and matrix. Here, we have identified that Mcl-1 in the outer mitochondrial membrane mediates mitochondrial fission, which is independent of its anti-apoptotic function. We demonstrate that Mcl-1 interacts with Drp1 to promote mitochondrial fission in response to various challenges known to perturb mitochondria morphology. Induction of fission by Mcl-1 reduces nutrient deprivation-induced cell death and the protection is independent of its BH3 domain. Finally, cardiac-specific overexpression of Mcl-1 OM , but not Mcl-1 Matrix , contributes to a shift in the balance towards fission and leads to reduced exercise capacity, suggesting that a pre-existing fragmented mitochondrial network leads to decreased ability to adapt to an acute increase in workload and energy demand. Overall, these findings highlight the importance of Mcl-1 in maintaining mitochondrial health in cells. Unlabelled Image • Mcl-1 interacts with Drp1 to promote mitochondrial fission during stress. • Drp1-mediated fission is independent of Mcl-1's traditional anti-apoptotic function. • Overexpression of Mcl-1 OM in heart leads to a shift in the balance towards fission. • Pre-existing fragmented mitochondria are associated with reduced exercise capacity. • Our findings highlight the importance of Mcl-1 in maintaining mitochondrial health. [ABSTRACT FROM AUTHOR]

Published

2020