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1. CHCHD4-TRIAP1 regulation of innate immune signaling mediates skeletal muscle adaptation to exercise

Author

Jin Ma, Ping-yuan Wang, Jie Zhuang, Annie Y. Son, Alexander K. Karius, Abu Mohammad Syed, Masahiro Nishi, Zhichao Wu, Mateus P. Mori, Young-Chae Kim, and Paul M. Hwang

Subjects
CP: Immunology, Biology (General), QH301-705.5
Abstract

Summary: Exercise training can stimulate the formation of fatty-acid-oxidizing slow-twitch skeletal muscle fibers, which are inversely correlated with obesity, but the molecular mechanism underlying this transformation requires further elucidation. Here, we report that the downregulation of the mitochondrial disulfide relay carrier CHCHD4 by exercise training decreases the import of TP53-regulated inhibitor of apoptosis 1 (TRIAP1) into mitochondria, which can reduce cardiolipin levels and promote VDAC oligomerization in skeletal muscle. VDAC oligomerization, known to facilitate mtDNA release, can activate cGAS-STING/NFKB innate immune signaling and downregulate MyoD in skeletal muscle, thereby promoting the formation of oxidative slow-twitch fibers. In mice, CHCHD4 haploinsufficiency is sufficient to activate this pathway, leading to increased oxidative muscle fibers and decreased fat accumulation with aging. The identification of a specific mediator regulating muscle fiber transformation provides an opportunity to understand further the molecular underpinnings of complex metabolic conditions such as obesity and could have therapeutic implications.

Published
2024
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2. Protective role of p53 in doxorubicin-induced cardiomyopathy as a mitochondrial disease

Author

Masahiro Nishi, Ping-Yuan Wang, and Paul M. Hwang

Subjects
doxorubicin, cardiomyopathy, p53, mitochondria, mtdna, tfam, p53r2, nad+, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Abstract

Doxorubicin is widely used against cancer but carries the risk of a progressive cardiomyopathy associated with mitochondrial loss. Using genetic models, our recent study demonstrates that mitochondrial genomic DNA regulation by tumor protein p53 (TP53, best known as p53) prevents the cardiotoxicity of low dose doxorubicin which does not activate the p53-dependent cell death pathway.

Published
2020
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3. A Mouse Homolog of a Human TP53 Germline Mutation Reveals a Lipolytic Activity of p53

Author

Ju-Gyeong Kang, Cory U. Lago, Ji-Eun Lee, Ji-Hoon Park, Matthew P. Donnelly, Matthew F. Starost, Chengyu Liu, Jaeyul Kwon, Audrey C. Noguchi, Kai Ge, Ping-yuan Wang, and Paul M. Hwang

Subjects
Biology (General), QH301-705.5
Abstract

Summary: The physiological effects of the many germline mutations of TP53, encoding the tumor suppressor protein p53, are poorly understood. Here we report generating a p53 R178C knockin mouse modeling the human TP53 R181C mutation, which is notable for its prevalence and prior molecular characterization. Consistent with its weak cancer penetrance in humans, homozygous p53178C/C mice show a modest increase in tumorigenesis but, surprisingly, are lean with decreased body fat content. They display evidence of increased lipolysis and upregulation of fatty acid metabolism in their inguinal white adipose tissue (iWAT). Gene expression and chromatin immunoprecipitation sequencing (ChIP-seq) analyses show that the mutant p53 bound and transactivated Beta-3-Adrenergic Receptor (ADRB3), a gene that is known to promote lipolysis and is associated with obesity. This study reveals that a germline mutation of p53 can affect fat metabolism, which has been implicated in cancer development. : Knockin of the mouse homolog of a human TP53 germline mutation known to cause Li-Fraumeni syndrome, a cancer predisposition disorder, results in a mouse model characterized by lower body fat content. Kang et al. show that enhancing transactivation of the lipolytic gene ADRB3 by mutant p53 contributes to this phenotype. Keywords: TP53 mutation, Li-Fraumeni syndrome, cancer, mouse model, fat, lipolysis, ADRB3

Published
2020
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5. Li–Fraumeni Syndrome–Associated Dimer-Forming Mutant p53 Promotes Transactivation-Independent Mitochondrial Cell Death

Author

Joshua H. Choe, Tatsuya Kawase, An Xu, Asja Guzman, Aleksandar Z. Obradovic, Ana Maria Low-Calle, Bita Alaghebandan, Ananya Raghavan, Kaitlin Long, Paul M. Hwang, Joshua D. Schiffman, Yan Zhu, Ruiying Zhao, Dung-Fang Lee, Chen Katz, and Carol Prives

Subjects
Oncology
Abstract

Cancer-relevant mutations in the oligomerization domain (OD) of the p53 tumor suppressor protein, unlike those in the DNA binding domain, have not been well elucidated. Here, we characterized the germline OD mutant p53(A347D), which occurs in cancer-prone Li–Fraumeni syndrome (LFS) patients. Unlike wild-type p53, mutant p53(A347D) cannot form tetramers and exists as a hyperstable dimeric protein. Further, p53(A347D) cannot bind or transactivate the majority of canonical p53 target genes. Isogenic cell lines harboring either p53(A347D) or no p53 yield comparable tumorigenic properties, yet p53(A347D) displays remarkable neomorphic activities. Cells bearing p53(A347D) possess a distinct transcriptional profile and undergo metabolic reprogramming. Further, p53(A347D) induces striking mitochondrial network aberration and associates with mitochondria to drive apoptotic cell death upon topoisomerase II inhibition in the absence of transcription. Thus, dimer-forming p53 demonstrates both loss-of-function (LOF) and gain-of-function (GOF) properties compared with the wild-type form of the protein. Significance: A mutant p53 (A347D), which can only form dimers, is associated with increased cancer susceptibility in LFS individuals. We found that this mutant wields a double-edged sword, driving tumorigenesis through LOF while gaining enhanced apoptogenic activity as a new GOF, thereby yielding a potential vulnerability to select therapeutic approaches. See related commentary by Stieg et al., p. 1046. See related article by Gencel-Augusto et al., p. 1230. This article is highlighted in the In This Issue feature, p. 1027

Published
2023

6. Supplementary Figures from Li–Fraumeni Syndrome–Associated Dimer-Forming Mutant p53 Promotes Transactivation-Independent Mitochondrial Cell Death

Author

Carol Prives, Chen Katz, Dung-Fang Lee, Ruiying Zhao, Yan Zhu, Joshua D. Schiffman, Paul M. Hwang, Kaitlin Long, Ananya Raghavan, Bita Alaghebandan, Ana Maria Low-Calle, Aleksandar Z. Obradovic, Asja Guzman, An Xu, Tatsuya Kawase, and Joshua H. Choe

Abstract

Supplementary Figures 1-9 demonstrating the GOF and LOF activities of p53(A347D)

Published
2023

7. Supplementary Data 2 from Li–Fraumeni Syndrome–Associated Dimer-Forming Mutant p53 Promotes Transactivation-Independent Mitochondrial Cell Death

Author

Carol Prives, Chen Katz, Dung-Fang Lee, Ruiying Zhao, Yan Zhu, Joshua D. Schiffman, Paul M. Hwang, Kaitlin Long, Ananya Raghavan, Bita Alaghebandan, Ana Maria Low-Calle, Aleksandar Z. Obradovic, Asja Guzman, An Xu, Tatsuya Kawase, and Joshua H. Choe

Abstract

Differentially expressed genes in U2OS cells varying in p53 allelic status combined from two independent RNA library preparations

Published
2023

9. Supplementary Data 6 from Li–Fraumeni Syndrome–Associated Dimer-Forming Mutant p53 Promotes Transactivation-Independent Mitochondrial Cell Death

Author

Carol Prives, Chen Katz, Dung-Fang Lee, Ruiying Zhao, Yan Zhu, Joshua D. Schiffman, Paul M. Hwang, Kaitlin Long, Ananya Raghavan, Bita Alaghebandan, Ana Maria Low-Calle, Aleksandar Z. Obradovic, Asja Guzman, An Xu, Tatsuya Kawase, and Joshua H. Choe

Abstract

p53 ChIPseq peaks from osteoblasts derived from normal and LFS individuals

Published
2023

11. Data from Li–Fraumeni Syndrome–Associated Dimer-Forming Mutant p53 Promotes Transactivation-Independent Mitochondrial Cell Death

Author

Carol Prives, Chen Katz, Dung-Fang Lee, Ruiying Zhao, Yan Zhu, Joshua D. Schiffman, Paul M. Hwang, Kaitlin Long, Ananya Raghavan, Bita Alaghebandan, Ana Maria Low-Calle, Aleksandar Z. Obradovic, Asja Guzman, An Xu, Tatsuya Kawase, and Joshua H. Choe

Abstract

Cancer-relevant mutations in the oligomerization domain (OD) of the p53 tumor suppressor protein, unlike those in the DNA binding domain, have not been well elucidated. Here, we characterized the germline OD mutant p53(A347D), which occurs in cancer-prone Li–Fraumeni syndrome (LFS) patients. Unlike wild-type p53, mutant p53(A347D) cannot form tetramers and exists as a hyperstable dimeric protein. Further, p53(A347D) cannot bind or transactivate the majority of canonical p53 target genes. Isogenic cell lines harboring either p53(A347D) or no p53 yield comparable tumorigenic properties, yet p53(A347D) displays remarkable neomorphic activities. Cells bearing p53(A347D) possess a distinct transcriptional profile and undergo metabolic reprogramming. Further, p53(A347D) induces striking mitochondrial network aberration and associates with mitochondria to drive apoptotic cell death upon topoisomerase II inhibition in the absence of transcription. Thus, dimer-forming p53 demonstrates both loss-of-function (LOF) and gain-of-function (GOF) properties compared with the wild-type form of the protein.Significance:A mutant p53 (A347D), which can only form dimers, is associated with increased cancer susceptibility in LFS individuals. We found that this mutant wields a double-edged sword, driving tumorigenesis through LOF while gaining enhanced apoptogenic activity as a new GOF, thereby yielding a potential vulnerability to select therapeutic approaches.See related commentary by Stieg et al., p. 1046.See related article by Gencel-Augusto et al., p. 1230.This article is highlighted in the In This Issue feature, p. 1027

Published
2023

12. Supplementary Data 1 from Li–Fraumeni Syndrome–Associated Dimer-Forming Mutant p53 Promotes Transactivation-Independent Mitochondrial Cell Death

Author

Carol Prives, Chen Katz, Dung-Fang Lee, Ruiying Zhao, Yan Zhu, Joshua D. Schiffman, Paul M. Hwang, Kaitlin Long, Ananya Raghavan, Bita Alaghebandan, Ana Maria Low-Calle, Aleksandar Z. Obradovic, Asja Guzman, An Xu, Tatsuya Kawase, and Joshua H. Choe

Abstract

Differentially expressed genes in U2OS cells varying in p53 allelic status

Published
2023

16. Data from Reducing Fatty Acid Oxidation Improves Cancer-free Survival in a Mouse Model of Li-Fraumeni Syndrome

Author

Paul M. Hwang, Ju-Gyeong Kang, Mehdi Pirooznia, Komudi Singh, Michael J. Wolfgang, Matthew F. Starost, Jie Li, Jin Ma, and Ping-Yuan Wang

Abstract

Germline mutations of TP53, which cause the cancer predisposition disorder Li-Fraumeni syndrome (LFS), can increase mitochondrial activity as well as fatty acid β-oxidation (FAO) in mice. Increased fatty acid metabolism can promote cancer malignancy, but its specific contribution to tumorigenesis in LFS remains unclear. To investigate this, we crossed LFS mice carrying the p53 R172H knock-in mutation (p53172H/H, homolog of the human TP53 R175H LFS mutation) with myoglobin-knockout (MB−/−) mice known to have decreased FAO. MB−/− p53172H/H double-mutant mice also showed mildly reduced FAO in thymus, a common site of T lymphoma development in LFS mice, in association with an approximately 40% improvement in cancer-free survival time. RNA sequencing profiling revealed that the p53 R172H mutation promotes mitochondrial metabolism and ribosome biogenesis, both of which are suppressed by the disruption of MB. The activation of ribosomal protein S6, involved in protein translation and implicated in cancer promotion, was also inhibited in the absence of MB. To further confirm the role of FAO in lymphomagenesis, mitochondrial FAO enzyme, carnitine palmitoyltransferase 2 (CPT2), was specifically disrupted in T cells of p53172H/H mice using a Cre-loxP–mediated strategy. The heterozygous knockout of CPT2 resulted in thymus FAO haploinsufficiency and an approximately 30% improvement in survival time, paralleling the antiproliferative signaling observed with MB disruption. Thus, this study demonstrates that moderating FAO in LFS can suppress tumorigenesis and improve cancer-free survival with potential implications for cancer prevention.Prevention Relevance:Mildly inhibiting the increased fatty acid oxidation observed in a mouse model of Li-Fraumeni syndrome, a cancer predisposition disorder caused by inherited mutations of TP53, dampens aberrant pro-tumorigenic cell signaling and improves the survival time of these mice, thereby revealing a potential strategy for cancer prevention in patients.

Published
2023

17. Data from Mouse Homolog of the Human TP53 R337H Mutation Reveals Its Role in Tumorigenesis

Author

Paul M. Hwang, Sharon A. Savage, Ping-yuan Wang, Ju-Gyeong Kang, Maria I. Achatz, Jichun Chen, Jie Zhuang, Chengyu Liu, Matthew F. Starost, Jie Li, and Ji-Hoon Park

Abstract

Inheritance of germline mutations in the tumor suppressor gene TP53 causes Li-Fraumeni syndrome (LFS), a cancer predisposition disorder. The arginine to histidine substitution at amino acid position 337 of p53 (R337H) is a founder mutation highly prevalent in southern and southeastern Brazil and is considered an LFS mutation. Although this mutation is of significant clinical interest, its role in tumorigenesis using animal models has not been described. Here, we generate a knockin mouse model containing the homologous R337H mutation (mouse R334H). De novo tumorigenesis was not significantly increased in either heterozygous (p53334R/H) or homozygous (p53334H/H) p53 R334H knockin mice compared with wild-type mice. However, susceptibility to diethylnitrosamine (DEN)-induced liver carcinogenesis was increased in a mutant allele dose-dependent manner. In parallel, p53334H/H mice exposed to DEN exhibited increased DNA damage but decreased cell-cycle regulation in the liver. Oligomerization of p53, which is required for transactivation of target genes, was reduced in R334H liver, consistent with its decreased nuclear activity compared with wild-type. By modeling a TP53 mutation in mice that has relatively weak cancer penetrance, this study provides in vivo evidence that the human R337H mutation can compromise p53 activity and promote tumorigenesis.Significance: A germline mutation in the oligomerization domain of p53 decreases its transactivation potential and renders mice susceptible to carcinogen-induced liver tumorigenesis. Cancer Res; 78(18); 5375–83. ©2018 AACR.

Published
2023

18. Supplementary Information from Mouse Homolog of the Human TP53 R337H Mutation Reveals Its Role in Tumorigenesis

Author

Paul M. Hwang, Sharon A. Savage, Ping-yuan Wang, Ju-Gyeong Kang, Maria I. Achatz, Jichun Chen, Jie Zhuang, Chengyu Liu, Matthew F. Starost, Jie Li, and Ji-Hoon Park

Abstract

This Supplemental Information file contains the Materials and Methods for the supplementary tables and figures merged into this same file. These are Tables 1-3 which show primer sequences, observed genotypes and gender of p53 R334H mouse crossings, and incidence of adrenal abnormalities; and Figures S1-S9 which provide additional data on mouse phenotype, DEN metabolism, tumor LOH, DNA damage time course, oncogene-induced senescence in MEFs, p53 expression levels, and further oligomerization studies.

Published
2023

19. Abstract LB361: Li-Fraumeni syndrome-associated dimer-forming mutant p53 promotes transactivation-independent mitochondrial cell death

Author

Joshua H. Choe, Tatsuya Kawase, An Xu, Asja Guzman, David R. Tong, Aleksandar Z. Obradovic, Ana M. Low-Calle, Bita Alaghebandan, Ananya Raghavan, Kaitlin Long, Paul M. Hwang, Joshua D. Schiffman, Yan Zhu, Ruiying Zhao, Dung-Fang Lee, Chen Katz, and Carol L. Prives

Subjects
Cancer Research, Oncology
Abstract

Mutations that occur within the oligomerization domain (OD) of the tumor suppressor p53 generally abolish p53 tetramerization and are associated with increased cancer susceptibility in Li-Fraumeni syndrome (LFS). Despite their prevalence, the impact of OD-mutant p53 proteins in cancer, especially beyond a loss of canonical p53 activity, has not been well elucidated. We sought to delineate the gain-of-function (GOF) vs. loss-of-function (LOF) activities of OD-mutant p53, specifically focusing on the LFS tumor-derived p53(A347D) variant. We obtained LFS patient-derived dermal fibroblasts heterozygous for the mutation and generated an allelic series of U2OS cancer cell lines expressing wild-type p53, heterozygous (p53+/AD) or homozygous (p53AD/AD) mutant p53 or no p53 (p53 KO). In contrast to wild-type p53, mutant p53(A347D) exclusively forms dimers in both fibroblasts and cancer cells and has lost the ability to bind and transactivate the majority of canonical p53 target genes, which yields comparable tumorigenic properties between mutant p53 and p53 KO cells. Mutant p53(A347D), however, displays neomorphic activities. Glycolysis and oxidative phosphorylation pathways are enriched in cells bearing p53(A347D) relative to both wild-type p53 and p53 KO cells. Furthermore, dimeric mutant p53 induces striking mitochondrial network aberration and preferentially associates with mitochondria to drive apoptotic cell death upon topoisomerase II inhibition in the absence of transcription. Ultimately, we describe dimeric mutant p53 as wielding a double-edged sword: driving tumorigenesis through LOF while gaining enhanced apoptogenic activity, thereby providing a potential basis for select therapeutic approaches. Citation Format: Joshua H. Choe, Tatsuya Kawase, An Xu, Asja Guzman, David R. Tong, Aleksandar Z. Obradovic, Ana M. Low-Calle, Bita Alaghebandan, Ananya Raghavan, Kaitlin Long, Paul M. Hwang, Joshua D. Schiffman, Yan Zhu, Ruiying Zhao, Dung-Fang Lee, Chen Katz, Carol L. Prives. Li-Fraumeni syndrome-associated dimer-forming mutant p53 promotes transactivation-independent mitochondrial cell death [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2023; Part 2 (Clinical Trials and Late-Breaking Research); 2023 Apr 14-19; Orlando, FL. Philadelphia (PA): AACR; Cancer Res 2023;83(8_Suppl):Abstract nr LB361.

Published
2023

21. Front Cover

Author

Rozhin Penjweini, Branden Roarke, Greg Alspaugh, Katie A. Link, Alessio Andreoni, Mateus P. Mori, Paul M. Hwang, Dan L. Sackett, and Jay R. Knutson

Subjects
General Engineering, General Physics and Astronomy, General Materials Science, General Chemistry, General Biochemistry, Genetics and Molecular Biology
Published
2022

22. A Mouse Homolog of a Human TP53 Germline Mutation Reveals a Lipolytic Activity of p53

Author

Matthew F. Starost, Ju-Gyeong Kang, Ji-Eun Lee, Cory U. Lago, Ping Yuan Wang, Chengyu Liu, Jaeyul Kwon, Kai Ge, Matthew P. Donnelly, Paul M. Hwang, Audrey Noguchi, and Ji-Hoon Park

Subjects
0301 basic medicine, Adipose Tissue, White, Lipolysis, Mutant, White adipose tissue, Biology, medicine.disease_cause, Article, General Biochemistry, Genetics and Molecular Biology, Li-Fraumeni Syndrome, Mice, 03 medical and health sciences, 0302 clinical medicine, Germline mutation, Downregulation and upregulation, 3T3-L1 Cells, Adipocytes, medicine, Animals, Humans, Metabolomics, lcsh:QH301-705.5, Germ-Line Mutation, Principal Component Analysis, Mutation, Base Sequence, Sequence Homology, Amino Acid, Fatty Acids, Homozygote, Penetrance, 3. Good health, Cell biology, Mice, Inbred C57BL, Phenotype, 030104 developmental biology, Gene Expression Regulation, lcsh:Biology (General), Receptors, Adrenergic, beta-3, Tumor Suppressor Protein p53, Carcinogenesis, 030217 neurology & neurosurgery, Signal Transduction
Abstract

SUMMARY The physiological effects of the many germline mutations of TP53, encoding the tumor suppressor protein p53, are poorly understood. Here we report generating a p53 R178C knockin mouse modeling the human TP53 R181C mutation, which is notable for its prevalence and prior molecular characterization. Consistent with its weak cancer penetrance in humans, homozygous p53178C/C mice show a modest increase in tumorigenesis but, surprisingly, are lean with decreased body fat content. They display evidence of increased lipolysis and upregulation of fatty acid metabolism in their inguinal white adipose tissue (iWAT). Gene expression and chromatin immunoprecipitation sequencing (ChIP-seq) analyses show that the mutant p53 bound and trans-activated Beta-3-Adrenergic Receptor (ADRB3), a gene that is known to promote lipolysis and is associated with obesity. This study reveals that a germline mutation of p53 can affect fat metabolism, which has been implicated in cancer development., Graphical Abstract, In Brief Knockin of the mouse homolog of a human TP53 germline mutation known to cause Li-Fraumeni syndrome, a cancer predisposition disorder, results in a mouse model characterized by lower body fat content. Kang et al. show that enhancing transactivation of the lipolytic gene ADRB3 by mutant p53 contributes to this phenotype.

Published
2020

23. Fluorescence lifetime imaging of metMyoglobin formation due to nitric oxide stress

Author

Rozhin Penjweini, Mateus P. Mori, Paul M. Hwang, Dan L. Sackett, and Jay R. Knutson

Subjects
biological sciences, Article
Abstract

Myoglobin is a protein that is expressed quite unevenly among different cell types. Nevertheless, it has been widely acknowledged that the Fe(3+) state of myoglobin, metmyoglobin (metMb) has a broad functional role in metabolism, oxidative/nitrative regulation and gene networks. Accordingly, real-time monitoring of oxygenated, deoxygenated and metMb proportions- or, more broadly, of the mechanisms by which metMb is formed, presents a promising line of research. We had previously introduced a Förster resonance energy transfer (FRET) method to read out the deoxygenation/oxygenation states of myoglobin, by creating the targetable oxygen (O(2)) sensor Myoglobin-mCherry. In this sensor, changes in myoglobin absorbance features that occur with lost O(2) occupancy -or upon metMb production- control the FRET rate from the fluorescent protein to myoglobin. When O(2) is bound, mCherry fluorescence is only slightly quenched, but if either O(2) is released or met is produced, FRET will increase- and this rate competing with emission reduces both emission yield and lifetime. Nitric oxide (NO) is an important signal (but also a toxic molecule) that can oxidize myoglobin to metMb with absorbance increases in the red visible range. mCherry thus senses both met and deoxygenated myoglobin, which cannot be easily separated at hypoxia. In order to dissect this, we treat cells with NO and investigate how the Myoglobin-mCherry lifetime is affected by generating metMb. More discriminatory power is then achieved when the fluorescent protein EYFP is added to Myoglobin-mCherry, creating a sandwich probe whose lifetime can selectively respond to metMb while being indifferent to O(2) occupancy.

Published
2022

24. Intracellular imaging of metmyoglobin and oxygen using new dual purpose probe EYFP-Myoglobin-mCherry

Author

Branden Roarke, Alessio Andreoni, Dan L. Sackett, Paul M. Hwang, Jay R. Knutson, Rozhin Penjweini, Greg Alspaugh, Katie A. Link, and Mateus Prates Mori

Subjects
General Physics and Astronomy, chemistry.chemical_element, Nitric Oxide, Oxygen, General Biochemistry, Genetics and Molecular Biology, Article, Nitric oxide, chemistry.chemical_compound, Fluorescence Resonance Energy Transfer, General Materials Science, chemistry.chemical_classification, Reactive oxygen species, Myoglobin, General Engineering, General Chemistry, Fluorescence, Förster resonance energy transfer, chemistry, Metmyoglobin, Biophysics, mCherry, Reactive Oxygen Species, Oxidation-Reduction
Abstract

The biological relevance of nitric oxide (NO) and reactive oxygen species (ROS) in signaling, metabolic regulation, and disease treatment has become abundantly clear. The dramatic change in NO/ROS processing that accompanies a changing oxygen landscape calls for new imaging tools that can provide cellular details about both [O2 ] and the production of reactive species. Myoglobin oxidation to the met state by NO/ROS is a known sensor with absorbance changes in the visible range. We previously employed Forster resonance energy transfer to read out the deoxygenation/oxygenation of myoglobin, creating the subcellular [O2 ] sensor Myoglobin-mCherry. We now add the fluorescent protein EYFP to this sensor to create a novel probe that senses both met formation, a proxy for ROS/NO exposure, and [O2 ]. Since both proteins are present in the construct, it can also relieve users from the need to measure fluorescence lifetime, making [O2 ] sensing available to a wider group of laboratories.

Published
2021

25. Mitochondria and oxygen homeostasis

Author

Jay R. Knutson, Rozhin Penjweini, Paul M. Hwang, Mateus Prates Mori, and Ping Yuan Wang

Subjects
Symbiogenesis, Free Radicals, Chemistry, Hypoxia (environmental), chemistry.chemical_element, Cell Biology, Metabolism, Mitochondrion, medicine.disease, medicine.disease_cause, Biochemistry, Oxygen, Cell biology, Mitochondria, Oxidative Stress, Oxygen homeostasis, medicine, Homeostasis, Reactive Oxygen Species, Molecular Biology, Oxygen toxicity, Oxidative stress
Abstract

Molecular oxygen possesses a dual nature due to its highly reactive free radical property: it is capable of oxidizing metabolic substrates to generate cellular energy, but can also serve as a substrate for genotoxic reactive oxygen species generation. As a labile substance upon which aerobic life depends, the mechanisms for handling cellular oxygen have been fine-tuned and orchestrated in evolution. Protection from atmospheric oxygen toxicity as originally posited by the Endosymbiotic Theory of the Mitochondrion is likely to be one basic principle underlying oxygen homeostasis. We briefly review the literature on oxygen homeostasis both in vitro and in vivo with a focus on the role of the mitochondrion where the majority of cellular oxygen is consumed. The insights gleaned from these basic mechanisms are likely to be important for understanding disease pathogenesis and developing strategies for maintaining health.

Published
2021

26. Extracellular acidity reprograms macrophage metabolism and innate responsiveness

Author

Wenyue Dong, Mingfang Lu, Wei Jiang, Yiwei Chu, Chen Yang, Xiaofang Cheng, James Le, Robert S. Munford, Margery G. Smelkinson, Ping Yuan Wang, and Paul M. Hwang

Subjects
medicine.medical_specialty, Immunology, Mitochondrion, Article, Proinflammatory cytokine, Mice, 03 medical and health sciences, 0302 clinical medicine, Immune system, Sepsis, Internal medicine, medicine, Extracellular, Animals, Immunology and Allergy, Macrophage, Cells, Cultured, chemistry.chemical_classification, Chemistry, Fatty acid, Metabolism, Hydrogen-Ion Concentration, Immunity, Innate, Mice, Inbred C57BL, Glutamine, Endocrinology, Macrophages, Peritoneal, Extracellular Space, 030215 immunology
Abstract

Although organ hypofunction and immunosuppression are life-threatening features of severe sepsis, the hypofunctioning organs and immune cells usually regain normal functionality if patients survive. Because tissue interstitial fluid can become acidic during the septic response, we tested the hypothesis that low extracellular pH (pHe) can induce reversible metabolic and functional changes in peritoneal macrophages from C57BL/6J mice. When compared with macrophages cultured at normal pHe, macrophages living in an acidic medium used less glucose and exogenous fatty acid to produce ATP. Lactate, glutamine, and de novo–synthesized fatty acids supported ATP production by mitochondria that gained greater mass, maximal oxygen consumption rate, and spare respiratory capacity. The cells transitioned to an M2-like state, with altered immune responses to LPS and slightly decreased phagocytic ability, yet they regained basal energy production, normal mitochondrial function, and proinflammatory responsiveness when neutral pHe was restored. Low pHe induces changes that support macrophage survival while rendering the cells less proinflammatory (more “tolerant”) and less able to phagocytose bacteria. Macrophage responses to low interstitial pH may contribute to the reversible organ hypofunction and immunoparalysis noted in many patients with sepsis.

Published
2021

27. p53 prevents doxorubicin cardiotoxicity independently of its prototypical tumor suppressor activities

Author

Nathaniel A. Long, Danielle A. Springer, Christopher K. E. Bleck, Yongshun Lin, Jizhong Zou, Ji-Hoon Park, Paul M. Hwang, Ping Yuan Wang, Ju-Gyeong Kang, Jie Li, and Jie Zhuang

Subjects
Male, 0301 basic medicine, Mitochondrial DNA, Heart Diseases, Anthracycline, Induced Pluripotent Stem Cells, Primary Cell Culture, Apoptosis, 030204 cardiovascular system & hematology, Biology, Mitochondrion, DNA, Mitochondrial, Mitochondria, Heart, Mitochondrial Proteins, Mice, 03 medical and health sciences, 0302 clinical medicine, medicine, Animals, Humans, Myocytes, Cardiac, Doxorubicin, Mice, Knockout, Cardiotoxicity, Organelle Biogenesis, Multidisciplinary, TFAM, DNA-Binding Proteins, Mice, Inbred C57BL, 030104 developmental biology, PNAS Plus, Mitochondrial biogenesis, Mutation, Cancer research, Tumor Suppressor Protein p53, Cardiomyopathies, Transcription Factors, medicine.drug
Abstract

Doxorubicin is a widely used chemotherapeutic agent that causes dose-dependent cardiotoxicity in a subset of treated patients, but the genetic determinants of this susceptibility are poorly understood. Here, we report that a noncanonical tumor suppressor activity of p53 prevents cardiac dysfunction in a mouse model induced by doxorubicin administered in divided low doses as in the clinics. While relatively preserved in wild-type (p53(+/+)) state, mice deficient in p53 (p53(−/−)) developed left ventricular (LV) systolic dysfunction after doxorubicin treatment. This functional decline in p53(−/−) mice was associated with decreases in cardiac oxidative metabolism, mitochondrial mass, and mitochondrial genomic DNA (mtDNA) homeostasis. Notably, mice with homozygous knockin of the p53 R172H (p53(172H/H)) mutation, which like p53(−/−) state lacks the prototypical tumor suppressor activities of p53 such as apoptosis but retains its mitochondrial biogenesis capacity, showed preservation of LV function and mitochondria after doxorubicin treatment. In contrast to p53-null state, wild-type and mutant p53 displayed distinct mechanisms of transactivating mitochondrial transcription factor A (TFAM) and p53-inducible ribonucleotide reductase 2 (p53R2), which are involved in mtDNA transcription and maintenance. Importantly, supplementing mice with a precursor of NAD(+) prevented the mtDNA depletion and cardiac dysfunction. These findings suggest that loss of mtDNA contributes to cardiomyopathy pathogenesis induced by doxorubicin administered on a schedule simulating that in the clinics. Given a similar mtDNA protection role of p53 in doxorubicin-treated human induced pluripotent stem cell (iPSC)-derived cardiomyocytes, the mitochondrial markers associated with cardiomyopathy development observed in blood and skeletal muscle cells may have prognostic utility.

Published
2019

28. Odorant-Binding Protein

Author

Paul M. Hwang, Jonathan Pevsner, Solomon H. Snyder, and Pamela Sklar

Subjects
Biochemistry, biology, Chemistry, Odorant-binding protein, biology.protein
Published
2021

29. Reducing fatty acid oxidation improves cancer-free survival in a mouse model of Li-Fraumeni syndrome

Author

Komudi Singh, Paul M. Hwang, Ju Gyeong Kang, Ping Yuan Wang, Michael J. Wolfgang, Jin Ma, Jie Li, Matthew F. Starost, and Mehdi Pirooznia

Subjects
0301 basic medicine, Male, Cancer Research, Carcinogenesis, medicine.disease_cause, Li-Fraumeni Syndrome, Myoblasts, chemistry.chemical_compound, Mice, 0302 clinical medicine, Gene Knock-In Techniques, Prospective Studies, Beta oxidation, Cells, Cultured, chemistry.chemical_classification, Aged, 80 and over, Mice, Knockout, Myoglobin, Fatty Acids, food and beverages, Middle Aged, Oncology, 030220 oncology & carcinogenesis, Ribosomal protein s6, Female, Haploinsufficiency, Oxidation-Reduction, Adult, Heterozygote, Adolescent, Primary Cell Culture, Biology, Article, Disease-Free Survival, 03 medical and health sciences, Young Adult, Germline mutation, medicine, Animals, Humans, Genetic Predisposition to Disease, Germ-Line Mutation, Aged, Fatty acid metabolism, Carnitine O-Palmitoyltransferase, Fatty acid, medicine.disease, Disease Models, Animal, 030104 developmental biology, chemistry, Li–Fraumeni syndrome, Case-Control Studies, Cancer research, Tumor Suppressor Protein p53, Energy Metabolism
Abstract

Germline mutations of TP53, which cause the cancer predisposition disorder Li-Fraumeni syndrome (LFS), can increase mitochondrial activity as well as fatty acid β-oxidation (FAO) in mice. Increased fatty acid metabolism can promote cancer malignancy, but its specific contribution to tumorigenesis in LFS remains unclear. To investigate this, we crossed LFS mice carrying the p53 R172H knock-in mutation (p53172H/H, homolog of the human TP53 R175H LFS mutation) with myoglobin-knockout (MB−/−) mice known to have decreased FAO. MB−/− p53172H/H double-mutant mice also showed mildly reduced FAO in thymus, a common site of T lymphoma development in LFS mice, in association with an approximately 40% improvement in cancer-free survival time. RNA sequencing profiling revealed that the p53 R172H mutation promotes mitochondrial metabolism and ribosome biogenesis, both of which are suppressed by the disruption of MB. The activation of ribosomal protein S6, involved in protein translation and implicated in cancer promotion, was also inhibited in the absence of MB. To further confirm the role of FAO in lymphomagenesis, mitochondrial FAO enzyme, carnitine palmitoyltransferase 2 (CPT2), was specifically disrupted in T cells of p53172H/H mice using a Cre-loxP–mediated strategy. The heterozygous knockout of CPT2 resulted in thymus FAO haploinsufficiency and an approximately 30% improvement in survival time, paralleling the antiproliferative signaling observed with MB disruption. Thus, this study demonstrates that moderating FAO in LFS can suppress tumorigenesis and improve cancer-free survival with potential implications for cancer prevention. Prevention Relevance: Mildly inhibiting the increased fatty acid oxidation observed in a mouse model of Li-Fraumeni syndrome, a cancer predisposition disorder caused by inherited mutations of TP53, dampens aberrant pro-tumorigenic cell signaling and improves the survival time of these mice, thereby revealing a potential strategy for cancer prevention in patients.

Published
2020

30. Tumor predisposition and cancer syndromes as models to study gene X environment interactions

Author

David Malkin, Giovanni Gaudino, John H.J. Petrini, James E. Cleaver, Webster K. Cavenee, Bruce Beutler, Angela Bononi, Haining Yang, Tak W. Mak, Elizabeth P. Henske, William D. Foulkes, Carlo M. Croce, Michele Carbone, Sarah T. Arron, Paul M. Hwang, Alan D. D'Andrea, Ian D. Hickson, Richard D. Kolodner, Flavia Novelli, Raymond J. Monnat, Laura S. Schmidt, Joanna L. Groden, and Harvey I. Pass

Subjects
Cell division, DNA damage, General Mathematics, Biology, Malignancy, Article, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Germline mutation, Neoplasms, medicine, Animals, Humans, Genetic Predisposition to Disease, Gene, Carcinogen, Germ-Line Mutation, Applied Mathematics, Cancer, medicine.disease, chemistry, 030220 oncology & carcinogenesis, Cancer research, Gene-Environment Interaction, DNA
Abstract

Cell division and organismal development are exquisitely orchestrated and regulated processes. The dysregulation of the molecular mechanisms underlying these processes may cause cancer, a consequence of cell-intrinsic and/or cell-extrinsic events. Cellular DNA can be damaged by spontaneous hydrolysis, reactive oxygen species, aberrant cellular metabolism, or other perturbations that cause DNA damage. Moreover, several environmental factors may damage the DNA, alter cellular metabolism, or affect the ability of cells to interact with their microenvironment. While some environmental factors are well established as carcinogens, there remains a large knowledge gap of others owing to the difficulty in identifying them because of the typically long interval between carcinogen exposure and cancer diagnosis. DNA damage increases in cells harboring mutations that impair their ability to correctly repair the DNA. Tumor predisposition syndromes in which cancers arise at an accelerated rate and in different organs - the equivalent of a sensitized background - provide a unique opportunity to examine how gene–environment interactions (GxE) influence cancer risk when the initiating genetic defect responsible for malignancy is known. Understanding the molecular processes that are altered by specific germline mutations, environmental exposures and related mechanisms that promote cancer, will allow the design of novel and effective preventive and therapeutic strategies.

Published
2020

31. Pilot Study Assessing Tolerability and Metabolic Effects of Metformin in Patients With Li-Fraumeni Syndrome

Author

Rebecca D. Huffstutler, Kevin W Dodd, Phuong L. Mai, Michael Pollak, Sharon A. Savage, Antonio Tito Fojo, Christine M Bryla, Christina M. Annunziata, Paul M. Hwang, Neha Singh, Ping Yuan Wang, Payal P. Khincha, and Farzana L. Walcott

Subjects
Cancer Research, medicine.medical_specialty, medicine.medical_treatment, medicine.disease_cause, Article, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, medicine, Adverse effect, 030304 developmental biology, 0303 health sciences, business.industry, Insulin, Cancer, medicine.disease, Metformin, Endocrinology, Oncology, Tolerability, Li–Fraumeni syndrome, 030220 oncology & carcinogenesis, Lactic acidosis, business, Oxidative stress, medicine.drug
Abstract

Background Li-Fraumeni syndrome (LFS) is a highly penetrant autosomal dominant cancer predisposition disorder caused by germline TP53 pathogenic variants. Patients with LFS have increased oxidative phosphorylation capacity in skeletal muscle and oxidative stress in blood. Metformin inhibits oxidative phosphorylation, reducing available energy for cancer cell proliferation and decreasing production of reactive oxygen species that cause DNA damage. Thus, metformin may provide pharmacologic risk reduction for cancer in patients with LFS, but its safety in nondiabetic patients with germline TP53 pathogenic variants has not been documented. Methods This study assessed safety and tolerability of metformin in nondiabetic LFS patients and measured changes in metabolic profiles. Adult patients with LFS and germline TP53 variant received 14 weeks of metformin. Blood samples were obtained for measurement of serum insulin-like growth factor–1, insulin, and insulin-like growth factor binding protein 3. Hepatic mitochondrial function was assessed with fasting exhaled CO2 after ingestion of 13C-labeled methionine. Changes in serum metabolome were measured. All statistical tests were 2-sided. Results We enrolled 26 participants: 20 females and 6 males. The most common adverse events were diarrhea (50.0%) and nausea (46.2%). Lactic acidosis did not occur, and there were no changes in fasting glucose. Cumulative mean 13C exhalation was statistically significantly suppressed by metformin (P = .001). Mean levels of insulin-like growth factor binding protein 3 and insulin-like growth factor-1 were statistically significantly lowered (P = .02). Lipid metabolites and branched-chain amino acids accumulated. Conclusions Metformin was safe and tolerable in patients with LFS. It suppressed hepatic mitochondrial function as expected in these individuals. This study adds to the rationale for development of a pharmacologic risk-reduction clinical trial of metformin in LFS.

Published
2020

32. Protective role of p53 in doxorubicin-induced cardiomyopathy as a mitochondrial disease

Author

Paul M. Hwang, Masahiro Nishi, and Ping Yuan Wang

Subjects
0301 basic medicine, p53, Cancer Research, Mitochondrial DNA, Mitochondrial disease, Cardiomyopathy, Mitochondrion, doxorubicin, 03 medical and health sciences, 0302 clinical medicine, NAD+, Genetic model, medicine, Doxorubicin, TFAM, Cardiotoxicity, business.industry, mtDNA, medicine.disease, mitochondria, Author's Views, 030104 developmental biology, p53R2, Cancer research, Molecular Medicine, business, cardiomyopathy, 030217 neurology & neurosurgery, medicine.drug
Abstract

Doxorubicin is widely used against cancer but carries the risk of a progressive cardiomyopathy associated with mitochondrial loss. Using genetic models, our recent study demonstrates that mitochondrial genomic DNA regulation by tumor protein p53 (TP53, best known as p53) prevents the cardiotoxicity of low dose doxorubicin which does not activate the p53-dependent cell death pathway.

Published
2019

33. Ambient oxygen promotes tumorigenesis.

Author

Ho Joong Sung, Wenzhe Ma, Matthew F Starost, Cory U Lago, Philip K Lim, Michael N Sack, Ju-Gyeong Kang, Ping-yuan Wang, and Paul M Hwang

Subjects
Medicine, Science
Abstract

Oxygen serves as an essential factor for oxidative stress, and it has been shown to be a mutagen in bacteria. While it is well established that ambient oxygen can also cause genomic instability in cultured mammalian cells, its effect on de novo tumorigenesis at the organismal level is unclear. Herein, by decreasing ambient oxygen exposure, we report a ∼50% increase in the median tumor-free survival time of p53-/- mice. In the thymus, reducing oxygen exposure decreased the levels of oxidative DNA damage and RAG recombinase, both of which are known to promote lymphomagenesis in p53-/- mice. Oxygen is further shown to be associated with genomic instability in two additional cancer models involving the APC tumor suppressor gene and chemical carcinogenesis. Together, these observations represent the first report directly testing the effect of ambient oxygen on de novo tumorigenesis and provide important physiologic evidence demonstrating its critical role in increasing genomic instability in vivo.

Published
2011
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34. Modeling the prevalent germline

Author

Ping Yuan Wang, Ji-Hoon Park, and Paul M. Hwang

Subjects
Genetics, Editorial, Oncology, Li–Fraumeni syndrome, mouse model, Mutation (genetic algorithm), medicine, p53 oligomerization, Li-Fraumeni syndrome, Biology, medicine.disease, Germline
Published
2019

35. Hypoxia-tropic Protein Nanocages for Modulation of Tumor- and Chemotherapy-Associated Hypoxia

Author

Jie Zhuang, Seung Woo Chung, Paul M. Hwang, Xinglu Huang, Gilad Halpert, Jun Yang, Karina Negron, Justin Hanes, Xuanrong Sun, Buwei Huang, Jung Soo Suk, and Yumin Oh

Subjects
medicine.medical_treatment, General Physics and Astronomy, Antineoplastic Agents, 02 engineering and technology, 010402 general chemistry, 01 natural sciences, Article, Polyethylene Glycols, Extracellular matrix, Nanocages, Nanocapsules, Cell Line, Tumor, Neoplasms, Spheroids, Cellular, medicine, Humans, General Materials Science, Fluorescent Dyes, Chemotherapy, biology, Tumor hypoxia, Chemistry, General Engineering, Hypoxia (medical), 021001 nanoscience & nanotechnology, Cell Hypoxia, 0104 chemical sciences, Ferritin, Oxygen, Tumor progression, Ferritins, Cancer research, biology.protein, PEGylation, medicine.symptom, Cisplatin, 0210 nano-technology
Abstract

Despite its central role in tumor progression and treatment resistance, poor vascularization that necessitates penetration of therapeutics through tumor extracellular matrix (ECM) constitutes a significant challenge to managing tumor hypoxia via conventional systemic treatment regimens. In addition, methods to target hypoxic tumor cells are lacking. Here, we discovered that human ferritin nanocages (FTn) possess an intrinsic ability to preferentially engage with hypoxic tumor tissues, in addition to normoxic tumor areas. We also developed a simple method of endowing FTn with spatially controlled "mosaic" surface poly(ethylene glycol) (PEG) coatings that facilitate deep penetration of FTn through ECM to reach hypoxic tumor tissues while retaining its inherent hypoxia-tropic property. Hypoxia-inhibiting agents systemically delivered via this surface-PEGylated FTn were readily accumulated in hypoxic tumor tissues, thereby providing significantly enhanced therapeutic benefits compared to the identical agents delivered in solution as a stand-alone therapy or an adjuvant to restore efficacy of conventional systemic chemotherapy.

Published
2018

36. Inhibiting mitochondrial respiration prevents cancer in a mouse model of Li-Fraumeni syndrome

Author

Jie Li, Rebecca D. Huffstutler, Sharon A. Savage, Ji-Hoon Park, Ju-Gyeong Kang, Jie Zhuang, Antonio Tito Fojo, Christina Bryla, Matthew F. Starost, Farzana L. Walcott, Ping Yuan Wang, Michael Pollak, Phuong L. Mai, S. Lalith Talagala, Christina M. Annunziata, and Paul M. Hwang

Subjects
Adult, Male, p53, 0301 basic medicine, medicine.medical_specialty, mouse model, Mutant, cyclin D1, Pilot Projects, Biology, medicine.disease_cause, Jurkat cells, Li-Fraumeni Syndrome, Jurkat Cells, Mice, 03 medical and health sciences, Oxygen Consumption, Germline mutation, DNA polymerase gamma, Internal medicine, medicine, Animals, Humans, Cell Proliferation, News and Thoughts, Autophagy, Cancer, Neoplasms, Experimental, General Medicine, Middle Aged, medicine.disease, Metformin, Mice, Mutant Strains, Mitochondria, 3. Good health, 030104 developmental biology, Endocrinology, Li–Fraumeni syndrome, Cancer research, Female, Tumor Suppressor Protein p53, Carcinogenesis, Signal Transduction, medicine.drug
Abstract

Li-Fraumeni syndrome (LFS) is a cancer predisposition disorder caused by germline mutations in TP53 that can lead to increased mitochondrial metabolism in patients. However, the implications of altered mitochondrial function for tumorigenesis in LFS are unclear. Here, we have reported that genetic or pharmacologic disruption of mitochondrial respiration improves cancer-free survival in a mouse model of LFS that expresses mutant p53. Mechanistically, inhibition of mitochondrial function increased autophagy and decreased the aberrant proliferation signaling caused by mutant p53. In a pilot study, LFS patients treated with metformin exhibited decreases in mitochondrial activity concomitant with activation of antiproliferation signaling, thus reproducing the effects of disrupting mitochondrial function observed in LFS mice. These observations indicate that a commonly prescribed diabetic medicine can restrain mitochondrial metabolism and tumorigenesis in an LFS model, supporting its further consideration for cancer prevention in LFS patients.

Published
2016

37. TP53 mutation, mitochondria and cancer

Author

Paul M. Hwang, Ping Yuan Wang, and William M. Kamp

Subjects
0301 basic medicine, Genetics, Mutation, Mutant, Mutation, Missense, Cancer, Mitochondrion, Biology, medicine.disease_cause, medicine.disease, Article, Mitochondria, Cell biology, 03 medical and health sciences, Basal (phylogenetics), 030104 developmental biology, Neoplasms, Cancer cell, medicine, Humans, Missense mutation, Tumor Suppressor Protein p53, Function (biology), Developmental Biology
Abstract

Under normal conditions, basal levels of wild-type p53 promote mitochondrial function through multiple mechanisms. Remarkably, some missense mutations of p53, in contrast to the null state, can result in the retention of its metabolic activities. These effects are particularly prominent in the mitochondria and demonstrate a functional role for mutant p53 in cancer metabolism. This review summarizes accumulating data on the mechanisms by which p53 missense mutations can regulate mitochondrial metabolism and promote the viability and survival of both normal and cancer cells, thus acting as a double edged sword for the host. Greater understanding of these mechanisms may provide insights for developing new treatment or preventive strategies against cancer.

Published
2016

38. Mouse homolog of the human TP53 R337H mutation reveals its role in tumorigenesis

Author

Jie Zhuang, Ji-Hoon Park, Paul M. Hwang, Sharon A. Savage, Ju-Gyeong Kang, Jie Li, Ping Yuan Wang, Chengyu Liu, Matthew F. Starost, Jichun Chen, and Maria Isabel Achatz

Subjects
0301 basic medicine, Male, Transcriptional Activation, Cancer Research, Tumor suppressor gene, DNA damage, Carcinogenesis, Mice, Transgenic, Biology, medicine.disease_cause, Article, 03 medical and health sciences, Transactivation, Mice, Germline mutation, medicine, Animals, Humans, Genetic Predisposition to Disease, Gene Knock-In Techniques, Allele, Alleles, Germ-Line Mutation, Mutation, Homozygote, Liver Neoplasms, Fibroblasts, Molecular biology, Penetrance, Mice, Inbred C57BL, 030104 developmental biology, Cell Transformation, Neoplastic, Oncology, Liver, Tumor Suppressor Protein p53, Brazil, DNA Damage
Abstract

Inheritance of germline mutations in the tumor suppressor gene TP53 causes Li-Fraumeni syndrome (LFS), a cancer predisposition disorder. The arginine to histidine substitution at amino acid position 337 of p53 (R337H) is a founder mutation highly prevalent in southern and southeastern Brazil and is considered an LFS mutation. Although this mutation is of significant clinical interest, its role in tumorigenesis using animal models has not been described. Here, we generate a knockin mouse model containing the homologous R337H mutation (mouse R334H). De novo tumorigenesis was not significantly increased in either heterozygous (p53334R/H) or homozygous (p53334H/H) p53 R334H knockin mice compared with wild-type mice. However, susceptibility to diethylnitrosamine (DEN)-induced liver carcinogenesis was increased in a mutant allele dose-dependent manner. In parallel, p53334H/H mice exposed to DEN exhibited increased DNA damage but decreased cell-cycle regulation in the liver. Oligomerization of p53, which is required for transactivation of target genes, was reduced in R334H liver, consistent with its decreased nuclear activity compared with wild-type. By modeling a TP53 mutation in mice that has relatively weak cancer penetrance, this study provides in vivo evidence that the human R337H mutation can compromise p53 activity and promote tumorigenesis. Significance: A germline mutation in the oligomerization domain of p53 decreases its transactivation potential and renders mice susceptible to carcinogen-induced liver tumorigenesis. Cancer Res; 78(18); 5375–83. ©2018 AACR.

Published
2018

39. Erratum to: Low ambient oxygen prevents atherosclerosis

Author

Audrey Noguchi, Ju Gyeong Kang, Ho Joong Sung, Marcelo Amar, Ji-Hoon Park, Paul M. Hwang, Danielle A. Springer, Michele D. Allen, Milton Pryor, Alan T. Remaley, Jichun Chen, Ping Yuan Wang, and Jaeyul Kwon

Subjects
medicine.medical_specialty, stomatognathic system, business.industry, Family medicine, Health science, Drug Discovery, medicine, nutritional and metabolic diseases, Molecular Medicine, Ambient oxygen, business, health care economics and organizations, Genetics (clinical)
Abstract

1 Center for Molecular Medicine, National Heart, Lung, and Blood Institute, National Institutes of Health, Bethesda, MD, USA 2 College of Health Science, Eulji University, Seongnam, South Korea 3 Cardiovascular-Pulmonary Branch, NHLBI, NIH, Bethesda, MD, USA 4 Murine Phenotyping Core, NHLBI, NIH, Bethesda, MD, USA 5 School of Medicine, ChungnamNational University, Daejeon, South Korea 6 Hematology Branch, NHLBI, NIH, Bethesda, MD, South Korea J Mol Med (2016) 94:287–289 DOI 10.1007/s00109-016-1399-y

Published
2016

40. Polo-like kinase 2 activates an antioxidant pathway to promote the survival of cells with mitochondrial dysfunction

Author

Paula J. Hurley, Jie Li, Paul M. Hwang, Fred Bunz, Wenzhe Ma, and Ping Yuan Wang

Subjects
Antioxidant, Cell Survival, NF-E2-Related Factor 2, medicine.medical_treatment, Transplantation, Heterologous, Active Transport, Cell Nucleus, Polo-like kinase, Protein Serine-Threonine Kinases, Mitochondrion, Biology, medicine.disease_cause, Biochemistry, Antioxidants, Article, Glycogen Synthase Kinase 3, Mice, Cell Line, Tumor, Physiology (medical), medicine, Animals, Humans, ASK1, Phosphorylation, RNA, Small Interfering, Kinase, HCT116 Cells, Mitochondria, Cell biology, Oxidative Stress, RNA Interference, Signal transduction, Oxidative stress
Abstract

We previously reported that Polo-like kinase 2 (PLK2) is highly expressed in cells with defective mitochondrial respiration and is essential for their survival. Although PLK2 has been widely studied as a cell cycle regulator, we have uncovered an antioxidant function for this kinase that activates the GSK3-NRF2 signaling pathway. Here, we report that the expression of PLK2 is responsive to oxidative stress and that PLK2 mediates antioxidant signaling by phosphorylating GSK3, thereby promoting the nuclear translocation of NRF2. We further show that the antioxidant activity of PLK2 is essential for preventing p53-dependent necrotic cell death. Thus, the regulation of redox homeostasis by PLK2 promotes the survival of cells with dysfunctional mitochondria, which may have therapeutic implications for cancer and neurodegenerative diseases.

Published
2014

41. Mitochondrial disulfide relay mediates translocation of p53 and partitions its subcellular activity

Author

Paul M. Hwang, Jie Zhuang, Ping Yuan Wang, Ju Gyeong Kang, Xiaoyuan Chen, and Xinglu Huang

Subjects
Mitochondrial DNA, DNA Repair, Blotting, Western, Oxidative phosphorylation, Biology, Mitochondrion, DNA, Mitochondrial, Mitochondrial Membrane Transport Proteins, Mice, Mitochondrial membrane transport protein, Mitochondrial Precursor Protein Import Complex Proteins, medicine, Animals, Humans, Disulfides, Nuclear protein, Cell Nucleus, Mice, Knockout, Microscopy, Confocal, Multidisciplinary, Biological Sciences, HCT116 Cells, Mitochondria, Cell biology, Transport protein, Mice, Inbred C57BL, Protein Transport, Cell nucleus, medicine.anatomical_structure, Mutation, biology.protein, RNA Interference, Tumor Suppressor Protein p53, Nuclear localization sequence, Protein Binding
Abstract

p53, a critical tumor suppressor, regulates mitochondrial respiration, but how a nuclear protein can orchestrate the function of an organelle encoded by two separate genomes, both of which require p53 for their integrity, remains unclear. Here we report that the mammalian homolog of the yeast mitochondrial disulfide relay protein Mia40 (CHCHD4) is necessary for the respiratory-dependent translocation of p53 into the mitochondria. In the setting of oxidative stress, increased CHCHD4 expression partitions p53 into the mitochondria and protects its genomic integrity while decreasing p53 nuclear localization and transcriptional activity. Conversely, decreased CHCHD4 expression prevents the mitochondrial translocation of p53 while augmenting its nuclear localization and activity. Thus, the mitochondrial disulfide relay system allows p53 to regulate two spatially segregated genomes depending on oxidative metabolic activity.

Published
2013

42. Increased Oxidative Metabolism in the Li–Fraumeni Syndrome

Author

Wenzhe Ma, Jeong W. Choi, Paul M. Hwang, Ju Gyeong Kang, Cory U. Lago, Louise C. Strong, Robert S. Balaban, Ping Yuan Wang, Jie Zhuang, Ross Arena, Qais A. Ali, D. Tripodi, S. Lalith Talagala, Joon-Young Park, and Francesco S. Celi

Subjects
Male, Heterozygote, medicine.medical_specialty, Phosphocreatine, Weight Lifting, Pilot Projects, Oxidative phosphorylation, Mitochondrion, medicine.disease_cause, Article, Li-Fraumeni Syndrome, Mice, Oxygen Consumption, Germline mutation, Internal medicine, medicine, Animals, Humans, Muscle, Skeletal, Exercise, Germ-Line Mutation, business.industry, Case-control study, Skeletal muscle, Heterozygote advantage, General Medicine, Genes, p53, medicine.disease, Mitochondria, Muscle, Disease Models, Animal, Endocrinology, medicine.anatomical_structure, Li–Fraumeni syndrome, Case-Control Studies, Female, Energy Metabolism, Carcinogenesis, business
Abstract

There is growing evidence that alterations in metabolism may contribute to tumorigenesis. Here, we report on members of families with the Li-Fraumeni syndrome who carry germline mutations in TP53, the gene encoding the tumor-suppressor protein p53. As compared with family members who are not carriers and with healthy volunteers, family members with these mutations have increased oxidative phosphorylation of skeletal muscle. Basic experimental studies of tissue samples from patients with the Li-Fraumeni syndrome and a mouse model of the syndrome support this in vivo finding of increased mitochondrial function. These results suggest that p53 regulates bioenergetic homeostasis in humans. (Funded by the National Heart, Lung, and Blood Institute and the National Institutes of Health; ClinicalTrials.gov number, NCT00406445.).

Published
2013

43. Forkhead Box O3A (FOXO3) and the Mitochondrial Disulfide Relay Carrier (CHCHD4) Regulate p53 Protein Nuclear Activity in Response to Exercise*

Author

Ping Yuan Wang, William M. Kamp, Jie Li, Jie Zhuang, Paul M. Hwang, Ju-Gyeong Kang, and Chengyu Liu

Subjects
0301 basic medicine, Active Transport, Cell Nucleus, Response Elements, Biochemistry, Mitochondrial Membrane Transport Proteins, 03 medical and health sciences, Mitochondrial membrane transport protein, Mice, 0302 clinical medicine, Sirtuin 1, Physical Conditioning, Animal, medicine, Animals, Humans, Gene Regulation, Molecular Biology, Transcription factor, Cell Nucleus, Mice, Knockout, biology, Forkhead Box Protein O3, Cell Biology, Cell biology, Cell nucleus, 030104 developmental biology, medicine.anatomical_structure, biology.protein, FOXO3, Histone deacetylase, Tumor Suppressor Protein p53, 030217 neurology & neurosurgery, Nuclear localization sequence
Abstract

Although exercise is linked with improved health, the specific molecular mechanisms underlying its various benefits require further clarification. Here we report that exercise increases the nuclear localization and activity of p53 by acutely down-regulating coiled-coil-helix-coiled-coil-helix domain 4 (CHCHD4), a carrier protein that mediates p53 import into the mitochondria. This response to exercise is lost in transgenic mice with constitutive expression of CHCHD4. Mechanistically, exercise-induced nuclear transcription factor FOXO3 binds to the CHCHD4 promoter and represses its expression, preventing the translocation of p53 to the mitochondria and thereby increasing p53 nuclear localization. The synergistic increase in nuclear p53 and FOXO3 by exercise can facilitate their known interaction in transactivating Sirtuin 1 (SIRT1), a NAD+-dependent histone deacetylase that mediates adaptation to various stresses. Thus, our results reveal one mechanism by which exercise could be involved in preventing cancer and potentially other diseases associated with aging.

Published
2016

44. p53 as guardian of the mitochondrial genome

Author

Jie Zhuang, Ji-Hoon Park, Paul M. Hwang, and Jie Li

Subjects
0301 basic medicine, Genome instability, Mitochondrial DNA, DNA Repair, DNA repair, Biophysics, Biology, Mitochondrion, medicine.disease_cause, Biochemistry, DNA, Mitochondrial, Models, Biological, Article, Genomic Instability, 03 medical and health sciences, Structural Biology, Genetics, medicine, Animals, Humans, Molecular Biology, Cell Nucleus, Mechanism (biology), Cell Biology, Nuclear DNA, Mitochondria, Cell nucleus, Protein Transport, 030104 developmental biology, medicine.anatomical_structure, Genome, Mitochondrial, Tumor Suppressor Protein p53, Carcinogenesis
Abstract

Participating in the repair of nuclear DNA is one mechanism by which p53 suppresses tumorigenesis, but there is growing evidence that p53 also helps maintain the mitochondrial genome through its translocation into mitochondria and interactions with mtDNA repair proteins. Because of the susceptibility of mtDNA to oxidative damage and replication errors, it is vital to protect mtDNA genomic stability to preserve health and fitness. Here, we focus on reviewing the evidence for the involvement of p53 in maintaining the integrity of mtDNA through its activities in both the nucleus and the mitochondria.

Published
2016

45. p53, Aerobic Metabolism, and Cancer

Author

Ho Joong Sung, Cory U. Lago, Wenzhe Ma, Ping Yuan Wang, and Paul M. Hwang

Subjects
Genome instability, Physiology, Cellular respiration, Cell Respiration, Clinical Biochemistry, Apoptosis, Computational biology, Biology, Mitochondrion, Biochemistry, Genomic Instability, Mice, Neoplasms, Autophagy, medicine, Animals, Humans, Anaerobiosis, Molecular Biology, Aerobic capacity, General Environmental Science, Genetics, Cancer prevention, Cancer, Cell Biology, Cell cycle, Forum Review Articles, medicine.disease, Aerobiosis, Mitochondria, General Earth and Planetary Sciences, Tumor Suppressor Protein p53, Oxidation-Reduction, Function (biology)
Abstract

p53 regulates the cell cycle and deoxyribonucleic acid (DNA) repair pathways as part of its unequivocally important function to maintain genomic stability. Intriguingly, recent studies show that p53 can also transactivate genes involved in coordinating the two major pathways of energy generation to promote aerobic metabolism, but how this serves to maintain genomic stability is less clear. In an attempt to understand the biology, this review presents human epidemiologic data on the inverse relationship between aerobic capacity and cancer incidence that appears to be mirrored by the impact of p53 on aerobic capacity in mouse models. The review summarizes mechanisms by which p53 regulates mitochondrial respiration and proposes how this might contribute to maintaining genomic stability. Although disparate in nature, the data taken together suggest that the promotion of aerobic metabolism by p53 serves as an important tumor suppressor activity and may provide insights for cancer prevention strategies in the future. Antioxid. Redox Signal. 15, 1739–1748.

Published
2011

46. Zinc Finger Protein Tristetraprolin Interacts with CCL3 mRNA and Regulates Tissue Inflammation

Author

Marcelo Amar, Ju Gyeong Kang, Alan T. Remaley, Paul M. Hwang, Ping Yuan Wang, Jaeyul Kwon, and Perry J. Blackshear

Subjects
Zinc finger, medicine.medical_treatment, Immunology, Tristetraprolin, CCL3, Inflammation, respiratory system, Biology, Systemic inflammation, Molecular biology, Proinflammatory cytokine, Cytokine, hemic and lymphatic diseases, medicine, Immunology and Allergy, Macrophage, heterocyclic compounds, medicine.symptom, neoplasms, therapeutics
Abstract

Zinc finger protein tristetraprolin (TTP) modulates macrophage inflammatory activity by destabilizing cytokine mRNAs. In this study, through a screen of TTP-bound mRNAs in activated human macrophages, we have identified CCL3 mRNA as the most abundantly bound TTP target mRNA and have characterized this interaction via conserved AU-rich elements. Compared to the wild-type cells, TTP−/− macrophages produced higher levels of LPS-induced CCL3. In addition, the plasma level of CCL3 in TTP−/− mice was markedly higher than that in wild-type mice. To determine the in vivo significance of TTP-regulated CCL3, we generated CCL3−/−TTP−/− double-knockout mice. Along with decreased proinflammatory cytokines in their paw joints, there were significant functional and histologic improvements in the inflammatory arthritis of TTP−/− mice when CCL3 was absent, although cachexia, reflecting systemic inflammation, was notably unaffected. Furthermore, the marked exacerbation of aortic plaque formation caused by TTP deficiency in the APOE−/− mouse model of atherosclerosis was also rescued by disrupting CCL3. Taken together, our data indicate that the interaction between TTP and CCL3 mRNA plays an important role in modulating localized inflammatory processes in tissues that are dissociated from the systemic manifestations of chronic inflammation.

Published
2011

47. FOS expression in blood as a LDL-independent marker of statin treatment

Author

Ho Joong Sung, Leslie G. Biesecker, Yesoda N. Rao, Cynthia L. Brenneman, Ju Gyeong Kang, Paul M. Hwang, Vandana Sachdev, Arshed A. Quyyumi, Sarah I. Jawed, Salman Sher, and Flavia M. Facio

Subjects
Male, medicine.medical_specialty, Statin, RHOA, medicine.drug_class, Inflammation, Pharmacology, Article, chemistry.chemical_compound, Internal medicine, medicine, Humans, Prospective Studies, Aged, biology, Vascular disease, Cholesterol, Macrophages, Monocyte, Genes, fos, Cholesterol, LDL, Middle Aged, medicine.disease, C-Reactive Protein, Endocrinology, medicine.anatomical_structure, chemistry, Monocyte differentiation, HMG-CoA reductase, Leukocytes, Mononuclear, biology.protein, Female, Hydroxymethylglutaryl-CoA Reductase Inhibitors, medicine.symptom, Cardiology and Cardiovascular Medicine, Proto-Oncogene Proteins c-fos, Biomarkers
Abstract

Statins have been proposed to exert pleiotropic benefits that extend beyond that predicted by cholesterol reduction (1,2), even though some analyses argue against the existence of such non-cholesterol related effects in preventing adverse cardiovascular events (3). A meta-regression analysis of data from statin and non-statin clinical treatment trials has shown that the changes in LDL cholesterol levels alone are sufficient to account for the decrease in cardiovascular events (3). However, at the cellular level, statins have potent anti-inflammatory and other beneficial effects on immune, endothelial and smooth muscle cells (2). At the molecular level, these HMG CoA reductase inhibitors not only decrease cholesterol synthesis but also inhibit the isoprenylation and activation of important intracellular signaling proteins such as RhoA and Ras that can affect pathogenesis (1,2). These disparate basic and clinical observations indicate a need for further translational investigations to improve our understanding of statin treatment effects. In this regard, the identification of biomarkers that provide additional information about the therapeutic activities of statins may be helpful. Various cellular elements and signaling pathways contribute to atherosclerosis, but circulating inflammatory cells play a pivotal role in the initiation and final manifestation of disease (4,5). Recent work examining the transcriptional profiles of blood cells in patients with coronary artery disease provide insights into cardiovascular pathogenesis supporting the potential clinical utility of such investigations (6-8). We previously reported that the mononuclear cell mRNA level of the Finkel-Biskis-Jinkins Osteosarcoma (FOS) gene, a transcription factor essential for monocyte differentiation into macrophages (9), was correlated with the severity of atherosclerosis (10). The localization of FOS to macrophages and smooth muscle cells in plaques and its importance in calcification suggest that it may also play a direct role in atherosclerosis (10-12). Based on the known transcriptional regulation of FOS through a cholesterol-independent pathway (13), we hypothesized that blood FOS levels will be sensitive to statin treatment independent of LDL cholesterol levels and in a dose dependent manner. The following translational study was designed to determine whether FOS expression in blood can serve as a statin treatment response marker that could then be evaluated further with regard to clinical application given, for example, the questions about the pleiotropic effects of statins.

Published
2010

48. p53 Improves Aerobic Exercise Capacity and Augments Skeletal Muscle Mitochondrial DNA Content

Author

Robert S. Balaban, Joon-Young Park, Takumi Matsumoto, Paul M. Hwang, Stasia A. Anderson, Jeong W. Choi, Wenzhe Ma, Scot C. Leary, Ju Gyeong Kang, Ho Joong Sung, and Ping Yuan Wang

Subjects
Male, Mitochondrial DNA, Time Factors, Physiology, Myoblasts, Skeletal, Physical Exertion, Physical exercise, Mitochondrion, Biology, Response Elements, Transfection, DNA, Mitochondrial, Article, Ventricular Function, Left, Cell Line, Mice, Oxygen Consumption, Transduction, Genetic, medicine, Animals, Aerobic exercise, Myocyte, Muscle Strength, Muscle, Skeletal, Swimming, Mice, Knockout, Binding Sites, Exercise Tolerance, Myocardium, High Mobility Group Proteins, Skeletal muscle, TFAM, Mitochondria, Muscle, Up-Regulation, Cell biology, DNA-Binding Proteins, Mice, Inbred C57BL, medicine.anatomical_structure, Liver, Mitochondrial biogenesis, Biochemistry, Mutation, RNA Interference, Tumor Suppressor Protein p53, Cardiology and Cardiovascular Medicine, Glycolysis, Muscle Contraction
Abstract

Rationale: Exercise capacity is a physiological characteristic associated with protection from both cardiovascular and all-cause mortality. p53 regulates mitochondrial function and its deletion markedly diminishes exercise capacity, but the underlying genetic mechanism orchestrating this is unclear. Understanding the biology of how p53 improves exercise capacity may provide useful insights for improving both cardiovascular as well as general health. Objective: The purpose of this study was to understand the genetic mechanism by which p53 regulates aerobic exercise capacity. Methods and Results: Using a variety of physiological, metabolic, and molecular techniques, we further characterized maximum exercise capacity and the effects of training, measured various nonmitochondrial and mitochondrial determinants of exercise capacity, and examined putative regulators of mitochondrial biogenesis. As p53 did not affect baseline cardiac function or inotropic reserve, we focused on the involvement of skeletal muscle and now report a wider role for p53 in modulating skeletal muscle mitochondrial function. p53 interacts with Mitochondrial Transcription Factor A ( TFAM ), a nuclear-encoded gene important for mitochondrial DNA (mtDNA) transcription and maintenance, and regulates mtDNA content. The increased mtDNA in p53 +/+ compared to p53 −/− mice was more marked in aerobic versus glycolytic skeletal muscle groups with no significant changes in cardiac tissue. These in vivo observations were further supported by in vitro studies showing overexpression of p53 in mouse myoblasts increases both TFAM and mtDNA levels whereas depletion of TFAM by shRNA decreases mtDNA content. Conclusions: Our current findings indicate that p53 promotes aerobic metabolism and exercise capacity by using different mitochondrial genes and mechanisms in a tissue-specific manner.

Published
2009

49. A pivotal role for p53: balancing aerobic respiration and glycolysis

Author

Paul M. Hwang, Satoaki Matoba, Wenzhe Ma, Ho Joong Sung, and Joon Y. Park

Subjects
Physiology, Cellular respiration, Cell Respiration, Oxidative phosphorylation, Biology, Oxidative Phosphorylation, law.invention, Oxygen Consumption, law, Neoplasms, Animals, Humans, Cytochrome c oxidase, Glycolysis, Mechanism (biology), Cell Biology, Warburg effect, Mitochondria, Cell biology, Biochemistry, Cancer cell, biology.protein, Suppressor, Tumor Suppressor Protein p53, Energy Metabolism
Abstract

The genetic basis of increased glycolytic activity observed in cancer cells is likely to be the result of complex interactions of multiple regulatory pathways. Here we review the recent evidence of a simple genetic mechanism by which tumor suppressor p53 regulates mitochondrial respiration with secondary changes in glycolysis that are reminiscent of the Warburg effect. The biological significance of this regulation of the two major pathways of energy generation by p53 remains to be seen.

Published
2007

50. Low ambient oxygen prevents atherosclerosis

Author

Marcelo Amar, Jichun Chen, Danielle A. Springer, Michele D. Allen, Milton Pryor, Ho Joong Sung, Ping Yuan Wang, Ji-Hoon Park, Jaeyul Kwon, Paul M. Hwang, Alan T. Remaley, Ju Gyeong Kang, and Audrey Noguchi

Subjects
0301 basic medicine, medicine.medical_specialty, medicine.medical_treatment, chemistry.chemical_element, Inflammation, 030204 cardiovascular system & hematology, Altitude Sickness, Oxygen, Article, Cell Line, Pathogenesis, 03 medical and health sciences, Mice, 0302 clinical medicine, Apolipoproteins E, Internal medicine, Drug Discovery, medicine, Animals, Humans, Genetics (clinical), Altitude sickness, Aortic atherosclerosis, Mice, Knockout, Chemistry, Lipid metabolism, Protective Factors, medicine.disease, Atherosclerosis, Hypoxia-Inducible Factor 1, alpha Subunit, Interleukin-10, Up-Regulation, Mice, Inbred C57BL, Interleukin 10, 030104 developmental biology, Cytokine, Endocrinology, Molecular Medicine, Female, medicine.symptom
Abstract

Large population studies have shown that living at higher altitudes, which lowers ambient oxygen exposure, is associated with reduced cardiovascular disease mortality. However, hypoxia has also been reported to promote atherosclerosis by worsening lipid metabolism and inflammation. We sought to address these disparate reports by reducing the ambient oxygen exposure of ApoE-/- mice. We observed that long-term adaptation to 10% O2 (equivalent to oxygen content at ∼5000 m), compared to 21% O2 (room air at sea level), resulted in a marked decrease in aortic atherosclerosis in ApoE-/- mice. This effect was associated with increased expression of the anti-inflammatory cytokine interleukin-10 (IL-10), known to be anti-atherogenic and regulated by hypoxia-inducible transcription factor-1α (HIF-1α). Supporting these observations, ApoE-/- mice that were deficient in IL-10 (IL10-/- ApoE-/- double knockout) failed to show reduced atherosclerosis in 10% oxygen. Our study reveals a specific mechanism that can help explain the decreased prevalence of ischemic heart disease in populations living at high altitudes and identifies ambient oxygen exposure as a potential factor that could be modulated to alter pathogenesis. Key messages: Chronic low ambient oxygen exposure decreases atherosclerosis in mice. Anti-inflammatory cytokine IL-10 levels are increased by low ambient O2. This is consistent with the established role of HIF-1α in IL10 transactivation. Absence of IL-10 results in the loss of the anti-atherosclerosis effect of low O2. This mechanism may contribute to decreased atherosclerosis at high altitudes.

Published
2015

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