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1. Disease characteristics, effectiveness, and safety of vestronidase alfa for the treatment of patients with mucopolysaccharidosis VII in a novel, longitudinal, multicenter disease monitoring program.

Author

Martins, Esmeralda, Martins, Esmeralda, Oussoren, Esmeralda, Hennermann, Julia, Chabrol, Brigitte, Grant, Christina, Sun, Angela, Durand, Consuelo, Hetzer, Joel, Malkus, Betsy, Marsden, Deborah, Merritt Ii, J, Giugliani, Roberto, Gonzalez-Meneses, Antonio, Scarpa, Maurizio, Burton, Barbara, Wang, Raymond, Martins, Esmeralda, Martins, Esmeralda, Oussoren, Esmeralda, Hennermann, Julia, Chabrol, Brigitte, Grant, Christina, Sun, Angela, Durand, Consuelo, Hetzer, Joel, Malkus, Betsy, Marsden, Deborah, Merritt Ii, J, Giugliani, Roberto, Gonzalez-Meneses, Antonio, Scarpa, Maurizio, Burton, Barbara, and Wang, Raymond

Published
2024

3. Enzymatic debranching is a key determinant of the xylan-degrading activity of family AA9 lytic polysaccharide monooxygenases

Author

Tolgo, Monika, Hegnar, Olav A., Larsbrink, Johan, Vilaplana, Francisco, Eijsink, Vincent G. H., Olsson, Lisbeth, Tolgo, Monika, Hegnar, Olav A., Larsbrink, Johan, Vilaplana, Francisco, Eijsink, Vincent G. H., and Olsson, Lisbeth

Abstract

Background Previous studies have revealed that some Auxiliary Activity family 9 (AA9) lytic polysaccharide monooxygenases (LPMOs) oxidize and degrade certain types of xylans when incubated with mixtures of xylan and cellulose. Here, we demonstrate that the xylanolytic activities of two xylan-active LPMOs, TtLPMO9E and TtLPMO9G from Thermothielavioides terrestris, strongly depend on the presence of xylan substitutions. Results Using mixtures of phosphoric acid-swollen cellulose (PASC) and wheat arabinoxylan (WAX), we show that removal of arabinosyl substitutions with a GH62 arabinofuranosidase resulted in better adsorption of xylan to cellulose, and enabled LPMO-catalyzed cleavage of this xylan. Furthermore, experiments with mixtures of PASC and arabinoglucuronoxylan from spruce showed that debranching of xylan with the GH62 arabinofuranosidase and a GH115 glucuronidase promoted LPMO activity. Analyses of mixtures with PASC and (non-arabinosylated) beechwood glucuronoxylan showed that GH115 action promoted LPMO activity also on this xylan. Remarkably, when WAX was incubated with Avicel instead of PASC in the presence of the GH62, both xylan and cellulose degradation by the LPMO9 were impaired, showing that the formation of cellulose-xylan complexes and their susceptibility to LPMO action also depend on the properties of the cellulose. These debranching effects not only relate to modulation of the cellulose-xylan interaction, which influences the conformation and rigidity of the xylan, but likely also affect the LPMO-xylan interaction, because debranching changes the architecture of the xylan surface. Conclusions Our results shed new light on xylanolytic LPMO9 activity and on the functional interplay and possible synergies between the members of complex lignocellulolytic enzyme cocktails. These findings will be relevant for the development of future lignocellulolytic cocktails and biomaterials., QC 20230127

Published
2023
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4. Longevity factor klotho enhances cognition in aged nonhuman primates.

Author

Castner, Stacy, Castner, Stacy, Gupta, Shweta, Wang, Dan, Moreno, Arturo, Chen, Chen, Poon, Yan, Groen, Aaron, Greenberg, Kenneth, David, Nathaniel, Boone, Tom, Baxter, Mark, Williams, Graham, Dubal, Dena, Park, Cana, Castner, Stacy, Castner, Stacy, Gupta, Shweta, Wang, Dan, Moreno, Arturo, Chen, Chen, Poon, Yan, Groen, Aaron, Greenberg, Kenneth, David, Nathaniel, Boone, Tom, Baxter, Mark, Williams, Graham, Dubal, Dena, and Park, Cana

Abstract

Cognitive dysfunction in aging is a major biomedical challenge. Whether treatment with klotho, a longevity factor, could enhance cognition in human-relevant models such as in nonhuman primates is unknown and represents a major knowledge gap in the path to therapeutics. We validated the rhesus form of the klotho protein in mice showing it increased synaptic plasticity and cognition. We then found that a single administration of low-dose, but not high-dose, klotho enhanced memory in aged nonhuman primates. Systemic low-dose klotho treatment may prove therapeutic in aging humans.

Published
2023

5. The Role of Klotho and FGF23 in Cardiovascular Outcomes of Diabetic Patients With Chronic Limb Threatening Ischemia: A Prospective Study

Author

Biscetti, Federico, Rando, Maria Margherita, Cecchini, Andrea Leonardo, Nicolazzi, Maria Anna, Rossini, Enrica, Angelini, Flavia, Iezzi, Roberto, Eraso, Luis H., DiMuzio, Paul J., Pitocco, Dario, Gasbarrini, Antonio, Massetti, Massimo, Flex, Andrea, Biscetti, Federico, Rando, Maria Margherita, Cecchini, Andrea Leonardo, Nicolazzi, Maria Anna, Rossini, Enrica, Angelini, Flavia, Iezzi, Roberto, Eraso, Luis H., DiMuzio, Paul J., Pitocco, Dario, Gasbarrini, Antonio, Massetti, Massimo, and Flex, Andrea

Abstract

Cardiovascular complications after lower extremity revascularization (LER) are common in diabetic patients with peripheral arterial disease (PAD) and chronic limb threatening ischemia (CLTI). The Klotho-fibroblast growth factor 23 (FGF23) axis is associated with endothelial injury and cardiovascular risk. We aimed to analyze the relationship between Klotho and FGF23 serum levels and the incidence of major adverse cardiovascular events (MACE) and major adverse limb events (MALE) after LER in diabetic patients with PAD and CLTI. Baseline levels of Klotho and FGF23, and their association with subsequent incidence of MACE and MALE were analyzed in a prospective, non-randomized study in a population of diabetic patients with PAD and CLTI requiring LER. A total of 220 patients were followed for 12 months after LER. Sixty-three MACE and 122 MALE were recorded during follow-up period. Baseline lower Klotho serum levels (295.3 ± 151.3 pg/mL vs. 446.4 ± 171.7 pg/mL, p < 0.01), whereas increased serum levels FGF23 (75.0 ± 11.8 pg/mL vs. 53.2 ± 15.4 pg/mL, p < 0.01) were significantly associated with the development of MACE. Receiver operating characteristic (ROC) analysis confirmed the predictive power of Klotho and FGF23 baseline levels. Furthermore, decreased Klotho levels were associated with the occurrence of MALE after LER (329.1 ± 136.8 pg/mL vs 495.4 ± 183.9 pg/mL, p < 0.01). We found that Klotho and FGF23 baseline levels are a potential biomarker for increased cardiovascular risk after LER in diabetic patients with PAD and CLTI.

Published
2023

6. KL1 Domain of Longevity Factor Klotho Mimics the Metabolome of Cognitive Stimulation and Enhances Cognition in Young and Aging Mice

Author

Gupta, Shweta, Gupta, Shweta, Moreno, Arturo J, Wang, Dan, Leon, Julio, Chen, Chen, Hahn, Oliver, Poon, Yan, Greenberg, Kenneth, David, Nathaniel, Wyss-Coray, Tony, Raftery, Daniel, Promislow, Daniel EL, Dubal, Dena B, Gupta, Shweta, Gupta, Shweta, Moreno, Arturo J, Wang, Dan, Leon, Julio, Chen, Chen, Hahn, Oliver, Poon, Yan, Greenberg, Kenneth, David, Nathaniel, Wyss-Coray, Tony, Raftery, Daniel, Promislow, Daniel EL, and Dubal, Dena B

Published
2022

7. Dihydroartemisinin suppresses renal fibrosis in mice by inhibiting DNA-methyltransferase 1 and increasing Klotho.

Author

Zhou, Wei, Zhou, Wei, Chen, Min-Min, Liu, Hui-Ling, Si, Zi-Lin, Wu, Wen-Hui, Jiang, Hong, Wang, Lin-Xiao, An, Xiao-Fei, Su, Ke, Chen, Cheng, Tan, Ning-Hua, Zhang, Zhi-Hao, Vaziri, Nosratola, Zhou, Wei, Zhou, Wei, Chen, Min-Min, Liu, Hui-Ling, Si, Zi-Lin, Wu, Wen-Hui, Jiang, Hong, Wang, Lin-Xiao, An, Xiao-Fei, Su, Ke, Chen, Cheng, Tan, Ning-Hua, Zhang, Zhi-Hao, and Vaziri, Nosratola

Published
2022

8. Microbial enzymes induce colitis by reactivating triclosan in the mouse gastrointestinal tract.

Author

Zhang, Jianan, Zhang, Jianan, Walker, Morgan, Sanidad, Katherine, Zhang, Hongna, Liang, Yanshan, Zhao, Ermin, Chacon-Vargas, Katherine, Yeliseyev, Vladimir, Parsonnet, Julie, Haggerty, Thomas, Wang, Guangqiang, Simpson, Joshua, Jariwala, Parth, Beaty, Violet, Yang, Jun, Yang, Haixia, Panigrahy, Anand, Minter, Lisa, Kim, Daeyoung, Gibbons, John, Liu, LinShu, Li, Zhengze, Xiao, Hang, Borlandelli, Valentina, Overkleeft, Hermen, Cloer, Erica, Major, Michael, Goldfarb, Dennis, Cai, Zongwei, Redinbo, Matthew, Zhang, Guodong, Zhang, Jianan, Zhang, Jianan, Walker, Morgan, Sanidad, Katherine, Zhang, Hongna, Liang, Yanshan, Zhao, Ermin, Chacon-Vargas, Katherine, Yeliseyev, Vladimir, Parsonnet, Julie, Haggerty, Thomas, Wang, Guangqiang, Simpson, Joshua, Jariwala, Parth, Beaty, Violet, Yang, Jun, Yang, Haixia, Panigrahy, Anand, Minter, Lisa, Kim, Daeyoung, Gibbons, John, Liu, LinShu, Li, Zhengze, Xiao, Hang, Borlandelli, Valentina, Overkleeft, Hermen, Cloer, Erica, Major, Michael, Goldfarb, Dennis, Cai, Zongwei, Redinbo, Matthew, and Zhang, Guodong

Published
2022

9. Circulating Klotho Is Higher in Cerebrospinal Fluid than Serum and Elevated Among KLOTHO Heterozygotes in a Cohort with Risk for Alzheimer's Disease.

Author

Gaitán, Julian M, Gaitán, Julian M, Asthana, Sanjay, Carlsson, Cynthia M, Engelman, Corinne D, Johnson, Sterling C, Sager, Mark A, Wang, Dan, Dubal, Dena B, Okonkwo, Ozioma C, Gaitán, Julian M, Gaitán, Julian M, Asthana, Sanjay, Carlsson, Cynthia M, Engelman, Corinne D, Johnson, Sterling C, Sager, Mark A, Wang, Dan, Dubal, Dena B, and Okonkwo, Ozioma C

Abstract

BackgroundKlotho is a longevity and neuroprotective hormone encoded by the KLOTHO gene, and heterozygosity for the KL-VS variant confers a protective effect against neurodegenerative disease.ObjectiveTest whether klotho concentrations in serum or cerebrospinal fluid (CSF) vary as a function of KLOTHO KL-VS genotype, determine whether circulating klotho concentrations from serum and CSF differ from one another, and evaluate whether klotho levels are associated with Alzheimer's disease risk factors.MethodsCirculating klotho was measured in serum (n = 1,116) and CSF (n = 183) of cognitively intact participants (aged 62.4 ± 6.5 years; 69.5% female). KLOTHO KL-VS zygosity (non-carrier; heterozygote; homozygote) was also determined. Linear regression was used to test whether klotho hormone concentration varied as a function of KL-VS genotype, specimen source, and demographic and clinical characteristics.ResultsSerum and CSF klotho were higher in KL-VS carriers than non-carriers. Klotho concentration was higher in CSF than in serum. Females had higher serum and CSF klotho, while younger age was associated with higher klotho in CSF.ConclusionIn a cohort enriched for risk for Alzheimer's disease, heterozygotic and homozygotic carriers of the KL-VS allele, females, and younger individuals have higher circulating klotho. Fluid source, KL-VS genotype, age, and sex should be considered in analyses of circulating klotho on brain health.

Published
2022

10. KL-VS heterozygosity is associated with lower amyloid-dependent tau accumulation and memory impairment in Alzheimer's disease.

Author

Neitzel, Julia, Neitzel, Julia, Franzmeier, Nicolai, Rubinski, Anna, Dichgans, Martin, Brendel, Matthias, Alzheimer’s Disease Neuroimaging Initiative (ADNI), Malik, Rainer, Ewers, Michael, Neitzel, Julia, Neitzel, Julia, Franzmeier, Nicolai, Rubinski, Anna, Dichgans, Martin, Brendel, Matthias, Alzheimer’s Disease Neuroimaging Initiative (ADNI), Malik, Rainer, and Ewers, Michael

Abstract

Klotho-VS heterozygosity (KL-VShet) is associated with reduced risk of Alzheimer's disease (AD). However, whether KL-VShet is associated with lower levels of pathologic tau, i.e., the key AD pathology driving neurodegeneration and cognitive decline, is unknown. Here, we assessed the interaction between KL-VShet and levels of beta-amyloid, a key driver of tau pathology, on the levels of PET-assessed neurofibrillary tau in 551 controls and patients across the AD continuum. KL-VShet showed lower cross-sectional and longitudinal increase in tau-PET per unit increase in amyloid-PET when compared to that of non-carriers. This association of KL-VShet on tau-PET was stronger in Klotho mRNA-expressing brain regions mapped onto a gene expression atlas. KL-VShet was related to better memory functions in amyloid-positive participants and this association was mediated by lower tau-PET. Amyloid-PET levels did not differ between KL-VShet carriers versus non-carriers. Together, our findings provide evidence to suggest a protective role of KL-VShet against amyloid-related tau pathology and tau-related memory impairments in elderly humans at risk of AD dementia.

Published
2021

11. KL-VS heterozygosity is associated with lower amyloid-dependent tau accumulation and memory impairment in Alzheimer's disease.

Author

Neitzel, Julia, Neitzel, Julia, Franzmeier, Nicolai, Rubinski, Anna, Dichgans, Martin, Brendel, Matthias, Alzheimer’s Disease Neuroimaging Initiative (ADNI), Malik, Rainer, Ewers, Michael, Neitzel, Julia, Neitzel, Julia, Franzmeier, Nicolai, Rubinski, Anna, Dichgans, Martin, Brendel, Matthias, Alzheimer’s Disease Neuroimaging Initiative (ADNI), Malik, Rainer, and Ewers, Michael

Abstract

Klotho-VS heterozygosity (KL-VShet) is associated with reduced risk of Alzheimer's disease (AD). However, whether KL-VShet is associated with lower levels of pathologic tau, i.e., the key AD pathology driving neurodegeneration and cognitive decline, is unknown. Here, we assessed the interaction between KL-VShet and levels of beta-amyloid, a key driver of tau pathology, on the levels of PET-assessed neurofibrillary tau in 551 controls and patients across the AD continuum. KL-VShet showed lower cross-sectional and longitudinal increase in tau-PET per unit increase in amyloid-PET when compared to that of non-carriers. This association of KL-VShet on tau-PET was stronger in Klotho mRNA-expressing brain regions mapped onto a gene expression atlas. KL-VShet was related to better memory functions in amyloid-positive participants and this association was mediated by lower tau-PET. Amyloid-PET levels did not differ between KL-VShet carriers versus non-carriers. Together, our findings provide evidence to suggest a protective role of KL-VShet against amyloid-related tau pathology and tau-related memory impairments in elderly humans at risk of AD dementia.

Published
2021

12. Gain-of-function of the 1-aminocyclopropane-1-carboxylate synthase gene ACS1G induces female flower development in cucumber gynoecy.

Author

Zhang, Huimin, Zhang, Huimin, Li, Shuai, Yang, Li, Cai, Guanghua, Chen, Huiming, Gao, Dongli, Lin, Tao, Cui, Qingzhi, Wang, Donghui, Li, Zheng, Cai, Run, Bai, Shunong, Lucas, William J, Huang, Sanwen, Zhang, Zhonghua, Sun, Jinjing, Zhang, Huimin, Zhang, Huimin, Li, Shuai, Yang, Li, Cai, Guanghua, Chen, Huiming, Gao, Dongli, Lin, Tao, Cui, Qingzhi, Wang, Donghui, Li, Zheng, Cai, Run, Bai, Shunong, Lucas, William J, Huang, Sanwen, Zhang, Zhonghua, and Sun, Jinjing

Abstract

Unisexual flowers provide a useful system for studying plant sex determination. In cucumber (Cucumis sativus L.), three major Mendelian loci control unisexual flower development, Female (F), androecious [a; 1-aminocyclopropane-1-carboxylate {ACC} synthase 11, acs11], and Monoecious (M; ACS2), referred to here as the Female, Androecious, Monoecious (FAM) model, in combination with two genes, gynoecious (g, the WIP family C2H2 zinc finger transcription factor gene WIP1) and the ethylene biosynthetic gene ACC oxidase 2 (ACO2). The F locus, conferring gynoecy and the potential for increasing fruit yield, is defined by a 30.2-kb tandem duplication containing three genes. However, the gene that determines the Female phenotype, and its mechanism, remains unknown. Here, we created a set of mutants and revealed that ACS1G is responsible for gynoecy conferred by the F locus. The duplication resulted in ACS1G acquiring a new promoter and expression pattern; in plants carrying the F locus duplication, ACS1G is expressed early in floral bud development, where it functions with ACO2 to generate an ethylene burst. The resulting ethylene represses WIP1 and activates ACS2 to initiate gynoecy. This early ACS1G expression bypasses the need for ACS11 to produce ethylene, thereby establishing a dominant pathway for female floral development. Based on these findings, we propose a model for how these ethylene biosynthesis genes cooperate to control unisexual flower development in cucumber.

Published
2021

15. Biomarkers of vascular disease in diabetes: the adipose-immune system cross talk

Author

Biscetti, Federico, Nardella, Elisabetta, Cecchini, Andrea Leonardo, Flex, Andrea, Landolfi, Raffaele, Biscetti F. (ORCID:0000-0001-7449-657X), Nardella E., Cecchini A. L., Flex A. (ORCID:0000-0003-2664-4165), Landolfi R. (ORCID:0000-0002-7913-8576), Biscetti, Federico, Nardella, Elisabetta, Cecchini, Andrea Leonardo, Flex, Andrea, Landolfi, Raffaele, Biscetti F. (ORCID:0000-0001-7449-657X), Nardella E., Cecchini A. L., Flex A. (ORCID:0000-0003-2664-4165), and Landolfi R. (ORCID:0000-0002-7913-8576)

Abstract

Experimental and clinical studies aimed at investigating the mechanism(s) underlying vascular complications of diabetes indicate that a great number of molecules are involved in the pathogenesis of these complications. Most of these molecules are inflammatory mediators or markers generated by immune or adipose tissue. Some of them, i.e. resistin and sortilin, have been shown to be involved in the cross talk between adipocytes and inflammatory cells. This interaction is an attractive area of research, particularly in type 2 diabetes and obesity. Other proteins, such as adiponectin and visfatin, appear to be more promising as possible vascular markers. In addition, some molecules involved in calcium/phosphorus metabolism, such as klotho and FGF23, have an involvement in the pathogenesis of diabetic vasculopathy, which appears to be dependent on the degree of vascular impairment. Inflammatory markers are a promising tool for treatment decisions while measuring plasma levels of adipokines, sortilin, Klotho and FGF23 in adequately sized longitudinal studies is expected to allow a more precise characterization of diabetic vascular disease and the optimal use of personalized treatment strategies.

Published
2020

16. Coupled Enzymatic Treatment and Mass Spectrometric Analysis for Identification of Glucuronidated Metabolites in Human Samples

Author

Correia, Mario S. P., Rao, Menghua, Ballet, Caroline, Globisch, Daniel, Correia, Mario S. P., Rao, Menghua, Ballet, Caroline, and Globisch, Daniel

Abstract

Glucuronidation is the most common phase II modification and plays an important role in human clearance metabolism. Glucuronidated metabolites have also been linked to disease development and microbiota-host co-metabolism. Although many of these compounds have been identified, the total number of unknown glucuronides and their impact on the human host's physiology can only be estimated. Herein, we describe the combination of an untargeted metabolomics analysis and enzymatic metabolic conversion for the selective detection of glucuronide conjugates by using UPLC-MS/MS in human urine samples. Our study demonstrates that this powerful strategy can be used for the selective identification of glucuronidated molecules and to discover unknown natural metabolites. In total, we identified 191 metabolites in a single sample including microbiota-derived compounds as well as previously unidentified molecules.

Published
2019
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17. Plasma Klotho and Frailty in Older Adults: Findings From the InCHIANTI Study.

Author

Shardell, Michelle, Shardell, Michelle, Semba, Richard D, Kalyani, Rita R, Bandinelli, Stefania, Prather, Aric A, Chia, Chee W, Ferrucci, Luigi, Shardell, Michelle, Shardell, Michelle, Semba, Richard D, Kalyani, Rita R, Bandinelli, Stefania, Prather, Aric A, Chia, Chee W, and Ferrucci, Luigi

Abstract

BackgroundThe hormone klotho, encoded by the gene klotho, is primarily expressed in the kidney and choroid plexus of the brain. Higher klotho concentrations have been linked to better physical performance; however, it is unknown whether klotho relates to frailty status in older adults.MethodsPlasma klotho was measured in 774 participants aged ≥65 years enrolled in InCHIANTI, a prospective cohort study comprising Italian adults. Frailty status was assessed at 3 and 6 years after enrollment. Frailty was defined as presence of at least three out of five criteria of unintentional weight loss, exhaustion, sedentariness, muscle weakness, and slow walking speed; prefrailty was defined as presence of one or two criteria; and robustness was defined as zero criteria. We assessed whether plasma klotho concentrations measured at the 3-year visit related to frailty.ResultsEach additional natural logarithm of klotho (pg/mL) was associated with lower odds of frailty versus robustness after adjustment for covariates (odds ratio [OR] 0.46; 95% confidence interval 0.21, 0.98; p-value = .045). Higher klotho was particularly associated with lower odds of exhaustion (OR 0.57; 95% CI 0.36, 0.89; p-value = .014). Participants with higher klotho also had lower estimated odds of weight loss and weakness, but these findings were not statistically significant.ConclusionsHigher plasma klotho concentrations were associated with lower likelihoods of frailty and particularly exhaustion. Future studies should investigate modifiable mechanisms through which klotho may affect the frailty syndrome.

Published
2019

18. CTC clusters induced by heparanase enhance breast cancer metastasis.

Author

Wei, Rong-Rui, Wei, Rong-Rui, Sun, Dan-Ni, Yang, Hong, Yan, Juan, Zhang, Xiong, Zheng, Xing-Ling, Fu, Xu-Hong, Geng, Mei-Yu, Huang, Xun, Ding, Jian, Wei, Rong-Rui, Wei, Rong-Rui, Sun, Dan-Ni, Yang, Hong, Yan, Juan, Zhang, Xiong, Zheng, Xing-Ling, Fu, Xu-Hong, Geng, Mei-Yu, Huang, Xun, and Ding, Jian

Abstract

Aggregated metastatic cancer cells, referred to as circulating tumor cell (CTC) clusters, are present in the blood of cancer patients and contribute to cancer metastasis. However, the origin of CTC clusters, especially intravascular aggregates, remains unknown. Here, we employ suspension culture methods to mimic CTC cluster formation in the circulation of breast cancer patients. CTC clusters generated using these methods exhibited an increased metastatic potential that was defined by the overexpression of heparanase (HPSE). Heparanase induced FAK- and ICAM-1-dependent cell adhesion, which promoted intravascular cell aggregation. Moreover, knockdown of heparanase or inhibition of its activity with JG6, a heparanase inhibitor, was sufficient to block the formation of cell clusters and suppress breast cancer metastasis. Our data reveal that heparanase-mediated cell adhesion is critical for metastasis mediated by intravascular CTC clusters. We also suggest that targeting the function of heparanase in cancer cell dissemination might limit metastatic progression.

Published
2018

19. Klotho controls the brain-immune system interface in the choroid plexus.

Author

Zhu, Lei, Zhu, Lei, Stein, Liana R, Kim, Daniel, Ho, Kaitlyn, Yu, Gui-Qiu, Zhan, Lihong, Larsson, Tobias E, Mucke, Lennart, Zhu, Lei, Zhu, Lei, Stein, Liana R, Kim, Daniel, Ho, Kaitlyn, Yu, Gui-Qiu, Zhan, Lihong, Larsson, Tobias E, and Mucke, Lennart

Abstract

Located within the brain's ventricles, the choroid plexus produces cerebrospinal fluid and forms an important barrier between the central nervous system and the blood. For unknown reasons, the choroid plexus produces high levels of the protein klotho. Here, we show that these levels naturally decline with aging. Depleting klotho selectively from the choroid plexus via targeted viral vector-induced knockout in Klotho flox/flox mice increased the expression of multiple proinflammatory factors and triggered macrophage infiltration of this structure in young mice, simulating changes in unmanipulated old mice. Wild-type mice infected with the same Cre recombinase-expressing virus did not show such alterations. Experimental depletion of klotho from the choroid plexus enhanced microglial activation in the hippocampus after peripheral injection of mice with lipopolysaccharide. In primary cultures, klotho suppressed thioredoxin-interacting protein-dependent activation of the NLRP3 inflammasome in macrophages by enhancing fibroblast growth factor 23 signaling. We conclude that klotho functions as a gatekeeper at the interface between the brain and immune system in the choroid plexus. Klotho depletion in aging or disease may weaken this barrier and promote immune-mediated neuropathogenesis.

Published
2018

20. Klotho controls the brain-immune system interface in the choroid plexus.

Author

Zhu, Lei, Zhu, Lei, Stein, Liana R, Kim, Daniel, Ho, Kaitlyn, Yu, Gui-Qiu, Zhan, Lihong, Larsson, Tobias E, Mucke, Lennart, Zhu, Lei, Zhu, Lei, Stein, Liana R, Kim, Daniel, Ho, Kaitlyn, Yu, Gui-Qiu, Zhan, Lihong, Larsson, Tobias E, and Mucke, Lennart

Abstract

Located within the brain's ventricles, the choroid plexus produces cerebrospinal fluid and forms an important barrier between the central nervous system and the blood. For unknown reasons, the choroid plexus produces high levels of the protein klotho. Here, we show that these levels naturally decline with aging. Depleting klotho selectively from the choroid plexus via targeted viral vector-induced knockout in Klotho flox/flox mice increased the expression of multiple proinflammatory factors and triggered macrophage infiltration of this structure in young mice, simulating changes in unmanipulated old mice. Wild-type mice infected with the same Cre recombinase-expressing virus did not show such alterations. Experimental depletion of klotho from the choroid plexus enhanced microglial activation in the hippocampus after peripheral injection of mice with lipopolysaccharide. In primary cultures, klotho suppressed thioredoxin-interacting protein-dependent activation of the NLRP3 inflammasome in macrophages by enhancing fibroblast growth factor 23 signaling. We conclude that klotho functions as a gatekeeper at the interface between the brain and immune system in the choroid plexus. Klotho depletion in aging or disease may weaken this barrier and promote immune-mediated neuropathogenesis.

Published
2018

21. Cord blood klotho levels are inversely associated with leptin in healthy Latino neonates at risk for obesity.

Author

Wojcicki, Janet M, Wojcicki, Janet M, Prather, Aric A, Epel, Elissa, Wang, Dan, Dubal, Dena B, Wojcicki, Janet M, Wojcicki, Janet M, Prather, Aric A, Epel, Elissa, Wang, Dan, and Dubal, Dena B

Abstract

BackgroundKlotho serum levels reflect nutritional state in adults including obesity and anorexia. The relationship between cord blood klotho levels at birth and parameters of growth including anthropometrics are not known.MethodsWe evaluated the relationship between cord blood klotho, leptin and adipocyte hormones and infant, child and maternal anthropometrics and maternal depression in a cohort of 73 children. Non-parametric tests were used to assess differences between dichotomous and categorical predictors and klotho levels and Spearman's rank coefficients were used to assess the relationship between klotho levels and continuous predictors. A multivariable log transformed linear regression model was used to test for independent predictors of serum klotho levels.ResultsMean klotho levels were 2864.9±1409.7 (pg/mL) in cord blood and we found no relationship with infant sex, delivery specifics including gestational age or anthropometrics at birth. There was similarly no association between klotho levels at birth and future obesity at age 2. Leptin levels at birth were inversely associated with klotho levels in multivariable models after adjusting for other covariates (p<0.01). Similarly, in multivariable models insulin levels were inversely correlated with klotho levels (p=0.03). Leptin levels in our cohort of at-risk infants were more than 50% higher than other studies with neonates.ConclusionsWe found no associations between weight or length at birth or obesity in early childhood and cord blood klotho levels. Cord blood klotho levels were inversely correlated with leptin and insulin levels at birth and should be further investigated to better understand the inter-relationship between this hormone and key regulators of growth and adiposity.

Published
2018

23. Systemic klotho is associated with KLOTHO variation and predicts intrinsic cortical connectivity in healthy human aging.

Author

Yokoyama, Jennifer S, Yokoyama, Jennifer S, Marx, Gabe, Brown, Jesse A, Bonham, Luke W, Wang, Dan, Coppola, Giovanni, Seeley, William W, Rosen, Howard J, Miller, Bruce L, Kramer, Joel H, Dubal, Dena B, Yokoyama, Jennifer S, Yokoyama, Jennifer S, Marx, Gabe, Brown, Jesse A, Bonham, Luke W, Wang, Dan, Coppola, Giovanni, Seeley, William W, Rosen, Howard J, Miller, Bruce L, Kramer, Joel H, and Dubal, Dena B

Abstract

Cognitive decline is a major biomedical challenge as the global population ages. Elevated levels of the longevity factor klotho suppress aging, enhance cognition, and promote synaptic plasticity and neural resilience against aging and Alzheimer's disease (AD)-related pathogenic proteins. Here, we examined the relationship between human genetic variants of KLOTHO and systemic klotho levels - and assessed neuroanatomic correlates of serum klotho in a cohort of healthy older adults. Serum klotho levels were increased with KL-VS heterozygosity, as anticipated. We report, for the first time, that serum klotho levels were paradoxically decreased with KL-VS homozygosity. Further, we found that higher serum klotho levels were associated with measures of greater intrinsic connectivity in key functional networks of the brain vulnerable to aging and AD such as the fronto-parietal and default mode networks. Our findings suggest that elevated klotho promotes a resilient brain, possibly through increased network connectivity of critical brain regions.

Published
2017

24. Peripheral Elevation of a Klotho Fragment Enhances Brain Function and Resilience in Young, Aging, and α-Synuclein Transgenic Mice.

Author

Leon, Julio, Leon, Julio, Moreno, Arturo J, Garay, Bayardo I, Chalkley, Robert J, Burlingame, Alma L, Wang, Dan, Dubal, Dena B, Leon, Julio, Leon, Julio, Moreno, Arturo J, Garay, Bayardo I, Chalkley, Robert J, Burlingame, Alma L, Wang, Dan, and Dubal, Dena B

Abstract

Cognitive dysfunction and decreased mobility from aging and neurodegenerative conditions, such as Parkinson and Alzheimer diseases, are major biomedical challenges in need of more effective therapies. Increasing brain resilience may represent a new treatment strategy. Klotho, a longevity factor, enhances cognition when genetically and broadly overexpressed in its full, wild-type form over the mouse lifespan. Whether acute klotho treatment can rapidly enhance cognitive and motor functions or induce resilience is a gap in our knowledge of its therapeutic potential. Here, we show that an α-klotho protein fragment (αKL-F), administered peripherally, surprisingly induced cognitive enhancement and neural resilience despite impermeability to the blood-brain barrier in young, aging, and transgenic α-synuclein mice. αKL-F treatment induced cleavage of the NMDAR subunit GluN2B and also enhanced NMDAR-dependent synaptic plasticity. GluN2B blockade abolished αKL-F-mediated effects. Peripheral αKL-F treatment is sufficient to induce neural enhancement and resilience in mice and may prove therapeutic in humans.

Published
2017

25. Systemic klotho is associated with KLOTHO variation and predicts intrinsic cortical connectivity in healthy human aging.

Author

Yokoyama, Jennifer S, Yokoyama, Jennifer S, Marx, Gabe, Brown, Jesse A, Bonham, Luke W, Wang, Dan, Coppola, Giovanni, Seeley, William W, Rosen, Howard J, Miller, Bruce L, Kramer, Joel H, Dubal, Dena B, Yokoyama, Jennifer S, Yokoyama, Jennifer S, Marx, Gabe, Brown, Jesse A, Bonham, Luke W, Wang, Dan, Coppola, Giovanni, Seeley, William W, Rosen, Howard J, Miller, Bruce L, Kramer, Joel H, and Dubal, Dena B

Abstract

Cognitive decline is a major biomedical challenge as the global population ages. Elevated levels of the longevity factor klotho suppress aging, enhance cognition, and promote synaptic plasticity and neural resilience against aging and Alzheimer's disease (AD)-related pathogenic proteins. Here, we examined the relationship between human genetic variants of KLOTHO and systemic klotho levels - and assessed neuroanatomic correlates of serum klotho in a cohort of healthy older adults. Serum klotho levels were increased with KL-VS heterozygosity, as anticipated. We report, for the first time, that serum klotho levels were paradoxically decreased with KL-VS homozygosity. Further, we found that higher serum klotho levels were associated with measures of greater intrinsic connectivity in key functional networks of the brain vulnerable to aging and AD such as the fronto-parietal and default mode networks. Our findings suggest that elevated klotho promotes a resilient brain, possibly through increased network connectivity of critical brain regions.

Published
2017

26. Heparan Sulfate Glycosaminoglycans in Glioblastoma Promote Tumor Invasion.

Author

Tran, Vy M, Tran, Vy M, Wade, Anna, McKinney, Andrew, Chen, Katharine, Lindberg, Olle R, Engler, Jane R, Persson, Anders I, Phillips, Joanna J, Tran, Vy M, Tran, Vy M, Wade, Anna, McKinney, Andrew, Chen, Katharine, Lindberg, Olle R, Engler, Jane R, Persson, Anders I, and Phillips, Joanna J

Abstract

Glioblastoma (GBM) is the most common primary malignant brain tumor of adults and confers a poor prognosis due, in part, to diffuse invasion of tumor cells. Heparan sulfate (HS) glycosaminoglycans, present on the cell surface and in the extracellular matrix, regulate cell signaling pathways and cell-microenvironment interactions. In GBM, the expression of HS glycosaminoglycans and the enzymes that regulate their function are altered, but the actual HS content and structure are unknown. However, inhibition of HS glycosaminoglycan function is emerging as a promising therapeutic strategy for some cancers. In this study, we use liquid chromatography-mass spectrometry analysis to demonstrate differences in HS disaccharide content and structure across four patient-derived tumorsphere lines (GBM1, 5, 6, 43) and between two murine tumorsphere lines derived from murine GBM with enrichment of mesenchymal and proneural gene expression (mMES and mPN, respectively) markers. In GBM, the heterogeneous HS content and structure across patient-derived tumorsphere lines suggested diverse functions in the GBM tumor microenvironment. In GBM5 and mPN, elevated expression of sulfatase 2 (SULF2), an extracellular enzyme that alters ligand binding to HS, was associated with low trisulfated HS disaccharides, a substrate of SULF2. In contrast, other primary tumorsphere lines had elevated expression of the HS-modifying enzyme heparanase (HPSE). Using gene editing strategies to inhibit HPSE, a role for HPSE in promoting tumor cell adhesion and invasion was identified. These studies characterize the heterogeneity in HS glycosaminoglycan content and structure across GBM and reveal their role in tumor cell invasion.Implications: HS-interacting factors promote GBM invasion and are potential therapeutic targets. Mol Cancer Res; 15(11); 1623-33. ©2017 AACR.

Published
2017

27. Transformation of plant isoflavones into bioactive isoflavones by lactic acid bacteria and bifidobacteria

Author

Peirotén, Ángela [0000-0002-1532-8530], Landete, José María [0000-0002-5147-3989], Gaya Sicilia, María Pilar, Peirotén, Ángela, Landete, José María, Peirotén, Ángela [0000-0002-1532-8530], Landete, José María [0000-0002-5147-3989], Gaya Sicilia, María Pilar, Peirotén, Ángela, and Landete, José María

Abstract

Isoflavones are usually found in nature in their glycosilated or methylated forms, and should be hydrolysed to become bioavailable and physiologically active. The deglycosylation of isoflavone C-glycosides and O-glycosides and the demethylase activity were studied in a selection of lactic acid bacteria (LAB) and bifidobacteria by assessing the degree of transformation of the pure precursor compounds, daidzin, genistin, puerarin, formononetin and biochanin A into daidzein or genistein. Only one Bifidobacterium strain and two Enterococcus strains hydrolysed the C-glycosidic bond of puerarin, while deglycosylation of O-glycosides daidzin and genistin was observed in all the tested strains. Demethylation of biochanin A and formononetin was observed in the most of LAB and bifidobacteria. Besides, the subsequent metabolites dihydrodaidzein and dihydrogenistein where produced by many of the strains via daidzein and genistein. In this work, we show the potential of LAB and bifidobacteria as part of functional foods because of their ability to transform plant isoflavones into their bioactive forms. © 2017 Elsevier Ltd

Published
2017

28. Inhibition of Age-Related Therapy Resistance in Melanoma by Rosiglitazone-Mediated Induction of Klotho.

Author

Behera, Reeti, Kaur, Amanpreet, Webster, Marie R., Kim, Suyeon, Ndoye, Abibatou, Kugel, Curtis H., Alicea, Gretchen M., Wang, Joshua, Ghosh, Kanad, Cheng, Phil, Lisanti, Sofia, Marchbank, Katie, Dang, Vanessa, Levesque, Mitchell, Dummer, Reinhard, Xu, Xiaowei, Herlyn, Meenhard, Aplin, Andrew E., Roesch, Alexander, Caino, Cecilia, Altieri, Dario C., Weeraratna, Ashani T., Behera, Reeti, Kaur, Amanpreet, Webster, Marie R., Kim, Suyeon, Ndoye, Abibatou, Kugel, Curtis H., Alicea, Gretchen M., Wang, Joshua, Ghosh, Kanad, Cheng, Phil, Lisanti, Sofia, Marchbank, Katie, Dang, Vanessa, Levesque, Mitchell, Dummer, Reinhard, Xu, Xiaowei, Herlyn, Meenhard, Aplin, Andrew E., Roesch, Alexander, Caino, Cecilia, Altieri, Dario C., and Weeraratna, Ashani T.

Abstract

Purpose: Aging is a poor prognostic factor for melanoma. We have shown that melanoma cells in an aged microenvironment are more resistant to targeted therapy than identical cells in a young microenvironment. This is dependent on age-related secreted factors. Klotho is an age-related protein whose serum levels decrease dramatically by age 40. Most studies on klotho in cancer have focused on the expression of klotho in the tumor cell. We have shown that exogenous klotho inhibits internalization and signaling of Wnt5A, which drives melanoma metastasis and resistance to targeted therapy. We investigate here whether increasing klotho in the aged microenvironment could be an effective strategy for the treatment of melanoma. Experimental Design: PPARg increases klotho levels and is increased by glitazones. Using rosiglitazone, we queried the effects of rosiglitazone on Klotho/Wnt5A cross-talk, in vitro and in vivo, and the implications of that for targeted therapy in young versus aged animals. Results: We show that rosiglitazone increases klotho and decreases Wnt5A in tumor cells, reducing the burden of both BRAF inhibitor-sensitive and BRAF inhibitor-resistant tumors in aged, but not young mice. However, when used in combination with PLX4720, tumor burden was reduced in both young and aged mice, even in resistant tumors. Conclusions: Using glitazones as adjuvant therapy for melanoma may provide a new treatment strategy for older melanoma patients who have developed resistance to vemurafenib. As klotho has been shown to play a role in other cancers too, our results may have wide relevance for multiple tumor types. ©2017 AACR.

Published
2017

29. Klotho gene silencing promotes pathology in the mdx mouse model of Duchenne muscular dystrophy

Author

Wehling-Henricks, Michelle, Wehling-Henricks, Michelle, Li, Zhenzhi, Lindsey, Catherine, Wang, Ying, Welc, Steven S, Ramos, Julian N, Khanlou, Négar, Kuro-o, Makoto, Tidball, James G, Wehling-Henricks, Michelle, Wehling-Henricks, Michelle, Li, Zhenzhi, Lindsey, Catherine, Wang, Ying, Welc, Steven S, Ramos, Julian N, Khanlou, Négar, Kuro-o, Makoto, and Tidball, James G

Published
2016

30. Clinical course of sly syndrome (mucopolysaccharidosis type VII)

Author

Montaño, Adriana M, Montaño, Adriana M, Lock-Hock, Ngu, Steiner, Robert D, Graham, Brett H, Szlago, Marina, Greenstein, Robert, Pineda, Mercedes, Gonzalez-Meneses, Antonio, Çoker, Mahmut, Bartholomew, Dennis, Sands, Mark S, Wang, Raymond, Giugliani, Roberto, Macaya, Alfons, Pastores, Gregory, Ketko, Anastasia K, Ezgü, Fatih, Tanaka, Akemi, Arash, Laila, Beck, Michael, Falk, Rena E, Bhattacharya, Kaustuv, Franco, José, White, Klane K, Mitchell, Grant A, Cimbalistiene, Loreta, Holtz, Max, Sly, William S, Montaño, Adriana M, Montaño, Adriana M, Lock-Hock, Ngu, Steiner, Robert D, Graham, Brett H, Szlago, Marina, Greenstein, Robert, Pineda, Mercedes, Gonzalez-Meneses, Antonio, Çoker, Mahmut, Bartholomew, Dennis, Sands, Mark S, Wang, Raymond, Giugliani, Roberto, Macaya, Alfons, Pastores, Gregory, Ketko, Anastasia K, Ezgü, Fatih, Tanaka, Akemi, Arash, Laila, Beck, Michael, Falk, Rena E, Bhattacharya, Kaustuv, Franco, José, White, Klane K, Mitchell, Grant A, Cimbalistiene, Loreta, Holtz, Max, and Sly, William S

Published
2016

31. Association of Serum Klotho with Loss of Bone Mineral Density and Fracture Risk in Older Adults.

Author

Chalhoub, Didier, Chalhoub, Didier, Marques, Elisa, Meirelles, Osorio, Semba, Richard D, Ferrucci, Luigi, Satterfield, Suzanne, Nevitt, Michael, Cauley, Jane A, Harris, Tamara, Health ABC Study, Chalhoub, Didier, Chalhoub, Didier, Marques, Elisa, Meirelles, Osorio, Semba, Richard D, Ferrucci, Luigi, Satterfield, Suzanne, Nevitt, Michael, Cauley, Jane A, Harris, Tamara, and Health ABC Study

Abstract

ObjectivesKlotho deficiency has been previously linked to aging-like phenotypes such as osteoporosis, cognitive impairment, and sarcopenia. Low serum klotho was shown to be related to grip strength and disability. Nonetheless, no previous study has explored the association between serum klotho and fractures. The purpose of this report is to examine the relationship of serum klotho with bone mineral density (BMD) loss and fractures in older adults.DesignThe Health, Aging, and Body Composition (Health ABC) Study is a longitudinal cohort study of 3,075 community-dwelling older adults.SettingUS clinical centers.ParticipantsTwo thousand seven hundred and seventy six well-functioning black and white adults aged 70 to 79 years with serum klotho measurements were followed up for a median of 5 years.MeasurementsPercent annualized BMD change and fracture risk were compared across klotho quartiles. A Poisson distribution was used to calculate age-adjusted fracture incidence rates, and Cox proportional hazards models for multivariable-adjusted hazard ratios.ResultsThe annualized percent changes in hip, femoral neck, and vertebral BMD were similar across klotho quartiles. Participants experienced 507 nonspine fractures, 203 hip fractures, and 135 vertebral fractures. The Incidence rate (IR) of nonspine fractures was 17 per 1,000 person-years. The most frequent site was hip (IR = 6 per 1,000 person-years) and the IR of vertebral fractures was 3 per 1,000 person-years. There was no association between the lowest quartile of plasma klotho and nonspine (hazard ratio (HR) = 1.19, 95% confidence interval (CI) = 0.86-1.65), hip (HR = 1.34, 95% CI = 0.79-2.27), or vertebral fractures (HR = 1.17, 95% CI = 0.65-2.11).ConclusionAlthough klotho gene is a susceptible gene for reduced BMD, klotho blood concentration does not appear to be a predictor of bone loss or fracture risk in well-functioning older adults.

Published
2016

32. Complement modulation of anti-aging factor klotho in ischemia/reperfusion injury and delayed graft function

Author

Castellano, G., Intini, A., Stasi, A., Divella, C., Gigante, M., Pontrelli, P., Franzin, R., Accetturo, M., Zito, A., Fiorentino, M., Montinaro, V., Lucarelli, G., Ditonno, P., Battaglia, M., Crovace, A., Staffieri, F., Oortwijn, B., Van Amersfoort, E., Pertosa, G., Grandaliano, Giuseppe, Gesualdo, L., Grandaliano G. (ORCID:0000-0003-1213-2177), Castellano, G., Intini, A., Stasi, A., Divella, C., Gigante, M., Pontrelli, P., Franzin, R., Accetturo, M., Zito, A., Fiorentino, M., Montinaro, V., Lucarelli, G., Ditonno, P., Battaglia, M., Crovace, A., Staffieri, F., Oortwijn, B., Van Amersfoort, E., Pertosa, G., Grandaliano, Giuseppe, Gesualdo, L., and Grandaliano G. (ORCID:0000-0003-1213-2177)

Abstract

Klotho is an anti-aging factor mainly produced by renal tubular epithelial cells (TEC) with pleiotropic functions. Klotho is down-regulated in acute kidney injury in native kidney; however, the modulation of Klotho in kidney transplantation has not been investigated. In a swine model of ischemia/reperfusion injury (IRI), we observed a remarkable reduction of renal Klotho by 24 h from IRI. Complement inhibition by C1-inhibitor preserved Klotho expression in vivo by abrogating nuclear factor kappa B (NF-kB) signaling. In accordance, complement anaphylotoxin C5a led to a significant down-regulation of Klotho in TEC in vitro that was NF-kB mediated. Analysis of Klotho in kidneys from cadaveric donors demonstrated a significant expression of Klotho in pre-implantation biopsies; however, patients affected by delayed graft function (DGF) showed a profound down-regulation of Klotho compared with patients with early graft function. Quantification of serum Klotho after 2 years from transplantation demonstrated significant lower levels in DGF patients. Our data demonstrated that complement might be pivotal in the down-regulation of Klotho in IRI leading to a permanent deficiency after years from transplantation. Considering the anti-senescence and anti-fibrotic effects of Klotho at renal levels, we hypothesize that this acquired deficiency of Klotho might contribute to DGF-associated chronic allograft dysfunction. The authors demonstrate a direct involvement of complement in regulating the expression of anti-aging factor Klotho in a swine model of ischemia/reperfusion injury, and lower levels of renal and soluble Klotho in patients affected by delayed graft function years after transplantation.

Published
2016

33. Impact of heparanase on renal fibrosis

Author

Masola, V, Zaza, G, Onisto, M, Lupo, A, Gambaro, Giovanni, Gambaro, Giovanni (ORCID:0000-0001-5733-2370), Masola, V, Zaza, G, Onisto, M, Lupo, A, Gambaro, Giovanni, and Gambaro, Giovanni (ORCID:0000-0001-5733-2370)

Published
2015

35. Genotypic and Phenotypic Characterization of Escherichia coli Isolates from Feces, Hands, and Soils in Rural Bangladesh via the Colilert Quanti-Tray System

Author

Julian, Timothy R, Elkins, CA1, Julian, Timothy R, Islam, M Aminul, Pickering, Amy J, Roy, Subarna, Fuhrmeister, Erica R, Ercumen, Ayse, Harris, Angela, Bishai, Jason, Schwab, Kellogg J, Julian, Timothy R, Elkins, CA1, Julian, Timothy R, Islam, M Aminul, Pickering, Amy J, Roy, Subarna, Fuhrmeister, Erica R, Ercumen, Ayse, Harris, Angela, Bishai, Jason, and Schwab, Kellogg J

Published
2015

36. Hepatic metabolism affects the atropselective disposition of 2,2',3,3',6,6'-hexachlorobiphenyl (PCB 136) in mice.

Author

Wu, Xianai, Wu, Xianai, Barnhart, Christopher, Lein, Pamela J, Lehmler, Hans-Joachim, Wu, Xianai, Wu, Xianai, Barnhart, Christopher, Lein, Pamela J, and Lehmler, Hans-Joachim

Abstract

To understand the role of hepatic vs extrahepatic metabolism in the disposition of chiral PCBs, we studied the disposition of 2,2',3,3',6,6'-hexachlorobiphenyl (PCB 136) and its hydroxylated metabolites (HO-PCBs) in mice with defective hepatic metabolism due to the liver-specific deletion of cytochrome P450 oxidoreductase (KO mice). Female KO and congenic wild type (WT) mice were treated with racemic PCB 136, and levels and chiral signatures of PCB 136 and HO-PCBs were determined in tissues and excreta 3 days after PCB administration. PCB 136 tissue levels were higher in KO compared to WT mice. Feces was a major route of PCB metabolite excretion, with 2,2',3,3',6,6'-hexachlorobiphenyl-5-ol being the major metabolite recovered from feces. (+)-PCB 136, the second eluting PCB 136 atropisomers, was enriched in all tissues and excreta. The second eluting atropisomers of the HO-PCBs metabolites were enriched in blood and liver; 2,2',3,3',6,6'-hexachlorobiphenyl-5-ol in blood was an exception and displayed an enrichment of the first eluting atropisomers. Fecal HO-PCB levels and chiral signatures changed with time and differed between KO and WT mice, with larger HO-PCB enantiomeric fractions in WT compared to KO mice. Our results demonstrate that hepatic and, possibly, extrahepatic cytochrome P450 (P450) enzymes play a role in the disposition of PCBs.

Published
2015

37. Reduced expression and growth inhibitory activity of the aging suppressor klotho in epithelial ovarian cancer.

Author

Lojkin, Irina, Lojkin, Irina, Rubinek, Tami, Orsulic, Sandra, Schwarzmann, Omer, Karlan, Beth Y, Bose, Shikha, Wolf, Ido, Lojkin, Irina, Lojkin, Irina, Rubinek, Tami, Orsulic, Sandra, Schwarzmann, Omer, Karlan, Beth Y, Bose, Shikha, and Wolf, Ido

Abstract

Klotho is an anti-aging transmembrane protein, which can be shed and function as a hormone. Accumulating data indicate klotho as a tumor suppressor in a wide array of malignancies, and we identified klotho as an inhibitor of the insulin-like growth factor (IGF-1) pathway in cancer cells. As this pathway is significant in the development of epithelial ovarian cancer (EOC) we studied klotho expression and activity in this tumor. Klotho mRNA levels were reduced in 16 of 19 EOC cell lines and immunohistochemistry analysis revealed high expression in normal ovaries, and reduced expression in 100 of 241 high grade papillary-serous adenocarcinoma of the ovaries, fallopian tubes and peritoneum. Reduced expression was associated with wild-type BRCA status. Klotho reduced EOC cell viability, enhanced cisplatin sensitivity, and reduced expression of mesenchymal markers. Finally, klotho inhibited IGF-1 pathway activation and inhibited transcriptional activity of the estrogen receptor. In conclusion, klotho is silenced in a substantial subset of the tumors and restoring its expression slows growth of EOC cells and inhibits major signaling pathways. As klotho is a hormone, treatment with klotho may serve as a novel treatment for EOC.

Published
2015

39. Hepatic metabolism affects the atropselective disposition of 2,2',3,3',6,6'-hexachlorobiphenyl (PCB 136) in mice.

Author

Wu, Xianai, Wu, Xianai, Barnhart, Christopher, Lein, Pamela J, Lehmler, Hans-Joachim, Wu, Xianai, Wu, Xianai, Barnhart, Christopher, Lein, Pamela J, and Lehmler, Hans-Joachim

Abstract

To understand the role of hepatic vs extrahepatic metabolism in the disposition of chiral PCBs, we studied the disposition of 2,2',3,3',6,6'-hexachlorobiphenyl (PCB 136) and its hydroxylated metabolites (HO-PCBs) in mice with defective hepatic metabolism due to the liver-specific deletion of cytochrome P450 oxidoreductase (KO mice). Female KO and congenic wild type (WT) mice were treated with racemic PCB 136, and levels and chiral signatures of PCB 136 and HO-PCBs were determined in tissues and excreta 3 days after PCB administration. PCB 136 tissue levels were higher in KO compared to WT mice. Feces was a major route of PCB metabolite excretion, with 2,2',3,3',6,6'-hexachlorobiphenyl-5-ol being the major metabolite recovered from feces. (+)-PCB 136, the second eluting PCB 136 atropisomers, was enriched in all tissues and excreta. The second eluting atropisomers of the HO-PCBs metabolites were enriched in blood and liver; 2,2',3,3',6,6'-hexachlorobiphenyl-5-ol in blood was an exception and displayed an enrichment of the first eluting atropisomers. Fecal HO-PCB levels and chiral signatures changed with time and differed between KO and WT mice, with larger HO-PCB enantiomeric fractions in WT compared to KO mice. Our results demonstrate that hepatic and, possibly, extrahepatic cytochrome P450 (P450) enzymes play a role in the disposition of PCBs.

Published
2015

40. Life extension factor klotho prevents mortality and enhances cognition in hAPP transgenic mice.

Author

Dubal, Dena B, Dubal, Dena B, Zhu, Lei, Sanchez, Pascal E, Worden, Kurtresha, Broestl, Lauren, Johnson, Erik, Ho, Kaitlyn, Yu, Gui-Qiu, Kim, Daniel, Betourne, Alexander, Kuro-O, Makoto, Masliah, Eliezer, Abraham, Carmela R, Mucke, Lennart, Dubal, Dena B, Dubal, Dena B, Zhu, Lei, Sanchez, Pascal E, Worden, Kurtresha, Broestl, Lauren, Johnson, Erik, Ho, Kaitlyn, Yu, Gui-Qiu, Kim, Daniel, Betourne, Alexander, Kuro-O, Makoto, Masliah, Eliezer, Abraham, Carmela R, and Mucke, Lennart

Abstract

Aging is the principal demographic risk factor for Alzheimer disease (AD), the most common neurodegenerative disorder. Klotho is a key modulator of the aging process and, when overexpressed, extends mammalian lifespan, increases synaptic plasticity, and enhances cognition. Whether klotho can counteract deficits related to neurodegenerative diseases, such as AD, is unknown. Here we show that elevating klotho expression decreases premature mortality and network dysfunction in human amyloid precursor protein (hAPP) transgenic mice, which simulate key aspects of AD. Increasing klotho levels prevented depletion of NMDA receptor (NMDAR) subunits in the hippocampus and enhanced spatial learning and memory in hAPP mice. Klotho elevation in hAPP mice increased the abundance of the GluN2B subunit of NMDAR in postsynaptic densities and NMDAR-dependent long-term potentiation, which is critical for learning and memory. Thus, increasing wild-type klotho levels or activities improves synaptic and cognitive functions, and may be of therapeutic benefit in AD and other cognitive disorders.

Published
2015

41. Reduced expression and growth inhibitory activity of the aging suppressor klotho in epithelial ovarian cancer.

Author

Lojkin, Irina, Lojkin, Irina, Rubinek, Tami, Orsulic, Sandra, Schwarzmann, Omer, Karlan, Beth Y, Bose, Shikha, Wolf, Ido, Lojkin, Irina, Lojkin, Irina, Rubinek, Tami, Orsulic, Sandra, Schwarzmann, Omer, Karlan, Beth Y, Bose, Shikha, and Wolf, Ido

Abstract

Klotho is an anti-aging transmembrane protein, which can be shed and function as a hormone. Accumulating data indicate klotho as a tumor suppressor in a wide array of malignancies, and we identified klotho as an inhibitor of the insulin-like growth factor (IGF-1) pathway in cancer cells. As this pathway is significant in the development of epithelial ovarian cancer (EOC) we studied klotho expression and activity in this tumor. Klotho mRNA levels were reduced in 16 of 19 EOC cell lines and immunohistochemistry analysis revealed high expression in normal ovaries, and reduced expression in 100 of 241 high grade papillary-serous adenocarcinoma of the ovaries, fallopian tubes and peritoneum. Reduced expression was associated with wild-type BRCA status. Klotho reduced EOC cell viability, enhanced cisplatin sensitivity, and reduced expression of mesenchymal markers. Finally, klotho inhibited IGF-1 pathway activation and inhibited transcriptional activity of the estrogen receptor. In conclusion, klotho is silenced in a substantial subset of the tumors and restoring its expression slows growth of EOC cells and inhibits major signaling pathways. As klotho is a hormone, treatment with klotho may serve as a novel treatment for EOC.

Published
2015

44. Life extension factor klotho enhances cognition.

Author

Dubal, Dena B, Dubal, Dena B, Yokoyama, Jennifer S, Zhu, Lei, Broestl, Lauren, Worden, Kurtresha, Wang, Dan, Sturm, Virginia E, Kim, Daniel, Klein, Eric, Yu, Gui-Qiu, Ho, Kaitlyn, Eilertson, Kirsten E, Yu, Lei, Kuro-o, Makoto, De Jager, Philip L, Coppola, Giovanni, Small, Gary W, Bennett, David A, Kramer, Joel H, Abraham, Carmela R, Miller, Bruce L, Mucke, Lennart, Dubal, Dena B, Dubal, Dena B, Yokoyama, Jennifer S, Zhu, Lei, Broestl, Lauren, Worden, Kurtresha, Wang, Dan, Sturm, Virginia E, Kim, Daniel, Klein, Eric, Yu, Gui-Qiu, Ho, Kaitlyn, Eilertson, Kirsten E, Yu, Lei, Kuro-o, Makoto, De Jager, Philip L, Coppola, Giovanni, Small, Gary W, Bennett, David A, Kramer, Joel H, Abraham, Carmela R, Miller, Bruce L, and Mucke, Lennart

Abstract

Aging is the primary risk factor for cognitive decline, an emerging health threat to aging societies worldwide. Whether anti-aging factors such as klotho can counteract cognitive decline is unknown. We show that a lifespan-extending variant of the human KLOTHO gene, KL-VS, is associated with enhanced cognition in heterozygous carriers. Because this allele increased klotho levels in serum, we analyzed transgenic mice with systemic overexpression of klotho. They performed better than controls in multiple tests of learning and memory. Elevating klotho in mice also enhanced long-term potentiation, a form of synaptic plasticity, and enriched synaptic GluN2B, an N-methyl-D-aspartate receptor (NMDAR) subunit with key functions in learning and memory. Blockade of GluN2B abolished klotho-mediated effects. Surprisingly, klotho effects were evident also in young mice and did not correlate with age in humans, suggesting independence from the aging process. Augmenting klotho or its effects may enhance cognition and counteract cognitive deficits at different life stages.

Published
2014

45. Demystifying heparan sulfate-protein interactions.

Author

Xu, Ding, Xu, Ding, Esko, Jeffrey D, Xu, Ding, Xu, Ding, and Esko, Jeffrey D

Abstract

Numerous proteins, including cytokines and chemokines, enzymes and enzyme inhibitors, extracellular matrix proteins, and membrane receptors, bind heparin. Although they are traditionally classified as heparin-binding proteins, under normal physiological conditions these proteins actually interact with the heparan sulfate chains of one or more membrane or extracellular proteoglycans. Thus, they are more appropriately classified as heparan sulfate-binding proteins (HSBPs). This review provides an overview of the various modes of interaction between heparan sulfate and HSBPs, emphasizing biochemical and structural insights that improve our understanding of the many biological functions of heparan sulfate.

Published
2014

46. Life extension factor klotho enhances cognition.

Author

Dubal, Dena B, Dubal, Dena B, Yokoyama, Jennifer S, Zhu, Lei, Broestl, Lauren, Worden, Kurtresha, Wang, Dan, Sturm, Virginia E, Kim, Daniel, Klein, Eric, Yu, Gui-Qiu, Ho, Kaitlyn, Eilertson, Kirsten E, Yu, Lei, Kuro-o, Makoto, De Jager, Philip L, Coppola, Giovanni, Small, Gary W, Bennett, David A, Kramer, Joel H, Abraham, Carmela R, Miller, Bruce L, Mucke, Lennart, Dubal, Dena B, Dubal, Dena B, Yokoyama, Jennifer S, Zhu, Lei, Broestl, Lauren, Worden, Kurtresha, Wang, Dan, Sturm, Virginia E, Kim, Daniel, Klein, Eric, Yu, Gui-Qiu, Ho, Kaitlyn, Eilertson, Kirsten E, Yu, Lei, Kuro-o, Makoto, De Jager, Philip L, Coppola, Giovanni, Small, Gary W, Bennett, David A, Kramer, Joel H, Abraham, Carmela R, Miller, Bruce L, and Mucke, Lennart

Abstract

Aging is the primary risk factor for cognitive decline, an emerging health threat to aging societies worldwide. Whether anti-aging factors such as klotho can counteract cognitive decline is unknown. We show that a lifespan-extending variant of the human KLOTHO gene, KL-VS, is associated with enhanced cognition in heterozygous carriers. Because this allele increased klotho levels in serum, we analyzed transgenic mice with systemic overexpression of klotho. They performed better than controls in multiple tests of learning and memory. Elevating klotho in mice also enhanced long-term potentiation, a form of synaptic plasticity, and enriched synaptic GluN2B, an N-methyl-D-aspartate receptor (NMDAR) subunit with key functions in learning and memory. Blockade of GluN2B abolished klotho-mediated effects. Surprisingly, klotho effects were evident also in young mice and did not correlate with age in humans, suggesting independence from the aging process. Augmenting klotho or its effects may enhance cognition and counteract cognitive deficits at different life stages.

Published
2014

47. Demystifying heparan sulfate-protein interactions.

Author

Xu, Ding, Xu, Ding, Esko, Jeffrey D, Xu, Ding, Xu, Ding, and Esko, Jeffrey D

Abstract

Numerous proteins, including cytokines and chemokines, enzymes and enzyme inhibitors, extracellular matrix proteins, and membrane receptors, bind heparin. Although they are traditionally classified as heparin-binding proteins, under normal physiological conditions these proteins actually interact with the heparan sulfate chains of one or more membrane or extracellular proteoglycans. Thus, they are more appropriately classified as heparan sulfate-binding proteins (HSBPs). This review provides an overview of the various modes of interaction between heparan sulfate and HSBPs, emphasizing biochemical and structural insights that improve our understanding of the many biological functions of heparan sulfate.

Published
2014

48. A genetic screen for mutants defective in IAA1-LUC degradation in Arabidopsis thaliana reveals an important requirement for TOPOISOMERASE6B in auxin physiology.

Author

Gilkerson, Jonathan, Gilkerson, Jonathan, Callis, Judy, Gilkerson, Jonathan, Gilkerson, Jonathan, and Callis, Judy

Abstract

Many plant growth and developmental processes are modulated by the hormone auxin. Auxin-modulated proteolysis of Aux/IAAs, a family of transcriptional repressors, represents a major mode of auxin action. Auxin facilitates the interaction of Aux/IAAs with TIR1/AFB F-box proteins, promoting their ubiquitination by the SCF(TIR1/AFB) ubiquitin E3 ligase leading to subsequent degradation by the 26S proteasome. To identify new genes regulating Aux/IAA proteolysis in Arabidopsis thaliana, we took a genetic approach, identifying individuals with altered degradation of an IAA1-luciferase fusion protein (IAA1-LUC). A mutant with 2-fold slower IAA1-LUC degradation rate compared with wild-type was isolated. Positional cloning identified the mutant as an allele of TOPOISOMERASE6B, named top6b-7. TOP6B encodes a subunit of a plant and archea-specific enzyme regulating endoreduplication, DNA damage repair and transcription in plants. T-DNA insertion alleles (top6b-8 and top6b-9) were also analyzed. top6b-7 seedlings are less sensitive to exogenous auxin than wild-type siblings in primary root growth assays, and experiments with DR5:GUS. Additionally, top6b-7 seedlings have a 40% reduction in the amount of endogenous IAA. These data suggest that increased IAA1-LUC half-life in top6b-7 probably results from a combination of both lower endogenous IAA levels and reduced sensitivity to auxin.

Published
2014

49. Life extension factor klotho enhances cognition.

Author

Dubal, Dena B, Dubal, Dena B, Yokoyama, Jennifer S, Zhu, Lei, Broestl, Lauren, Worden, Kurtresha, Wang, Dan, Sturm, Virginia E, Kim, Daniel, Klein, Eric, Yu, Gui-Qiu, Ho, Kaitlyn, Eilertson, Kirsten E, Yu, Lei, Kuro-o, Makoto, De Jager, Philip L, Coppola, Giovanni, Small, Gary W, Bennett, David A, Kramer, Joel H, Abraham, Carmela R, Miller, Bruce L, Mucke, Lennart, Dubal, Dena B, Dubal, Dena B, Yokoyama, Jennifer S, Zhu, Lei, Broestl, Lauren, Worden, Kurtresha, Wang, Dan, Sturm, Virginia E, Kim, Daniel, Klein, Eric, Yu, Gui-Qiu, Ho, Kaitlyn, Eilertson, Kirsten E, Yu, Lei, Kuro-o, Makoto, De Jager, Philip L, Coppola, Giovanni, Small, Gary W, Bennett, David A, Kramer, Joel H, Abraham, Carmela R, Miller, Bruce L, and Mucke, Lennart

Abstract

Aging is the primary risk factor for cognitive decline, an emerging health threat to aging societies worldwide. Whether anti-aging factors such as klotho can counteract cognitive decline is unknown. We show that a lifespan-extending variant of the human KLOTHO gene, KL-VS, is associated with enhanced cognition in heterozygous carriers. Because this allele increased klotho levels in serum, we analyzed transgenic mice with systemic overexpression of klotho. They performed better than controls in multiple tests of learning and memory. Elevating klotho in mice also enhanced long-term potentiation, a form of synaptic plasticity, and enriched synaptic GluN2B, an N-methyl-D-aspartate receptor (NMDAR) subunit with key functions in learning and memory. Blockade of GluN2B abolished klotho-mediated effects. Surprisingly, klotho effects were evident also in young mice and did not correlate with age in humans, suggesting independence from the aging process. Augmenting klotho or its effects may enhance cognition and counteract cognitive deficits at different life stages.

Published
2014

50. Demystifying Heparan Sulfate–Protein Interactions

Author

Xu, Ding, Xu, Ding, Esko, Jeffrey D, Xu, Ding, Xu, Ding, and Esko, Jeffrey D

Abstract

Numerous proteins, including cytokines and chemokines, enzymes and enzyme inhibitors, extracellular matrix proteins, and membrane receptors, bind heparin. Although they are traditionally classified as heparin-binding proteins, under normal physiological conditions these proteins actually interact with the heparan sulfate chains of one or more membrane or extracellular proteoglycans. Thus, they are more appropriately classified as heparan sulfate-binding proteins (HSBPs). This review provides an overview of the various modes of interaction between heparan sulfate and HSBPs, emphasizing biochemical and structural insights that improve our understanding of the many biological functions of heparan sulfate.

Published
2014

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