Your search keyword '"Naia, Luana"' showing total 6 results

1. Amyloid-beta accumulation in human astrocytes induces mitochondrial disruption and changed energy metabolism

Author

Zyśk, Marlena, Beretta, Chiara, Naia, Luana, Dakhel, Abdulkhalek, Pavenius, Linnea, Brismar, Hjalmar, Lindskog, Maria, Ankarcrona, Maria, Erlandsson, Anna, Zyśk, Marlena, Beretta, Chiara, Naia, Luana, Dakhel, Abdulkhalek, Pavenius, Linnea, Brismar, Hjalmar, Lindskog, Maria, Ankarcrona, Maria, and Erlandsson, Anna

Abstract

Background: Astrocytes play a central role in maintaining brain energy metabolism, but are also tightly connected to the pathogenesis of Alzheimer's disease (AD). Our previous studies demonstrate that inflammatory astrocytes accumulate large amounts of aggregated amyloid-beta (A beta). However, in which way these A beta deposits influence their energy production remain unclear. Methods: The aim of the present study was to investigate how A beta pathology in astrocytes affects their mitochondria functionality and overall energy metabolism. For this purpose, human induced pluripotent cell (hiPSC)-derived astrocytes were exposed to sonicated A beta(42) fibrils for 7 days and analyzed over time using different experimental approaches. Results: Our results show that to maintain stable energy production, the astrocytes initially increased their mitochondrial fusion, but eventually the A beta-mediated stress led to abnormal mitochondrial swelling and excessive fission. Moreover, we detected increased levels of phosphorylated DRP-1 in the A beta-exposed astrocytes, which co-localized with lipid droplets. Analysis of ATP levels, when blocking certain stages of the energy pathways, indicated a metabolic shift to peroxisomal-based fatty acid beta-oxidation and glycolysis. Conclusions: Taken together, our data conclude that A beta pathology profoundly affects human astrocytes and changes their entire energy metabolism, which could result in disturbed brain homeostasis and aggravated disease progression., De två första författarna delar förstaförfattarskapet.

Published

2023

2. Amyloid-beta accumulation in human astrocytes induces mitochondrial disruption and changed energy metabolism

Author

Zyśk, Marlena, Beretta, Chiara, Naia, Luana, Dakhel, Abdulkhalek, Pavenius, Linnea, Brismar, Hjalmar, Lindskog, Maria, Ankarcrona, Maria, Erlandsson, Anna, Zyśk, Marlena, Beretta, Chiara, Naia, Luana, Dakhel, Abdulkhalek, Pavenius, Linnea, Brismar, Hjalmar, Lindskog, Maria, Ankarcrona, Maria, and Erlandsson, Anna

Abstract

Background: Astrocytes play a central role in maintaining brain energy metabolism, but are also tightly connected to the pathogenesis of Alzheimer's disease (AD). Our previous studies demonstrate that inflammatory astrocytes accumulate large amounts of aggregated amyloid-beta (A beta). However, in which way these A beta deposits influence their energy production remain unclear. Methods: The aim of the present study was to investigate how A beta pathology in astrocytes affects their mitochondria functionality and overall energy metabolism. For this purpose, human induced pluripotent cell (hiPSC)-derived astrocytes were exposed to sonicated A beta(42) fibrils for 7 days and analyzed over time using different experimental approaches. Results: Our results show that to maintain stable energy production, the astrocytes initially increased their mitochondrial fusion, but eventually the A beta-mediated stress led to abnormal mitochondrial swelling and excessive fission. Moreover, we detected increased levels of phosphorylated DRP-1 in the A beta-exposed astrocytes, which co-localized with lipid droplets. Analysis of ATP levels, when blocking certain stages of the energy pathways, indicated a metabolic shift to peroxisomal-based fatty acid beta-oxidation and glycolysis. Conclusions: Taken together, our data conclude that A beta pathology profoundly affects human astrocytes and changes their entire energy metabolism, which could result in disturbed brain homeostasis and aggravated disease progression., De två första författarna delar förstaförfattarskapet.

Published

2023

3. Amyloid-beta accumulation in human astrocytes induces mitochondrial disruption and changed energy metabolism

Author

Zyśk, Marlena, Beretta, Chiara, Naia, Luana, Dakhel, Abdulkhalek, Pavenius, Linnea, Brismar, Hjalmar, Lindskog, Maria, Ankarcrona, Maria, Erlandsson, Anna, Zyśk, Marlena, Beretta, Chiara, Naia, Luana, Dakhel, Abdulkhalek, Pavenius, Linnea, Brismar, Hjalmar, Lindskog, Maria, Ankarcrona, Maria, and Erlandsson, Anna

Abstract

Background: Astrocytes play a central role in maintaining brain energy metabolism, but are also tightly connected to the pathogenesis of Alzheimer's disease (AD). Our previous studies demonstrate that inflammatory astrocytes accumulate large amounts of aggregated amyloid-beta (A beta). However, in which way these A beta deposits influence their energy production remain unclear. Methods: The aim of the present study was to investigate how A beta pathology in astrocytes affects their mitochondria functionality and overall energy metabolism. For this purpose, human induced pluripotent cell (hiPSC)-derived astrocytes were exposed to sonicated A beta(42) fibrils for 7 days and analyzed over time using different experimental approaches. Results: Our results show that to maintain stable energy production, the astrocytes initially increased their mitochondrial fusion, but eventually the A beta-mediated stress led to abnormal mitochondrial swelling and excessive fission. Moreover, we detected increased levels of phosphorylated DRP-1 in the A beta-exposed astrocytes, which co-localized with lipid droplets. Analysis of ATP levels, when blocking certain stages of the energy pathways, indicated a metabolic shift to peroxisomal-based fatty acid beta-oxidation and glycolysis. Conclusions: Taken together, our data conclude that A beta pathology profoundly affects human astrocytes and changes their entire energy metabolism, which could result in disturbed brain homeostasis and aggravated disease progression., De två första författarna delar förstaförfattarskapet.

Published

2023

4. Amyloid-beta accumulation in human astrocytes induces mitochondrial disruption and changed energy metabolism

Author

Zysk, Marlena, Beretta, Chiara, Naia, Luana, Dakhel, Abdulkhalek, Pavenius, Linnea, Brismar, Hjalmar, Lindskog, Maria, Ankarcrona, Maria, Erlandsson, Anna, Zysk, Marlena, Beretta, Chiara, Naia, Luana, Dakhel, Abdulkhalek, Pavenius, Linnea, Brismar, Hjalmar, Lindskog, Maria, Ankarcrona, Maria, and Erlandsson, Anna

Abstract

BackgroundAstrocytes play a central role in maintaining brain energy metabolism, but are also tightly connected to the pathogenesis of Alzheimer's disease (AD). Our previous studies demonstrate that inflammatory astrocytes accumulate large amounts of aggregated amyloid-beta (A beta). However, in which way these A beta deposits influence their energy production remain unclear.MethodsThe aim of the present study was to investigate how A beta pathology in astrocytes affects their mitochondria functionality and overall energy metabolism. For this purpose, human induced pluripotent cell (hiPSC)-derived astrocytes were exposed to sonicated A beta(42) fibrils for 7 days and analyzed over time using different experimental approaches.ResultsOur results show that to maintain stable energy production, the astrocytes initially increased their mitochondrial fusion, but eventually the A beta-mediated stress led to abnormal mitochondrial swelling and excessive fission. Moreover, we detected increased levels of phosphorylated DRP-1 in the A beta-exposed astrocytes, which co-localized with lipid droplets. Analysis of ATP levels, when blocking certain stages of the energy pathways, indicated a metabolic shift to peroxisomal-based fatty acid beta-oxidation and glycolysis.ConclusionsTaken together, our data conclude that A beta pathology profoundly affects human astrocytes and changes their entire energy metabolism, which could result in disturbed brain homeostasis and aggravated disease progression., QC 20230321

Published

2023

5. Amyloid-beta accumulation in human astrocytes induces mitochondrial disruption and changed energy metabolism

Author

Zyśk, Marlena, Beretta, Chiara, Naia, Luana, Dakhel, Abdulkhalek, Pavenius, Linnea, Brismar, Hjalmar, Lindskog, Maria, Ankarcrona, Maria, Erlandsson, Anna, Zyśk, Marlena, Beretta, Chiara, Naia, Luana, Dakhel, Abdulkhalek, Pavenius, Linnea, Brismar, Hjalmar, Lindskog, Maria, Ankarcrona, Maria, and Erlandsson, Anna

Abstract

Background: Astrocytes play a central role in maintaining brain energy metabolism, but are also tightly connected to the pathogenesis of Alzheimer's disease (AD). Our previous studies demonstrate that inflammatory astrocytes accumulate large amounts of aggregated amyloid-beta (A beta). However, in which way these A beta deposits influence their energy production remain unclear. Methods: The aim of the present study was to investigate how A beta pathology in astrocytes affects their mitochondria functionality and overall energy metabolism. For this purpose, human induced pluripotent cell (hiPSC)-derived astrocytes were exposed to sonicated A beta(42) fibrils for 7 days and analyzed over time using different experimental approaches. Results: Our results show that to maintain stable energy production, the astrocytes initially increased their mitochondrial fusion, but eventually the A beta-mediated stress led to abnormal mitochondrial swelling and excessive fission. Moreover, we detected increased levels of phosphorylated DRP-1 in the A beta-exposed astrocytes, which co-localized with lipid droplets. Analysis of ATP levels, when blocking certain stages of the energy pathways, indicated a metabolic shift to peroxisomal-based fatty acid beta-oxidation and glycolysis. Conclusions: Taken together, our data conclude that A beta pathology profoundly affects human astrocytes and changes their entire energy metabolism, which could result in disturbed brain homeostasis and aggravated disease progression., De två första författarna delar förstaförfattarskapet.

Published

2023

6. Amyloid-beta accumulation in human astrocytes induces mitochondrial disruption and changed energy metabolism

Author

Zyśk, Marlena, Beretta, Chiara, Naia, Luana, Dakhel, Abdulkhalek, Pavenius, Linnea, Brismar, Hjalmar, Lindskog, Maria, Ankarcrona, Maria, Erlandsson, Anna, Zyśk, Marlena, Beretta, Chiara, Naia, Luana, Dakhel, Abdulkhalek, Pavenius, Linnea, Brismar, Hjalmar, Lindskog, Maria, Ankarcrona, Maria, and Erlandsson, Anna

Abstract

Background: Astrocytes play a central role in maintaining brain energy metabolism, but are also tightly connected to the pathogenesis of Alzheimer's disease (AD). Our previous studies demonstrate that inflammatory astrocytes accumulate large amounts of aggregated amyloid-beta (A beta). However, in which way these A beta deposits influence their energy production remain unclear. Methods: The aim of the present study was to investigate how A beta pathology in astrocytes affects their mitochondria functionality and overall energy metabolism. For this purpose, human induced pluripotent cell (hiPSC)-derived astrocytes were exposed to sonicated A beta(42) fibrils for 7 days and analyzed over time using different experimental approaches. Results: Our results show that to maintain stable energy production, the astrocytes initially increased their mitochondrial fusion, but eventually the A beta-mediated stress led to abnormal mitochondrial swelling and excessive fission. Moreover, we detected increased levels of phosphorylated DRP-1 in the A beta-exposed astrocytes, which co-localized with lipid droplets. Analysis of ATP levels, when blocking certain stages of the energy pathways, indicated a metabolic shift to peroxisomal-based fatty acid beta-oxidation and glycolysis. Conclusions: Taken together, our data conclude that A beta pathology profoundly affects human astrocytes and changes their entire energy metabolism, which could result in disturbed brain homeostasis and aggravated disease progression., De två första författarna delar förstaförfattarskapet.

Published

2023