CKD is diagnosed when there’s a decreased kidney function shown by a GFR less than 60 ml / min (established for a reference man with 1.73 m² body surface area), or markers of kidney damage, or both, of at least 3 months duration. The severity of complications increases in parallel with the GFR decline. We focused on three comorbidities extremely common in CKD patients: oxidative stress and inflammation; anemia and dysbiosis. We investigated these CKD comorbidities both with in vitro and in vivo approaches. More in detail, regarding in vivo studies, we measured oxidative stress biomarkers in a population of ESRD patients before and after the hemodialysis treatment, comparing the results with a population of healthy subjects; we evaluated oxidative stress biomarkers in the plasma of HD patients before, during and after two type of iron treatments (intravenous and sucrosomial iron). Regarding in vitro experiments, we focused on two uremic toxins, urea and indoxyl sulphate, and we evaluated their effects on a human endothelial cell line (Human Microvascular Endothelial Cells 1, HMEC-1).

IN VITRO AND IN VIVO APPROACHES TO STUDY OXIDATIVE STRESS, ANEMIA AND DYSBIOSIS IN CHRONIC KIDNEY DISEASE / E. Astori ; tutor: I. Dalle Donne ; commissario interno: N. Gagliano ; commissario esterno: S. Moreno ; commissario esterno: A. E. Colombo ; head pf phd course: F. Ficetola. Università degli Studi di Milano, 2021 Feb 23. 33. ciclo, Anno Accademico 2020. [10.13130/astori-emanuela_phd2021-02-23].

IN VITRO AND IN VIVO APPROACHES TO STUDY OXIDATIVE STRESS, ANEMIA AND DYSBIOSIS IN CHRONIC KIDNEY DISEASE

E. Astori
2021

Abstract

CKD is diagnosed when there’s a decreased kidney function shown by a GFR less than 60 ml / min (established for a reference man with 1.73 m² body surface area), or markers of kidney damage, or both, of at least 3 months duration. The severity of complications increases in parallel with the GFR decline. We focused on three comorbidities extremely common in CKD patients: oxidative stress and inflammation; anemia and dysbiosis. We investigated these CKD comorbidities both with in vitro and in vivo approaches. More in detail, regarding in vivo studies, we measured oxidative stress biomarkers in a population of ESRD patients before and after the hemodialysis treatment, comparing the results with a population of healthy subjects; we evaluated oxidative stress biomarkers in the plasma of HD patients before, during and after two type of iron treatments (intravenous and sucrosomial iron). Regarding in vitro experiments, we focused on two uremic toxins, urea and indoxyl sulphate, and we evaluated their effects on a human endothelial cell line (Human Microvascular Endothelial Cells 1, HMEC-1).
23-feb-2021
Settore BIO/06 - Anatomia Comparata e Citologia
chronic kidney disease; kidneys; hemodialysis; oxidative stress; protein carbonyls; proteins thiols; advanced oxidation protein products; sucrosomial iron; anemia; inflammation; disbyosis; uremia; uremic toxins; urea; indoxyl sulphate; proteomics
DALLE DONNE, ISABELLA
COLOMBO, GRAZIANO
MILZANI, ALDO DOMENICO GUIDO
FICETOLA, GENTILE FRANCESCO
Doctoral Thesis
IN VITRO AND IN VIVO APPROACHES TO STUDY OXIDATIVE STRESS, ANEMIA AND DYSBIOSIS IN CHRONIC KIDNEY DISEASE / E. Astori ; tutor: I. Dalle Donne ; commissario interno: N. Gagliano ; commissario esterno: S. Moreno ; commissario esterno: A. E. Colombo ; head pf phd course: F. Ficetola. Università degli Studi di Milano, 2021 Feb 23. 33. ciclo, Anno Accademico 2020. [10.13130/astori-emanuela_phd2021-02-23].
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2434/818976
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