Affiliation:
1. UNIVERSITY OF HEALTH SCIENCES, INSTITUTE OF HEALTH SCIENCES, MEDICAL BIOCHEMISTRY (MEDICINE) (DR)
2. KUTAHYA HEALTH SCIENCES UNIVERSITY, FACULTY OF ENGINEERING AND NATURAL SCIENCES, DEPARTMENT OF BASIC SCIENCES OF ENGINEERING
3. KUTAHYA HEALTH SCIENCES UNIVERSITY, VOCATIONAL SCHOOL OF HEALTH SERVICES, MEDICAL IMAGING TECHNIQUES PR.
4. KUTAHYA HEALTH SCIENCES UNIVERSITY, VOCATIONAL SCHOOL OF HEALTH SERVICES, MEDICAL LABORATORY TECHNIQUES PR.
Abstract
Objective: Scleroderma (SSc) is a rare autoimmune tissue disease. There is currently no effective treatment for SSc. The aim of this
study was to investigate the antioxidant and anti-inflammatory effects of upadacitinib and PD29 on total oxidant status (TOS), total
antioxidant status (TAS), malondialdehyde (MDA), catalase (CAT), glutathione (GSH) peroxidase levels, and interleukin-6 (IL-6) and
interleukin-13 ( IL-13) in kidney tissues of an experimental SSc model.
Materials and Methods: The experimental design was established with five groups of eight mice: Control, bleomycin (BLM) (5 μg/kg),
BLM + upadacitinib (3mg/kg), BLM + PD29 (5 mg/kg) and BLM + PD29 + upadacitinib group. BLM was administered subcutaneously
once a day for 21 days. PD29 was administered subcutaneously and upadacitinib (gavage) were injected for 21 days. Renal tissues were
collected at the end of the experiment. Renal TOS, TAS, MDA, CAT, GSH levels, and IL-6 and IL-13 gene expressions were evaluated.
Results: Upadacitinib and PD29 affected oxidant status and TOS. MDA levels decreased, and GSH, CAT, and TAS levels increased.
Also, upadacitinib and PD29 decreased inflammation via IL-6 and IL-13 cytokines.
Conclusion: Upadacitinib and PD29 may have therapeutic roles for SSc renal crisis.