3 research outputs found
Endothelial Dysfunction and Systemic Inflammation in the Pathogenesis and Progression of Portal Hypertension
Get PDFHepatic and extrahepatic factors contribute to mortality related to liver cirrhosis and therefore much research is still to be done in order to understand the condition thoroughly and to possibly intervene in the process. It is considered that the currently applied prognostic scores are not ideal mortality predictors. On the other hand, recent scientific concepts have revealed the significant contributing role of endothelial dysfunction and of systemic inflammation in the pathogenesis of portal hypertension. Consequently, these concepts are inevitably leading towards proposing and validating new prognostic indicators in cirrhotic patients. Von-Willebrand factor as an indicator of endothelial dysfunction and C-reactive protein as a surrogate marker of systemic inflammation and several other parameters and biological markers have been emerging as a relevant and potentially useful prognostic indicators. Also, the coagulopathy associated to liver disease is in close relation with these entities and still an important research topic. Despite the promising data regarding their prognostic potential, additional research is needed in order to define and validate their value more precisely in clinical and prognostic settings
ΠΡΠΎΡΠ΅Π½ΠΊΠ° Π½Π° ΠΎΡΡΠ΅ΠΎΠΏΠΎΡΠΎΠ·Π°ΡΠ° ΠΈ ΠΏΠΎΡΠ°Π²Π° Π½Π° Π²Π΅ΡΡΠ΅Π±ΡΠ°Π»Π½ΠΈ ΡΡΠ°ΠΊΡΡΡΠΈ ΠΊΠ°Ρ ΠΏΠΎΡΡΠΌΠ΅Π½ΠΎΠΏΠ°ΡΠ·Π½ΠΈ ΠΏΠ°ΡΠΈΠ΅Π½ΡΠΊΠΈ ΡΠΎ ΡΠ΅Π²ΠΌΠ°ΡΠΎΠΈΠ΄Π΅Π½ Π°ΡΡΡΠΈΡΠΈΡ ΡΡΠ΅ΡΠΈΡΠ°Π½ΠΈ ΡΠΎ ΠΌΠ°Π»ΠΈ Π΄ΠΎΠ·ΠΈ Π½Π° Π³Π»ΠΈΠΊΠΎΠΊΠΎΡΡΠΈΠΊΠΎΠΈΠ΄ΠΈ
Get PDFOsteoporosis (OP) is a serious extracorporeal manifestation that occurs in patients with rheumatoid arthritis (RA). One of the risk factors is long-term use of glucocorticoids (GC). Osteoporosis together with the increased risk of vertebral (VF) and non-vertebral fractures (non-VF) in particular has a negative impact on quality of life in patients with rheumatoid arthritis. The aim of the study was to detect the occurrence of OP and VF in postmenopausal patients with RA and their association with long-term use of small doses of glucocorticoids. Material and methods: A total of 46 patients were analyzed. All respondents underwent imaging for osteoporosis evaluation with a DXA scanner (Lunar iDXA, GE) and VF with incorporated Vertebral Fracture Assessment (VFA). Results: The values of bone mineral densities (BMD) were significantly smaller in the group that received glucocorticoids. According to VFA, 37,0% of patients were registered to have a fracture of middle degree, a mild fracture was registered in 19.6% of patients, and severe fractures were registered in 3 patients (6.5%). Conclusion: In postmenopausal patients with RA receiving GC therapy, a more common occurrence of osteoporosis and vertebral fractures was reported compared with the remaining group of RA patients. All patients with RA in menopause need to be screened for timely detection and treatment of osteoporosis and prevention of its complications.ΠΡΡΠ΅ΠΎΠΏΠΎΡΠΎΠ·Π°ΡΠ° (OP) Π΅ ΡΠ΅ΡΠΈΠΎΠ·Π½Π° Π²ΠΎΠ½Π·Π³Π»ΠΎΠ±Π½Π° ΠΌΠ°Π½ΠΈΡΠ΅ΡΡΠ°ΡΠΈΡΠ° ΠΊΠΎΡΠ° ΡΠ΅ ΡΠ°Π²ΡΠ²Π° ΠΊΠ°Ρ ΠΏΠ°ΡΠΈΠ½Π΅ΡΠΊΠΈ ΡΠΎ ΡΠ΅Π²ΠΌΠ°ΡΠΎΠΈΠ΄Π΅Π½ Π°ΡΡΡΠΈΡΠΈΡ (RA). ΠΠ΄Π΅Π½ ΠΎΠ΄ ΡΠΈΠ·ΠΈΠΊ-ΡΠ°ΠΊΡΠΎΡΠΈΡΠ΅ ΠΏΡΠ΅ΡΡΡΠ°Π²ΡΠ²Π° Π΄ΠΎΠ»Π³ΠΎΡΡΠ°ΡΠ½Π°ΡΠ° ΠΏΡΠΈΠΌΠ΅Π½Π° Π½Π° Π³Π»ΠΈΠΊΠΎΠΊΠΎΡΡΠΈΠΊΠΎΠΈΠ΄ΠΈ (GC). ΠΡΡΠ΅ΠΎΠΏΠΎΡΠΎΠ·Π°ΡΠ° Π·Π°Π΅Π΄Π½ΠΎ ΡΠΎ Π·Π³ΠΎΠ»Π΅ΠΌΠ΅Π½ΠΈΠΎΡ ΡΠΈΠ·ΠΈΠΊ ΠΎΠ΄ Π²Π΅ΡΡΠ΅Π±ΡΠ°Π»Π½ΠΈ (VF) ΠΈ Π½Π΅Π²Π΅ΡΡΠ΅Π±ΡΠ°Π»Π½ΠΈ ΡΡΠ°ΠΊΡΡΡΠΈ (non-VF) ΠΈΠΌΠ° Π½Π΅Π³Π°ΡΠΈΠ²Π½ΠΎ Π²Π»ΠΈΡΠ°Π½ΠΈΠ΅ Π²ΡΠ· ΠΊΠ²Π°Π»ΠΈΡΠ΅ΡΠΎΡ Π½Π° ΠΆΠΈΠ²ΠΎΡ ΠΊΠ°Ρ ΠΏΠ°ΡΠΈΠ΅Π½ΡΠΊΠΈΡΠ΅ ΡΠΎ ΡΠ΅Π²ΠΌΠ°ΡΠΎΠΈΠ΄Π΅Π½ Π°ΡΡΡΠΈΡΠΈΡ. Π¦Π΅Π»ΡΠ° Π½Π° ΡΡΡΠ΄ΠΎΡ Π±Π΅ΡΠ΅ Π΄Π° ΡΠ΅ Π΄Π΅ΡΠ΅ΠΊΡΠΈΡΠ° ΠΏΠΎΡΠ°Π²Π°ΡΠ° Π½Π° OP ΠΈ VF ΠΊΠ°Ρ ΠΏΠΎΡΡΠΌΠ΅Π½ΠΎΠΏΠ°ΡΠ·Π½ΠΈ ΠΏΠ°ΡΠΈΠ΅Π½ΡΠΊΠΈ ΡΠΎ RΠ ΠΈ Π½ΠΈΠ²Π½Π°ΡΠ° ΠΏΠΎΠ²ΡΠ·Π°Π½ΠΎΡΡ ΡΠΎ Π΄ΠΎΠ»Π³ΠΎΡΡΠ°ΡΠ½Π°ΡΠ° ΠΏΡΠΈΠΌΠ΅Π½Π° Π½Π° ΠΌΠ°Π»ΠΈ Π΄ΠΎΠ·ΠΈ Π³Π»ΠΈΠΊΠΎΠΊΠΎΡΡΠΈΠΊΠΎΠΈΠ΄ΠΈ. ΠΠ°ΡΠ΅ΡΠΈΡΠ°Π» ΠΈ ΠΌΠ΅ΡΠΎΠ΄ΠΈ: ΠΠ΅Π° Π°Π½Π°Π»ΠΈΠ·ΠΈΡΠ°Π½ΠΈ 46 ΠΏΠ°ΡΠΈΠ΅Π½ΡΠΊΠΈ. ΠΠ°Ρ ΡΠΈΡΠ΅ Π±Π΅ΡΠ΅ Π½Π°ΠΏΡΠ°Π²Π΅Π½o ΡΠ½ΠΈΠΌΠ°ΡΠ΅ Π·Π° Π΅Π²Π°Π»ΡΠ°ΡΠΈΡΠ° Π½Π° ΠΎΡΡΠ΅ΠΎΠΏΠΎΡΠΎΠ·Π° ΡΠΎ Π°ΠΏΠ°ΡΠ°Ρ Π·Π° Π΄Π²ΠΎΡΠ½ΠΎ-Π΅Π½Π΅ΡΠ³Π΅ΡΡΠΊΠ° x-Π·ΡΠ°ΡΠ½Π° aΠΏΡΠΎΡΠΏΡΠΈΠΎΠΌΠ΅ΡΡΠΈΡΠ° - DXA ΡΠΊΠ΅Π½, βLunar iDXAβ, ΠΏΡΠΎΠΈΠ·Π²ΠΎΠ΄ΡΡΠ²ΠΎ Π½Π° GE, ΡΠΎ Π²Π³ΡΠ°Π΄Π΅Π½ ΡΠΎΡΡΠ²Π΅Ρ Π·Π° ΠΏΡΠΎΡΠ΅Π½ΠΊΠ° Π½Π° VF, VFA (Vertebral Fracture Assessment). Π Π΅Π·ΡΠ»ΡΠ°ΡΠΈ: ΠΡΠ΅Π΄Π½ΠΎΡΡΠΈΡΠ΅ Π½Π° ΠΊΠΎΡΠΊΠ΅Π½ΠΈΠΎΡ ΠΌΠΈΠ½Π΅ΡΠ°Π»Π΅Π½ Π΄Π΅Π½Π·ΠΈΡΠ΅Ρ (BMD) Π±Π΅Π° ΡΠΈΠ³Π½ΠΈΡΠΈΠΊΠ°Π½ΡΠ½ΠΎ ΠΏΠΎΠΌΠ°Π»ΠΈ Π²ΠΎ Π³ΡΡΠΏΠ°ΡΠ° ΠΊΠΎΡΠ° ΠΏΡΠΈΠΌΠ°Π»Π° Π³Π»ΠΈΠΊΠΎΠΊΠΎΡΡΠΈΠΊΠΎΠΈΠ΄ΠΈ. Π‘ΠΏΠΎΡΠ΅Π΄ VFA, ΠΊΠ°Ρ 37,0% ΠΎΠ΄ ΠΏΠ°ΡΠΈΠ΅Π½ΡΠΊΠΈΡΠ΅ Π±Π΅ΡΠ΅ ΡΠ΅Π³ΠΈΡΡΡΠΈΡΠ°Π½Π° ΡΡΠ°ΠΊΡΡΡa ΠΎΠ΄ ΡΡΠ΅Π΄Π΅Π½ ΡΡΠ΅ΠΏΠ΅Π½, ΠΊΠ°Ρ 19,6% Π»Π΅ΡΠ½a ΡΡΠ°ΠΊΡΡΡa, a ΡΠ΅ΡΠΊΠ° ΡΡΠ°ΠΊΡΡΡΠ° Π±Π΅ΡΠ΅ ΡΠ΅Π³ΠΈΡΡΡΠΈΡΠ°Π½Π° ΠΊΠ°Ρ ΡΡΠΈ ΠΏΠ°ΡΠΈΠ΅Π½ΡΠΊΠΈ (6,5%). ΠΠ°ΠΊΠ»ΡΡΠΎΠΊ: ΠΠ°Ρ ΠΏΠΎΡΡΠΌΠ΅Π½ΠΎΠΏΠ°ΡΠ·Π½ΠΈΡΠ΅ ΠΏΠ°ΡΠΈΠ΅Π½ΡΠΊΠΈ ΡΠΎ RA ΠΊΠΎΠΈ ΠΏΡΠΈΠΌΠ°Π° ΡΠ΅ΡΠ°ΠΏΠΈΡΠ° ΡΠΎ GC Π±Π΅ΡΠ΅ ΡΠ΅Π³ΠΈΡΡΡΠΈΡΠ°Π½Π° ΠΏΠΎΡΠ΅ΡΡΠ° ΠΏΠΎΡΠ°Π²Π° Π½Π° OP ΠΊΠ°ΠΊΠΎ ΠΈ VF ΡΠΏΠΎΡΠ΅Π΄Π΅Π½ΠΎ ΡΠΎ ΠΎΡΡΠ°Π½Π°ΡΠ°ΡΠ° Π³ΡΡΠΏΠ° ΠΏΠ°ΡΠΈΠ΅Π½ΡΠΊΠΈ ΡΠΎ ΡΠ΅Π²ΠΌΠ°ΡΠΎΠΈΠ΄Π΅Π½ Π°ΡΡΡΠΈΡΠΈΡ. ΠΠ°Ρ ΡΠΈΡΠ΅ ΠΏΠ°ΡΠΈΠ΅Π½ΠΊΠΈ ΡΠΎ RA Π²ΠΎ ΠΌΠ΅Π½ΠΎΠΏΠ°ΡΠ·Π°, ΠΏΠΎΡΡΠ΅Π±Π½ΠΎ Π΅ Π½Π°Π²ΡΠ΅ΠΌΠ΅Π½ΠΎ Π΄Π΅ΡΠ΅ΠΊΡΠΈΡΠ°ΡΠ΅ ΠΈ ΡΡΠ΅ΡΠΌΠ°Π½ Π½Π° ΠΎΡΡΠ΅ΠΎΠΏΠΎΡΠΎΠ·Π°ΡΠ° ΠΈ ΠΏΡΠ΅Π²Π΅Π½ΠΈΡΠ°ΡΠ΅ Π½Π° Π½Π΅ΡΠ·ΠΈΠ½ΠΈΡΠ΅ ΠΊΠΎΠΌΠΏΠ»ΠΈΠΊΠ°ΡΠΈΠΈ
Atorvastatin in Combination with Pegylated Interferon and Ribavirin Provided High Rate of Sustained Virological Response in Patients with Genotype 3 Hepatitis C Virus
Get PDFBACKGROUND: Chronic hepatitis C virus infection represents a more frequent cause of liver cirrhosis and hepatocellular carcinoma. Statins, inhibit HCV replication in vitro, enhance the antiviral effect of the already known antiviral drugs and reduce their resistance.
AIM: To determine the impact of additional therapy (treatment with Atorvastatin 20 mg) to the standard antiviral therapy (pegylated interferon alpha-peg-IFN ΓΒ± and ribavirin) on achieving sustained virological response (SVR).
MATERIAL AND METHODS: In the study which is comparative, open-label, prospective-retrospective, 70 patients diagnosed with chronic hepatitis C virus infection who met criteria for treatment with standard antiviral therapy combined with anti-lipemic therapy (Atorvastatin 20 mg) were included. Patients in the study were divided into two groups: one group of 35 patients receiving combination therapy (Atorvastatin + peg-IFN ΓΒ± + Ribavirin) and another group of 35 patients received only standard antiviral therapy. Those parameters were followed in all patients: genotyping, quantification of the virus, histological assessment of liver inflammation and fibrosis degree (before starting treatment), the presence of steatosis, laboratory analysis: hematology, liver, lipid and carbohydrate status, insulin blood level (the calculation of HOMA-IR) and body mass index (BMI) calculation. The overall treatment of the patients depends from the virus genotype, thus, patients with genotype 1 and 4 received 48 weeks standard antiviral therapy, but patients with genotypes 2 and 3 received 24 weeks of antiviral therapy. SVR was considered an undetectable level of HCV RNA levels 24 weeks after completion of antiviral therapy. The results were statistically analysed, and all results for p < 0.05 were considered statistically significant.
RESULTS: Combination therapy leads to a slightly higher percentage of SVR (85.71%) in patients with chronic hepatitis C versus standard therapy (74.29%), but in a group of patients with genotype 3 this rate of SVR amounting to 95.83%. Combination therapy leads to significant improvement of lipid and glucose status after treatment, and in terms of side effects, there was no appearance of serious adverse events that would be a reason for discontinuation of the therapy.
CONCLUSION: Combination therapy Atorvastatin + pegylated interferon alpha + Ribavirin leads to high rate of SVR of 95.83% in patients with chronic hepatitis C, genotype 3. Statins can be used safely in patients with chronic hepatitis C
