4 research outputs found
Hormonal (Im)Balance and Reproductive System’s Disorders in Transplant Recipients—A Review
The rising need for treatment of end stage of organ failure results in an increased number of graft recipients yearly. The most commonly transplanted organs are kidney, heart, liver, bone marrow, lung and skin. The procedure of transplantation saves and prolongs the lives of chronically ill patients or at least improves the quality. However, following transplantation recipients must take immunosuppressive drugs on a daily basis. Usually, the immunosuppressive therapy comprises two or three drugs from different groups, as the mechanism of their action varies. Although the benefits of intake of immunosuppressants is undeniable, numerous side effects are associated with them. To different extents, they are neurotoxic, nephrotoxic and may influence the function of the reproductive system. Nowadays, when infertility is an urgent problem even among healthy pairs, transplant recipients face the problem of disturbance in the hypothalamic−pituitary axis. This review will provide an overview of the most common disturbances among the concentration of sex-related hormones in recipients of both sexes at different ages, including sexually immature children, adults of reproductive age as well as elderly women and men. We have also focused on the numerous side effects of immunosuppressive therapy regarding function and morphology of reproductive organs both in males and females. The current review also presents the regimen of immunosuppressive therapy and time since transplantation
The Effects of Short-Term Immunosuppressive Therapy on Redox Parameters in the Livers of Pregnant Wistar Rats
Immunosuppressive drugs are widely used to avoid graft rejection, but they are also known to be strongly hepatotoxic. The goal of the current study was to determine: (i) the immunoexpression of SOD1, CAT, GPX1; (ii) the concentration of MDA, GSH; (iii) the activity of SOD, CAT, GPX, in the native liver of a pregnant female rats undergoing immunosuppressive therapy. The study was based on archival material obtained from Department of Nephrology, Transplantology and Internal Medicine of the Independent Public Clinical Hospital No. 2 at the Pomeranian Medical University in Szczecin, Poland. The study was carried out on 32 female rats exposed to oral administration of immunosuppressants two weeks before and during pregnancy. The percentage of SOD1 immunopositive hepatocytes in rats treated with cyclosporine A, mycophenolate mofetil, everolimus, and glucocorticosteroid was significantly elevated above that of the control rats. The concentration of MDA in the liver of animals exposed to cyclosporine A, everolimus, and glucocorticosteroid was significantly higher than in other groups. Among the groups of dams treated with immunosuppressive drugs, the highest significant concentration of GSH was found in the livers of rats treated with cyclosporine A, mycophenolate mofetil and glucocorticosteroid. Immunosuppressive therapy during pregnancy affects the oxidoreductive balance in the livers of rats, depending on the regimen used
Modulatory effect of inulin with soya isoflavones on plasma lipid profile and liver SCD-18 index in rats with induced type-2 diabetes mellitus
Obesity and type-2 diabetes are often
associated with nonalcoholic fatty liver disease
(NAFLD). Soya isoflavones act as antidiabetic agents
and protect against NAFLD. There are data suggesting
that inulin may increase the plasma concentration and
effect of soya isoflavones. The aim of the present study
was to compare the effect of soya isoflavones, as
opposed to the effect of soya isoflavones with inulin, on
plasma lipid profile, liver morphology, and liver fatty
acids in rats with induced type-2 diabetes mellitus.
Data were collected on thirty-six male Sprague-
Dawley rats divided into control and diabetic groups.
Animals in the diabetic (DM) group were on a high-fat
diet and were injected with low doses of streptozotocin.
Animals in the control groups were fed a regular diet and
were injected with a buffer. After the injections, the
animals were divided into three groups of nondiabetic
rats (nDM)-controls (c-nDM), rats treated with
isoflavones (IS-nDM), and rats treated with isoflavones
plus inulin (IS+IN-nDM)-and three parallel diabetic
(DM) subgroups: controls (c-DM), rats treated with
isoflavone (IS-DM), and rats treated with isoflavones
plus inulin (IS+IN-DM). Hepatic steatosis and fibrosis
were examined using hematoxylin-eosin staining and
Mallory’s trichrome methods respectively. Liver fatty
acids were extracted and analyzed by gas
chromatography. A lipid blood test was performed.
The study showed significant changes in liver fatty
acids, liver morphology, and plasma lipid profile. The
estimated SCD-18 index significantly decreased in both
the control and DM groups after isoflavone
supplementation. The level of liver steatosis and fibrosis
also decreased after isoflavone supplementation in the
DM groups. The plasma lipid profile showed increased
levels of HDL-C after isoflavone supplementation in the
DM groups.
These results support the protective use of
isoflavones in liver steatosis and as beneficial to plasma
lipid profile in individuals with diabetes. A novelty of
this work is its comparison of supplementation using
soya isoflavones with supplementation using both soya
isoflavones and inulin. Surprisingly, additional
supplementation with inulin modulates the positive
effect of isoflavone