Histological and immunohistochemical effects of Curcuma longa on activation of rat hepatic stellate cells after cadmium induced hepatotoxicity

The liver is a target for toxic chemicals such as cadmium (Cd). When the liver is damaged, hepatic stellate cells (HSC) are activated and transformed into myofibroblast-like cells, which are responsible for liver fibrosis. Curcuma longa has been reported to exert a hepato-protective effect under various pathological conditions. We investigated the effects of C. longa administration on HSC activation in response to Cd induced hepatotoxicity. Forty adult male albino rats were divided into: group 1 (control), group 2 (Cd treated), group 3 (C. longa treated) and group 4 (Cd and C. longa treated). After 6 weeks, liver specimens were prepared for light and electron microscopy examination of histological changes and immunohistochemical localization of alpha smooth muscle actin (αSMA) as a specific marker for activated HSC. Activated HSC with a positive αSMA immune reaction were not detected in groups 1 and 3. Large numbers of activated HSC with αSMA immune reactions were observed in group 2 in addition to Cd induced hepatotoxic changes including excess collagen deposition in thickened portal triads, interlobular septa with hepatic lobulation, inflammatory cell infiltration, a significant increase in Kupffer cells and degenerated hepatocytes. In group 4, we observed a significant decrease in HSC that expressed αSMA with amelioration of the hepatotoxic changes. C. longa administration decreased HSC activation and ameliorated hepatotoxic changes caused by Cd in adult rats.     

Inhibition of interferon secretion by vinblastine

The plant alkaloids vinblastine and colchicine are known to arrest cells in mitosis by virtue of their binding to spindle protein. These drugs are also capable of binding to microtubule protein and causing these structures to disaggregate into nonfunctional subunits (1, 2). Microtubular structures are thought to be involved in the secretory process of a number of proteins including insulin (7), collagen (4), and thyroid hormone (12). In this report we present our findings on the effects of these two drugs on the synthesis and secretion of interferon in a high producing human foreskin fibroblast strain (FS-4) (11).     

Neuronal organization of the periaqueductal gray matter in the cat midbrain

It is shown by the use of Golgi's method in Antonova's modification that the neuronal structure of the periaqueductal gray matter (PGM) in the frontal plane is characterized by the presence of small and medium-sized cells of "reticular type," which can be subdivided into three types: fusiform, triangular, and multipolar. On the basis of the visual distribution of these types of neurons and also of statistical analysis of 800 identified neurons, two regions can be distinguished: medial, directly surrounding the aqueduct of Sylvius, containing small neurons, among which the fusiform kind predominate significantly (P<0.001), and a lateral region with larger neurons, with significantly (P<0.001) more triangular cells. Neurons in the medial region show a characteristic and strong (P<0.001) tendency for their dendrites to be oriented toward the lumen of the aqueduct, and through them the physiologically active substances of the CSF may influence the functional activity of neurons of PGM.Central Research Institute of Reflex Therapy, Moscow City Council Main Health Board, Moscow. Translated from Neirofiziologiya, Vol. 16, No. 6, pp. 773–777, November–December, 1984.     

Comparative characteristics of activity in grafted and intact neocortex in slice preparations

Background single unit activity and mixed single and multiunit responses to electrical stimulation of rat's embryonic cortex grafted into the somatosensory cortex of adult rats were investigated in a slice preparation. The relative number of neurons exhibiting background activity in the grafts was higher than in slices of intact cortex (23 and 6%, respectively), however, the portion of neurons responding to electrical stimulation of areas of neighboring neocortex in the recipient was lower than in intact cortex. The latent periods of population responses in the grafts were consistently longer than in those in intact neocortex (19.4±5 and 5.8±1.1 msec, respectively), although the extreme values coincided. The duration of population responses in the grafts was approximately an order of magnitude longer. The data presented suggests the existence of local connections between the graft and the brain of the recipient and shows weakness of inhibitory processes in the grafts. A functional integration of graft and brain in recipients with craniocerebral trauma was demonstrated.Institute of Biophysics, Academy of Sciences of the USSR, Pushchino, Moscow. Institute of Neurosurgery, Ministry of Public Health of the Ukrainian SSR, Kiev. Translated from Neirofiziologiya, Vol. 23, No. 3, pp. 273–280, May–June, 1991.     

Changes in pain reactions and 3H-naloxone binding to opiate receptors of the hypothalamus and midbrain in rats after repeated swimming in cold water

The dynamics of nociceptive reactions and character of 3H-naloxone binding to hypothalamus and midbrain synaptic membranes were studied in rats subjected to repeated cold swim stress (3 min. daily during 3, 5 and 15 days). It was shown that an increase of latencies of background nociceptive reactions (hot-plate and tail-flick tests) was accompanied by an ambiguous changes of kinetic parameters of 3H-naloxone binding in the studied brain structures. The results suggest that an increase of antinociceptive systems tone under repeated cold swim stress may be caused by a dynamic transformation of opiate u-receptor apparatus in various brain structures.     

Influence of a natural and a synthetic inhibitor of factor XIIIa on fibrin clot rheology

We investigated the origins of greater clot rigidity associated with FXIIIa-dependent cross-linking. Fibrin clots were examined in which cross-linking was controlled through the use of two inhibitors: a highly specific active-center-directed synthetic inhibitor of FXIIIa, 1,3-dimethyl-4,5-diphenyl-2[2(oxopropyl)thio]imidazolium trifluoromethylsulfonate, and a patient-derived immunoglobulin directed mainly against the thrombin-activated catalytic A subunits of thrombin-activated FXIII. Cross-linked fibrin chains were identified and quantified by one- and two-dimensional gel electrophoresis and immunostaining with antibodies specific for the alpha- and gamma-chains of fibrin. Gamma-dimers, gamma-multimers, alpha(n)-polymers, and alpha(p)gamma(q)-hybrids were detected. The synthetic inhibitor was highly effective in preventing the production of all cross-linked species. In contrast, the autoimmune antibody of the patient caused primarily an inhibition of alpha-chain cross-linking. Clot rigidities (storage moduli, G') were measured with a cone and plate rheometer and correlated with the distributions of the various cross-linked species found in the clots. Our findings indicate that the FXIIIa-induced dimeric cross-linking of gamma-chains by itself is not sufficient to stiffen the fibrin networks. Instead, the augmentation of clot rigidity was more strongly correlated with the formation of gamma-multimers, alpha(n)-polymers, and alpha(p)gamma(q)-hybrid cross-links. A mechanism is proposed to explain how these cross-linked species may enhance clot rigidity.