109 research outputs found
Sex steroids, carcinogenesis, and cancer progression
The relationship between sex steroids and cancer has been studied for more than a century. Using an original intact cell analysis, we investigated sex steroid metabolism in a panel of human cancer cell lines, either hormone responsive or unresponsive, originating from human breast, endometrium, and prostate. We found that highly divergent patterns of steroid metabolism exist and that the catalytic preference (predominantly reductive or oxidative) is strictly associated with the steroid receptor status of cells. We explored intra-tissue concentrations and profiles of estrogens in a set of human breast tumors as compared to normal mammary tissues, also in relation to their estrogen receptor status. In particular, we showed that, with hydroxyestrogens representing the majority of all tissue estrogens, concentrations of individual metabolites, as well as their ratios, significantly differ when comparing normal tissue with cancer tissues or when they are related to the overall survival of cancer patients. © 2004 New York Academy of Sciences
Androgen metabolism and inhibition of interleukin-1 synthesis in primary cultured human synovial macrophages
The presence of androgen receptors on synovial macrophages in human normal and rheumatoid synovial tissues has been described previously. It is now reported that primary cultured human macrophages obtained from normal and rheumatoid synovia express functional androgen receptors. We have investigated the capacity of cultured macrophages to metabolize androgens and have found that these cells were capable of metabolizing testosterone to the bioactive metabolite dihydrotestosterone. Therefore, macrophages contain the key enzymes of steroidogenesis, in particular the 5α-treductase. Furthermore, interleukin-1β production by primary cultured rheumatoid macrophages was analysed, following exposure to physiological concentrations of testosterone (10−8 M). A significant decrease of IL-1β levels in conditioned media after 24 h (p < 0.05) was observed. It is concluded that androgens may act directly on human macrophages and may interfere with some of their functions via receptor-dependent mechanisms
Combined Docking and Quantum Chemical Study on CYP-mediated Metabolism of Estrogens in Man
Long-term exposure
to estrogens seriously increases the incidence
of various diseases including breast cancer. Experimental studies
indicate that cytochrome P450 (CYP) enzymes catalyze the bioactivation
of estrogens to catechols, which can exert their harmful effects via
various routes. It has been shown that the 4-hydroxylation pathway
of estrogens is the most malign, while 2-hydroxylation is considered
a benign pathway. It is also known experimentally that with increasing
unsaturation of ring B of estrogens the prevalence of the 4-hydroxylation
pathway significantly increases. In this study, we used a combination
of structural analysis, docking, and quantum chemical calculations
at the B3LYP/6-311+G* level to investigate the factors that influence
the regioselectivity of estrogen metabolism in man. We studied the
structure of human estrogen metabolizing enzymes (CYP1A1, CYP1A2,
CYP1B1, and CYP3A4) in complex with estrone using docking and investigated
the susceptibility of estrone, equilin, and equilenin (which only
differ in the unsaturation of ring B) to undergo 2- and 4-hydroxylation
using several models of CYP enzymes (Compound I, methoxy, and phenoxy
radical). We found that even the simplest models could account for
the experimental difference between the 2- and 4- hydroxylation pathways
and thus might be used for fast screening purposes. We also show that
reactivity indices, specifically in this case the radical and nucleophilic
condensed Fukui functions, also correctly predict the likeliness of
estrogen derivatives to undergo 2- or 4-hydroxylation
Intervertebral disc and endplate cell characterisation highlights annulus fibrosus cells as the most promising for tissue-specific disc degeneration therapy
Degenerative processes of the intervertebral disc (IVD) and cartilaginous endplate lead to chronic spine pathologies. Several studies speculated on the intrinsic regenerative capacity of degenerated IVD related to the presence of local mesenchymal progenitors. However, a complete characterisation of the resident IVD cell populations, particularly that isolated from the endplate, is lacking. The purpose of the present study was to characterise the gene expression profiles of human nucleus pulposus (NPCs), annulus fibrosus (AFCs) and endplate (EPCs) cells, setting the basis for future studies aimed at identifying the most promising cells for regenerative purposes. Cells isolated from NP, AF and EP were analysed after in vitro expansion for their stemness ability, immunophenotype and gene profiles by large-scale microarray analysis. The three cell populations shared a similar clonogenic, adipogenic and osteogenic potential, as well as an immunophenotype with a pattern resembling that of mesenchymal stem cells. NPCs maintained the greatest chondrogenic potential and shared with EPCs the loss of proliferation capability during expansion. The largest number of selectively highly expressed stemness, chondrogenic/tissue-specific and surface genes was found in AFCs, thus representing the most promising source of tissue-specific expanded cells for the treatment of IVD degeneration
- …