HIV-1-associated disruption of intestinal homeostasis is a major factor
contributing to chronic immune activation and inflammation. Dendritic cells
(DCs) are crucial in maintaining intestinal homeostasis, but the impact of HIV-1
infection on intestinal DC number and function has not been extensively studied.
We compared the frequency and activation/maturation status of colonic myeloid DC
(mDC) subsets (CD1c+ and CD1cneg) and plasmacytoid DCs in
untreated HIV-1-infected subjects with uninfected controls. Colonic mDCs in
HIV-1-infected subjects had increased CD40 but decreased CD83 expression, and
CD40 expression on CD1c+ mDCs positively correlated with mucosal
HIV-1 viral load, with mucosal and systemic cytokine production, and with
frequencies of activated colon and blood T cells. Percent of
CD83+CD1c+ mDCs negatively correlated with frequencies
of IFN-γ-producing colon CD4+ and CD8+ T cells.
CD40 expression on CD1c+ mDCs positively associated with abundance of
high prevalence mucosal Prevotella copri and P.
stercorea, but negatively associated with a number of low
prevalence mucosal species including Rumminococcus bromii.
CD1c+ mDC cytokine production was greater in response to
in vitro stimulation with Prevotella
species relative to R. bromii. These findings suggest that
during HIV infection, colonic mDCs become activated upon exposure to mucosal
pathobiont bacteria leading to mucosal and systemic immune activation.
Among 162 young female family planning clients at four school-based health centers, a step-wise regression analysis shows that students' consistency of contraceptive use is associated with only a few specific service and provider characteristics. For example, clients who have more contacts with the family planning program use contraceptives more consistently than those with fewer contacts. On the other hand, young women whose follow-up visits are scheduled to occur within one month of their previous visit are less consistent contraceptive users than other clients. Contraceptive use is not related to whether contraceptives are dispensed on site, whether health education and counseling are provided by a health educator, whether contraceptive services are part of a comprehensive array of services that include medical or counseling services, or whether a family planning visit results in the dispensing of contraceptives or a prescription for contraceptives.
The tumour-bearing state is known to induce immune dysfunction that contributes to increased infectious complications and tumour progression. However, the mechanisms underlying this immunosuppression remain unclear. This study investigated in a murine model the effects of melanoma growth on nitric oxide (NO) production by peritoneal macrophages in vivo and in vitro. B16 and K1735 melanoma cells were inoculated subcutaneously into C57BL/6 and C3H/HeN mice, respectively. Stimulated NO production by elicited peritoneal macrophages was examined in control and melanoma- bearing mice. An in vitro system was established to assess the effects of co-culturing melanoma cells (B16 and K1735) or melanoma-conditioned medium with normal peritoneal macrophages on subsequent NO production. NO production was significantly suppressed in macrophages from melanoma-bearing mice. Co-culture of normal macrophages with melanoma cells in a transwell system or with melanoma-conditioned media in vitro reproduced the defects observed in vivo without affecting macrophage viability, pointing to a melanoma-derived product as the basis for the observed suppression of NO production. This inhibition required RNA and protein synthesis and was dose and time dependent. Using inhibition profiles and neutralizing antibodies, it was demonstrated that this melanoma inhibitory activity was distinct from known NO inhibitors. Preliminary characterization attributed this activity to a melanoma-secreted protein moiety.
Leptin may be an important mediator of weight loss and decreased food intake in PEM. Elevated serum leptin in PEM may be secondary to elevated serum corticosterone, with other factors inherent in the host response to protein restriction also contributing to elevated serum leptin.
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