Osteoporosis Clinical Trial
Official title:
Bone Loss and Immune Reconstitution in HIV/AIDS (BLIR-HIV)
With the increasing age of people living with HIV/AIDS, age-induced osteoporosis is likely to be compounded by HIV/AIDS and HAART-associated bone loss. Mechanistically, osteoclasts the cells responsible for bone resorption form under the influence of the key osteoclastogenic cytokine receptor activator of nuclear factor kappa-Β ligand (RANKL). The osteoclastogenic and proresorptive activities of RANKL are moderated by its physiological decoy receptor osteoprotegerin (OPG). Imbalance in the ratio of RANKL to OPG alters osteoclastic bone resorption and lead to osteoporosis. Activated T- and B-cells are a major source of RANKL, while normal physiological B-cells are a major source of OPG. T-cells regulate the production of OPG by B-cells. Thus changes in the immune system induced by HIV/AIDS and/or by HAART could affect B-cell and T-cells RANKL and OPG production. Indeed, data from our group shows that in an animal model of HIV/AIDS, the HIV-1 Transgenic rat, the development of osteoporosis is recapitulated as observed in HIV-infected patients, and B-cell OPG and RANKL production are concurrently down regulated and upregulated respectively. Furthermore, preliminary data in HIV-infected subjects suggests dramatic acute upswing in bone resorption following HAART initiation that peaks at 12 weeks and then declines. Based on these findings, the investigators hypothesize HAART associated bone loss is driven by immune reconstitution. Because this effect of HAART is dramatic in magnitude but short in duration, the investigators propose to apply antiresorptive agent (zoledronic acid, reclast®) to specifically spare patients from this dramatic but acute bone damage.
In a prospective, blinded placebo-controlled randomized trial, treatment naïve HIV-infected
subjects initiating HAART will be assigned to HAART + zoledronic acid or HAART + placebo.
Serial assessment of serum levels of bone markers, cellular expression of OPG/RANKL and other
cytokines, cellular immune activation markers, serum bone regulating hormones, and bone
mineral density (BMD) by dual-energy X-ray absorptiometry (DXA) scan will be undertaken at
pre-defined time points from baseline through week 144 of HAART.
In the primary analysis, changes in serum C-Terminal Telopeptide (CTx) level, BMD, and
cellular OPG/RANKL expression from baseline through week 24 will be quantitated and
subsequently compared between treatment arms. In addition, the impact of zoledronic acid
administration on these covariates will be assessed at various study time points. The
relationship between OPG/RANKL expression, immune activation, serum bone regulating hormonal
levels, and bone turnover will be evaluated.
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