| Literature DB >> 21116816 |
S L Silverman1, A Kriegman, J Goncalves, F Kianifard, T Carlson, E Leary.
Abstract
UNLABELLED: A randomized, double-blind, placebo-controlled study assessed the efficacy of acetaminophen or fluvastatin in preventing post-dose symptoms (increases in body temperature or use of rescue medication) following a single infusion of the intravenous (IV) bisphosphonate zoledronic acid (ZOL). Acetaminophen, but not fluvastatin, significantly reduced the incidence and severity of post-dose symptoms.Entities:
Mesh:
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Year: 2010 PMID: 21116816 PMCID: PMC3132314 DOI: 10.1007/s00198-010-1448-2
Source DB: PubMed Journal: Osteoporos Int ISSN: 0937-941X Impact factor: 4.507
Fig. 1Proportion of patients with fever (clinically significant increase in oral body temperature [1°C or more from baseline and 38.5°C or more overall]) or use of at least one dose of rescue medication during the 3-day period following IV zoledronic acid infusion (intent-to-treat population). Cross-hatching indicates proportion of patients in each group with one or more episodes of fever recorded in the patient diary (no p values shown for the latter comparisons). acet acetaminophen, fluv fluvastatin, plac placebo
Clinically significant increase in oral body temperature, rescue medication use, worsening symptoms, and severe symptoms during the 3-day period following IV zoledronic acid infusion
| Variables | PLAC ( | ACET ( | FLUV ( | |||
|---|---|---|---|---|---|---|
| Number | Percentage (%) | Number | Percentage (%) | Number | Percentage (%) | |
| Clinically significant increase in temperaturea | 28 | 10.5 | 13 | 4.9b | 30 | 11.5 |
| Use of rescue medication | 153 | 57.3 | 102 | 38.6c | 156 | 59.5 |
| Major increase in severity of symptoms | ||||||
| Feeling feverish | 105 | 39.3 | 62 | 23.5c | 104 | 39.7 |
| Headache | 104 | 39.0 | 67 | 25.4c | 115 | 43.9 |
| Aches and pains | 127 | 47.6 | 89 | 33.7c | 121 | 46.2 |
| Severe symptoms (reported at least once) | ||||||
| Feeling feverish | 36 | 13.5 | 20 | 7.6b | 38 | 14.5 |
| Headache | 42 | 15.7 | 18 | 6.8c | 42 | 16.0 |
| Aches and pains | 81 | 30.3 | 56 | 21.2b | 79 | 30.2 |
ACET acetaminophen, FLUV fluvastatin, PLAC placebo
a1°C or more from baseline and 38.5°C or more overall
b p < 0.05 vs. placebo
c p ≤ 0.001 vs. placebo
Fig. 2Change from baseline in a mean body temperature and b VAS scores following IV zoledronic acid infusion in patients who received pretreatment with fluvastatin (fluv), acetaminophen four times daily over 3 days (acet), or placebo (plac)
Serum levels of inflammatory biomarkers
| PLAC ( | ACET ( | FLUV ( | |
|---|---|---|---|
| IL-6 (pg/ml): median (min, max)a | |||
| Baseline | 2.0 (1, 61) | 2.1 (0, 31) | 2.5 (0, 8) |
| 24 h | 14.5 (2, 154) | 9.7 (2, 73) | 14.8 (2, 79) |
| 72 h | 3.9 (1, 160) | 2.8 (1, 56) | 3.5 (2, 79) |
| TNF-alpha (pg/ml): median (min, max)b | |||
| Baseline | 1.9 (1, 5) | 1.9 (1, 9) | 1.8 (1, 7) |
| 24 h | 3.8 (1, 9) | 3.7 (2, 11) | 4.1 (2, 12) |
| 72 h | 2.6 (1, 7) | 2.2 (0, 12) | 3.8 (1, 9) |
| IFN-gamma (pg/ml): median (min, max)c | |||
| Baseline | 0.6 (1, 4) | 0.6 (1, 4) | 0.6 (1, 2) |
| 24 h | 75.5 (1, 363) | 40.7 (1, 872) | 98.2 (4, 3479) |
| 72 h | 2.0 (1, 24) | 1.6 (1, 12) | 3.1 (1, 10) |
| hs-CRP (mg/l): median (min, max)d | |||
| Baseline | 2.3 (0, 13) | 2.3 (1, 8) | 1.8 (0, 49) |
| 24 h | 8.0 (0, 81) | 4.7 (1, 45) | 7.8 (0, 77) |
| 72 h | 25.1 (0, 89) | 19.3 (1, 133) | 20.2 (0, 71) |
ACET acetaminophen, FLUV fluvastatin, hs-CRP highly sensitive C-reactive protein, PLAC placebo
aIL-6 (pg/ml) normal reference range: 0.51–4.92
bTNF-alpha (pg/ml) normal reference range: less than 1.86
cIFN-gamma (pg/ml) normal reference range: less than 1.9
dhs-CRP (mg/l) normal reference range: less than 3.0
Fig. 3Change from baseline in serum levels of a IL-6, b TNF-alpha, c IFN-gamma, and d hs-CRP following IV zoledronic acid infusion in a subset of 96 patients receiving treatment with placebo (plac), acetaminophen (acet), or fluvastatin (fluv). Measurements were taken at baseline and at 24 and 72 h post-infusion. hs-CRP highly sensitive C-reactive protein, IFN interferon, IL interleukin, TNF tumor necrosis factor