| Literature DB >> 17961258 |
Asunción Mejías1, Susana Chávez-Bueno, Martin B Raynor, John Connolly, Peter A Kiener, Hasan S Jafri, Octavio Ramilo.
Abstract
Motavizumab (MEDI-524) is a monoclonal antibody with enhanced neutralizing activity against RSV. In mice, motavizumab suppressed RSV replication which resulted in significant reduction of clinical parameters of disease severity. We evaluated the effect of motavizumab on the local and systemic immune response induced by RSV in the mouse model. Balb/c mice were intranasally inoculated with 106.5 PFU RSV A2 or medium. Motavizumab was given once intraperitoneally (1.25 mg/mouse) as prophylaxis, 24 h before virus inoculation. Bronchoalveolar lavage (BAL) and serum samples were obtained at days 1, 5 (acute) and 28 (long-term) post inoculation and analyzed with a multiplex assay (Beadlyte Upstate, NY) for simultaneous quantitation of 18 cytokines: IL-1alpha, IL-1beta, IL-2, IL-3, IL-4, IL-5, IL-6, KC (similar to human IL-8), IL-10, IL-12p40, IL-12p70, IL-13, IL-17, TNF-alpha, MCP-1, RANTES, IFN-gamma and GM-CSF. Overall, cytokine concentrations were lower in serum than in BAL samples. By day 28, only KC was detected in BAL specimens at low concentrations in all groups. Administration of motavizumab significantly reduced (p < 0.05) BAL concentrations of IL-1alpha, IL-12p70 and TNF-alpha on day 1, and concentrations of IFN-gamma on days 1 and 5 compared with RSV-infected untreated controls. In the systemic compartment, the concentrations of IL-10, IFN-gamma and KC were significantly reduced in the motavizumab-treated mice compared with the untreated controls. In summary, prophylactic administration of motavizumab was associated with significant reductions on RSV replication and concentrations of cytokine and chemokines, which are likely related to the improvement observed in clinical markers of disease severity.Entities:
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Year: 2007 PMID: 17961258 PMCID: PMC2222633 DOI: 10.1186/1743-422X-4-109
Source DB: PubMed Journal: Virol J ISSN: 1743-422X Impact factor: 4.099
Figure 1Effect of the anti-RSV mAb (motavizumab) on pulmonary function. Airway obstruction was assessed by whole body plethysmograph by measuring basal Penh daily during the first two weeks after infection and weekly up to day 28. Values represent median; errors bars, 25th–75th percentile. Each group consisted of 8 mice. Results of two separate experiments are shown. * p < 0.001 by Kruskal-Wallis ANOVA on ranks for comparison between RSV-infected untreated, sham inoculated controls and RSV-infected treated with motavizumab at -24 h.
BAL/serum cytokine concentrations (pg/mL) in RSV infected mice treated with motavizumab compared with untreated RSV infected controls on day 1 after inoculation. Each group consisted of 4 samples randomly selected from two independent experiments.
| 67.16 ± (24.6) | 28.01 ± (13.8) | ND | ND | --- | ||
| 1930.68 ± (716.6) | 1088.12 ± (307.8) | 0.07 | 381.83 (341.0–554.8) | 230.65 (217.43–298.83) | 0.6 | |
| 1952.10 ± (999.05) | 671.66 ± (340.4) | 0.051 | ND | ND | --- | |
| 39.29 ± (27.0) | 14.47 ± (7.8) | 0.1 | 102.23 ± (22.5) | 16.78 ± (13.56) | ||
| 2290.90 ± (1100.2) | 279.03 ± (204.7) | ND | ND | --- | ||
| 101.42 (45.7–144.9) | 25.14 (22.1–34.0) | 0.1 | ND | ND | --- | |
| 44.14 ± (13.5) | 22.59 ± (8.7) | 45.85 ± (17.5) | 23.75 ± (16.1) | 0.16 | ||
| 3967.43 (2039.8–5795.3) | 1303.57 (946.4–1657.1) | 0.1 | 215.86 ± (125.8) | 37.63 ± (32.5) | ||
| 2580.89 ± (1413.6) | 821.79 ± (290.13) | 0.051 | 91.39 (45.43–135.31) | 31.17 (18.97–35.85) | 0.2 | |
| 477.52 (231.53–831.92) | 182.78 (179.4–214.3) | 0.3 | 266.88 ± (74.4) | 119.70 ± (143.5) | 0.16 | |
| 289.75 ± (114.0) | 76.28 ± (29.1) | ND | ND | --- | ||
| ND | ND | --- | 20.68 (11.94–31.85) | 10.67 (10.06–12.03) | 0.2 | |
Note: Data are shown as mean ± SD, or medians and 25–75% range as appropriate according to whether they were normally distributed. ND (non-detected)
BAL/serum cytokine concentrations in RSV infected mice treated with motavizumab compared with untreated RSV infected controls on day 5 after inoculation. Each group consisted of 4 samples randomly selected from two independent experiments.
| 1291.29 ± (561.3) | 640.84 ± (388.8) | 116.58 ± (43.1) | 28.29 ± * (35.7) | |||
| 291.10 ± (128.6) | 132.0 ± (105.8) | 0.15 | 311.95 ± (78.3) | 343.26 ± (81.2) | 0.6 | |
| 118.82 ± (28.3) | 48.50 ± (51.9) | 0.055 | ND | ND | --- | |
| 59.7 ± (52.91) | 25.68 ± (18.5) | 0.3 | 15.18 (10.0–71.9) | 23.28 (15.18–48.82) | 0.6 | |
| 13.65 (10.32–17.35) | 10.0 (10.0–11.18) | 0.2 | ND | ND | --- | |
| ND | ND | --- | 39.72 ± (20.6) | 38.07 ± (5.8) | 0.7 | |
| 209.9 ± (88.8) | 117.75 ± (54.2) | 0.12 | 32.54 ± (27.96) | 25.82 ± (19.6) | 0.7 | |
| 101.38 ± (51.22) | 30.46 ± (28.87) | 0.052 | ND | ND | ND | |
| 34.63 ± (34.59) | 52.25 ± (54.3) | 0.6 | 180.66 ± (87.03) | 126.09 ± (58.3) | 0.4 | |
| 12.59 ± (3.05) | 13.84 ± (3.7) | 0.6 | ND | ND | ND | |
| ND | ND | --- | 13.02 (10.0–22.98) | 10.61 (10.0–11.77) | 0.5 | |
Note: Data are shown as mean ± SD, or medians and 25–75% range as appropriate according to whether they were normally distributed. ND (non-detected).