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Items: 5

1.
FIG 1

FIG 1. From: Limited Activity of Clofazimine as a Single Drug in a Mouse Model of Tuberculosis Exhibiting Caseous Necrotic Granulomas.

CFZ was highly effective at reducing bacterial CFU in BALB/c mice (A) in the lungs (filled symbols) and in the spleen (open symbols). In contrast, CFZ activity was significantly attenuated in the lungs of C3HeB/FeJ mice (B), while comparable activity was observed in the spleen. Data represent mean log10 CFU counts ± SEM; detection limit = 50 CFU. *, P < 0.001.

Scott M. Irwin, et al. Antimicrob Agents Chemother. 2014 Jul;58(7):4026-4034.
2.
FIG 4

FIG 4. From: Limited Activity of Clofazimine as a Single Drug in a Mouse Model of Tuberculosis Exhibiting Caseous Necrotic Granulomas.

CFZ was effective in immunocompromised GKO mice. Gamma interferon gene-disrupted mice were treated for 9 days with 20 mg/kg CFZ beginning on day 13 postinfection. CFZ reduced bacterial loads in the lungs (A) by 3.1 log10 CFU and in the spleens (B) by 3.95 log10 CFU compared to results for untreated controls. Data represent mean log10 CFU counts ± SEM; detection limit = 50 CFU. *, P < 0.001.

Scott M. Irwin, et al. Antimicrob Agents Chemother. 2014 Jul;58(7):4026-4034.
3.
FIG 5

FIG 5. From: Limited Activity of Clofazimine as a Single Drug in a Mouse Model of Tuberculosis Exhibiting Caseous Necrotic Granulomas.

CFZ activity decreased as the oxygen concentration decreased. CFZ was highly effective in vitro under high aeration (A). Under low aeration (B), CFZ had reduced but demonstrable activity despite similar bacterial growth. However, CFZ activity was lowest under completely anaerobic conditions achieved in the rapid anaerobic dormancy (RAD) culture model (C). CFZ was added at a final concentration of 50 mg/ml. Data represent mean log10 CFU counts ± SD; detection limit = 50 CFU. *, P < 0.001.

Scott M. Irwin, et al. Antimicrob Agents Chemother. 2014 Jul;58(7):4026-4034.
4.
FIG 3

FIG 3. From: Limited Activity of Clofazimine as a Single Drug in a Mouse Model of Tuberculosis Exhibiting Caseous Necrotic Granulomas.

Attenuation of CFZ activity was related to pulmonary pathology. Administration of CFZ to C3HeB/FeJ mice prior to the formation of well-defined pulmonary granulomas (A) (3 weeks postinfection) reconstituted bactericidal activity in the lungs (filled symbols). Initiation of CFZ treatment after the formation of well-defined pulmonary granulomas with significant caseous necrosis (B) (7 weeks postinfection) resulted in significant attenuation of bactericidal activity in C3HeB/FeJ mice. CFZ exhibited comparable activity in the spleens (open symbols) of C3HeB/FeJ mice, which lack well-defined granulomas and caseous necrosis. Data represent mean log10 CFU counts ± SEM; detection limit = 50 CFU. *, P < 0.001; †, P < 0.05.

Scott M. Irwin, et al. Antimicrob Agents Chemother. 2014 Jul;58(7):4026-4034.
5.
FIG 2

FIG 2. From: Limited Activity of Clofazimine as a Single Drug in a Mouse Model of Tuberculosis Exhibiting Caseous Necrotic Granulomas.

Pathological progression of disease in BALB/c and C3HeB/FeJ mice. Cellular aggregates in the lungs of BALB/c mice at 3 weeks postinfection (A) (magnification, ×100) were composed predominantly of macrophage cells with distinct regions of lymphocytic perivascular and peribronchiolar cuffing (arrows). C3HeB/FeJ mice at 3 weeks postinfection (B) (×100) exhibited cellular lesions composed predominantly of neutrophilic clusters (arrows) and epithelioid macrophages, with evidence of an early fibrotic response. By 7 weeks (C) (×40), the cellular aggregates in BALB/c mice formed loosely organized inflammatory granulomas lacking a well-defined collagen rim. In contrast, by 7 weeks (D) (×40), highly organized granulomas had formed in the lungs of C3HeB/FeJ mice possessing a hypoxic neutrophilic central caseous necrotic core region (CN) and a layer of foamy macrophages (FM) delineated by a collagen rim (arrows) that encapsulated the granuloma structure. By 7 weeks postinfection, no caseating necrotic granulomas were observed in the spleens of BALB/c (E) (×40) or C3HeB/FeJ (F) (×40) mice.

Scott M. Irwin, et al. Antimicrob Agents Chemother. 2014 Jul;58(7):4026-4034.

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