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1 nfective dose of 10(4)B. anthracis cells for inhalation anthrax.
2 ely devoid of virulence, in a mouse model of inhalation anthrax.
3 ternative clinical treatment regimen against inhalation anthrax.
4 the incubation period distribution for human inhalation anthrax.
5 that accurately predict the effects of human inhalation anthrax.
6 effective emergency therapy of postexposure inhalation anthrax.
7 racis may be critical in the early stages of inhalation anthrax.
8 AD is highly attenuated in a mouse model for inhalation anthrax.
9 0-4) for injection to 7 days (IQR, 4-9) for inhalation anthrax.
11 lete solution for population protection from inhalation anthrax and has been associated with concerns
12 the onset of symptoms in all 6 survivors of inhalation anthrax and in 7 of 11 survivors of cutaneous
13 ients with bioterrorism-related cutaneous or inhalation anthrax and in a patient with laboratory-acqu
18 F detection as a tool for early diagnosis of inhalation anthrax before the onset of fulminant systemi
19 cells were detectable in all 6 survivors of inhalation anthrax but in only 2 of 7 patients with cuta
20 hylococcus aureus hematogenous pneumonia and inhalation anthrax but no activity against Streptococcus
22 toxin may play a role in the pathogenesis of inhalation anthrax by facilitating the dissemination of
23 Systemic sepsis, most often associated with inhalation anthrax, can cause massive ascites, electroly
24 % (CI, 96% to 100%), respectively, when only inhalation anthrax cases or higher-quality case reports
25 f-life confer significant protection against inhalation anthrax despite their lack of Fc regions.
28 amase-expressing bacteria) was evaluated for inhalation anthrax in cynomolgus macaques in 2 studies.
31 To better understand the pathogenesis of an inhalation anthrax infection, we propose a two-compartme
37 us in the two most accepted animal models of inhalation anthrax, nonhuman primates and rabbits, but r
40 oxins in a New Zealand White rabbit model of inhalation anthrax; survival following a lethal aerosoli
41 the site of entry for Bacillus anthracis in inhalation anthrax, the deadliest form of the disease.
43 with 1 or more antimicrobials; patients with inhalation anthrax without meningitis fared better with
45 emination and lethality in a murine model of inhalation anthrax, yet the roles for the toxins during