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1 cine for efficacy in a BALB/c mouse model of vaginal infection.
2 rm birth rates in a mouse model of ascending vaginal infection.
3 se rendered recipients more resistant to HSV vaginal infection.
4 protect against disseminated candidiasis and vaginal infection.
5 imental disseminated candidiasis and Candida vaginal infection.
6 l concentration of oxytetracycline following vaginal infection.
7 ibodies, can help the host to resist Candida vaginal infection.
8 possible source of initial cell contact for vaginal infection.
9 cacy of a novel regimen to prevent recurrent vaginal infections.
10 in prevention of diseases that develop from vaginal infections.
11 ually transmitted infections and symptomatic vaginal infections.
12 ion during primary and secondary C. albicans vaginal infections.
13 en observed in experimental Candida albicans vaginal infections.
14 c factors controlling the immune response to vaginal infections.
15 rtain intestinal and, possibly, treatment of vaginal infections.
16 y lactobacilli have decreased acquisition of vaginal infections.
17 ral treatment administered monthly to reduce vaginal infections among Kenyan women at risk for HIV-1
18 significantly reduced the clinical signs of vaginal infection and effectively decreased animal morta
19 11,392 women who enrolled in the multicenter Vaginal Infections and Prematurity Study (1984-1989) at
20 s play a role in limiting and clearing HSV-2 vaginal infections and that they are, in association wit
21 ch higher for paint applications, influenza, vaginal infections, and ultrasound (reaching, e.g., 4-6)
22 innate resistance by neutrophils against the vaginal infection appear negligible, significant in vitr
23 nt experimental rodent models of C. albicans vaginal infection are used for many applications, the ro
26 w these marked differences in the biology of vaginal infection between these otherwise genetically si
28 tions were significantly less susceptible to vaginal infection by C. glabrata, suggesting a potential
30 uent contact with HSV-specific T cells after vaginal infection compared with epicutaneous infection.
31 or kidney infections (UTIs) and cervical or vaginal infections (CVIs) during pregnancy, as well as o
32 eudoestrus that were given MAb C3.1 prior to vaginal infection developed fewer vaginal Candida CFU th
33 terval (CI) 1.2-4.0), medical treatments for vaginal infection during pregnancy (OR = 2.4, 95% CI 1.2
34 ficantly elevated odds ratios were noted for vaginal infections during pregnancy (odds ratio (OR) = 2
35 d for the ability to protect against Candida vaginal infection, established by intravaginal (i.vg.) i
36 f delivery about pregnancy events, including vaginal infections, genital herpes, urinary tract infect
38 der estrogen-treated conditions, resulted in vaginal infection in rhesus, but not pig-tailed, macaque
39 titative analysis in response to C. albicans vaginal infection in the presence of hormones.Our data s
40 egative women 18-45 years old with 1 or more vaginal infections, including bacterial vaginosis (BV),
41 n conclusion, susceptibility to a chlamydial vaginal infection is dependent on the age of the mice, w
44 However, the subcutaneous group resolved the vaginal infection more slowly, with 60% (6 of 10 mice) o
45 ently, biofilms have also been implicated in vaginal infections, notably bacterial vaginosis (BV) and
46 bitor (NNRTI) MIV-150 in carrageenan reduced vaginal infection of macaques with simian immunodeficien
49 of vaginal T cells occurred during a primary vaginal infection or during a secondary vaginal infectio
51 om the United States and Kenya with a recent vaginal infection received intravaginal metronidazole 75
52 ers significantly greater protection against vaginal infection than seen in unvaccinated mice (P < .0
54 ilar, but not identical, fashions and caused vaginal infection; (vi) different switch phenotypes of t
56 riodic presumptive treatment (PPT) to reduce vaginal infections, we observed a significant reduction
57 riodic presumptive treatment (PPT) to reduce vaginal infections were analyzed to assess the effect of
58 roup (19 [23%] vs three [4%], p=0.0005), but vaginal infections were less common (one [1%] vs eight [
59 mary vaginal infection or during a secondary vaginal infection where partial protection was observed.
61 ct a substantial proportion of macaques from vaginal infection with a CCR5-using virus (SHIV-162P3).
70 Women with bacterial vaginosis have complex vaginal infections with many newly recognized species, i
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