A S Mourad scite author profile

Campylobacter jejuni infection of mice initiated by intranasal administration was investigated as a potential model for studies of pathogenesis and immunity. By using a standard challenge (5 ؋ 10 9 CFU), C. jejuni 81-176 was more virulent for BALB/c (72% mortality) than for C3H/Hej (50%), CBA/CAJ (30%), or C58/J (0%). Intranasal challenge of BALB/c was used to compare the relative virulence of three reference strains; C. jejuni 81-176 was more virulent (killing 83% of challenged mice) than C. jejuni HC (0%) or C. coli VC-167 (0%). The course of intranasally initiated C. jejuni 81-176 infection in BALB/c was determined. C. jejuni was recovered from the lungs, intestinal tract, liver, and spleen at 4 h after challenge, the first interval evaluated. After this initial interval, three distinct patterns of infection were recognized: (i) a progressive decline in number of C. jejuni CFU (stomach, blood, lungs), (ii) decline followed by a second peak in the number of organisms recovered at 2 or 3 days postchallenge (intestine, liver, mesenteric lymph nodes), and (iii) persistence of approximately the same number of C. jejuni CFU during the course of the experiment (spleen). Intranasally induced infection initiated with a sublethal number of bacteria or intranasal immunization with killed Campylobacter preparations resulted in both the generation of Campylobacter antigen-specific immune responses and an acquired resistance to homologous rechallenge. The model was used to evaluate the relative virulence of nine low-in vitro-passage (no more than five passages) isolates of C. jejuni species from patients with diarrhea. The patient isolates were differentially virulent for mice; one killed all exposed mice, three were avirulent (no deaths) and the remainder showed an intermediate virulence, killing 17 to 33%. Mouse virulence of Campylobacter strains showed a trend toward isolates originating from individuals with watery diarrhea; however, no association was found between mouse virulence and other signs or symptoms. There were no observed relationships between mouse virulence and bacterial Lior serotype or Fla polymorphic group. Intranasal challenge of BALB/c with C. jejuni is a useful model for the study of infection and vaccination-acquired immunity to this agent. Campylobacter jejuni is a major cause of gastroenteritis (36, 38) and enterocolitis in humans. Infection may be asymptomatic or associated with disease ranging in severity from acute watery diarrhea (13) to inflammatory disease that may be associated with a tissue invasion (26) and at times with bacteremia (19). Immunity to Campylobacter disease can develop as the result of repeated infections (11, 13, 36), and, thus, the feasibility of a vaccine for prevention of Campylobacter disease is suggested. The mechanism(s) of immune protection to Campylobacter infection and disease is poorly understood, and thus little information is available to guide vaccine development. In part, this deficit in knowledge results from the lack of an animal model of Campylobacter infect...

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Relative resistance to erythromycin in Chlamydia trachomatis

Mourad¹,

Sweet²,

Sugg³

et al. 1980

Antimicrob Agents Chemother

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Recent Chlamydia trachomatis isolates were tested in a tissue culture system for susceptibility to tetracycline, erythromycin, rosaramicin, rifampin, and clindamycin. Rifampin was the most active drug (miniimal inhibitory concentration, -0.02 ,g/ml). Tetracycline and rosaramicin were highly active, with a concentration of s0.25 ug/ml being chlamydicidal. Clindamycin was least active on a weight basis, requiring up to 16 ,ug/ml to prevent the passage of chlamydiae into a drugfree tissue culture system. Relative resistance to erythromycin was detected; two isolates were capable of limited replication in 1 ,ug/ml.

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Multiple-Drug-Resistant Salmonella typhi

Mourad

Metwally

Deen

et al. 1993

Clinical Infectious Diseases

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Campylobacter jejuniEnteritis

et al. 2001

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We report the development of Campylobacter jejuni enteritis in a patient with preexisting humoral and cellular immune recognition of C. jejuni antigens. This is one of few studies in which the immunologic status of a person with regard to C. jejuni before and after C. jejuni infection is directly compared, and it is the only study of which we are aware that includes measurements of cellular immunity. The findings may be important to Campylobacter vaccine development efforts.

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Standardization of measurement of immunoglobulin-secreting cells in human peripheral circulation

Baqar

Din

Scott

et al. 1997

Clin Diagn Lab Immunol

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A sensitive, and at times the most sensitive, measurement of human vaccine immunogenicity is enumeration of antibody-secreting cells (ASC) in peripheral blood. However, this assay, which is inherently capable of measurement of the absolute number of antigen-specific ASC, is not standardized. Thus, quantitative comparison of results between laboratories is not currently possible. To address this issue, isotype-specific ASC were enumerated from paired fresh and cryopreserved mononuclear cell (MNC) preparations from healthy adult volunteers resident in either the United States (US group) or Egypt (EG group). Analysis of fresh cells from US volunteers revealed mean numbers of ASC per 10 6 MNC of 617, 7,738, and 868 for immunoglobulin M (IgM), IgG, and IgA, respectively, whereas EG volunteers had 2,086, 7,580, and 1,677 ASC/10 6 MNC for the respective isotypes. Cryopreservation resulted in a slight reduction in group mean IgM, IgG, and IgA ASC (maximum reduction in group mean, 14%), but in no instance were results obtained with cryopreserved cells significantly lower than those obtained with fresh cells. To determine if cryopreservation affected the number of bacterial antigen-specific ASC detected, cells from a group of US adult volunteers who received a single oral dose of a mutated Escherichia coli heat-labile enterotoxin (LT R192G) were tested. There was no significant difference (P > 0.05) in the number of antigen-specific IgA or IgG ASC detected between fresh and cryopreserved MNC. The results support the views that ASC assays can be standardized to yield quantitative results and that the methodology can be changed to make the test more practical.

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A S Mourad

Murine intranasal challenge model for the study of Campylobacter pathogenesis and immunity

Relative resistance to erythromycin in Chlamydia trachomatis

Multiple-Drug-Resistant Salmonella typhi

Campylobacter jejuniEnteritis

Standardization of measurement of immunoglobulin-secreting cells in human peripheral circulation

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