Your search keyword '"Kress-Bennett, Jennifer"' showing total 5 results

1. Preliminary study: Treatment with intramuscular interferon beta-1a results in increased levels of IL-12Rβ2+ and decreased levels of IL23R+ CD4+ T - Lymphocytes in multiple sclerosis

Author

Kress-Bennett Jennifer M, Ehrlich Garth D, Bruno Ashley, Post J Christopher, Hu Fen Z, and Scott Thomas F

Subjects

Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Background There are a lack of biomarkers which can be used to predict clinical outcomes for multiple sclerosis (MS) patients receiving interferon beta (IFN-β). Thus the objective of this study was to characterize changes in CD4+ T-lymphocyte expression in an unbiased manner following initiation of intramuscular (IM) IFN-β-1a treatment, and then to verify those findings using marker-specific assays. Methods Peripheral blood specimens were collected from twenty MS patients before and after treatment with intramuscular (IM) IFN-β-1a and were used for isolation of mononuclear cells (PBMCs). mRNA expression patterns of negatively-selected CD4+ T-cells from the PBMCs were analyzed using microarray gene expression technology. IL-12 and IL-23 receptor levels on PBMC-derived CD4+ T-cells were analyzed by flow cytometry. The phosphorylation status of Stat4 was measured by performing densitometry on western blots. Results Microarray analyses demonstrated that mRNA expression of the IL-12Rβ2 gene was uniformly up-regulated in response to IFN-β-1a treatment and was associated with an increased number of IL-12Rβ2+ CD4+ T-cells by flow cytometry in 4 of 6 patients. This finding was substantiated by demonstrating that Stat4 phosphorylation, a transcription factor for IL-12, was increased after treatment. Conversely, the number of IL-23R+ CD4+ T-cells was decreased following treatment. Conclusions The IL-12 receptor shares a common subunit, the IL-12Rβ2, with the IL-23 receptor. Both of these receptors have a probable role in regulating IL-17 and TH-17 cells, important mediators of inflammation in multiple sclerosis (MS). Thus, the changes in the numbers of CD4+ T-cells expressing these receptors in response to IFN-β-1a treatment may point to an important mechanism of action for this drug, but further large scale studies are needed to confirm these preliminary observations.

Published

2011

2. Identification and Characterization of msf, a Novel Virulence Factor in Haemophilus influenzae

Author

Kress-Bennett, Jennifer M., primary, Hiller, N. Luisa, additional, Eutsey, Rory A., additional, Powell, Evan, additional, Longwell, Mark J., additional, Hillman, Todd, additional, Blackwell, Tenisha, additional, Byers, Barbara, additional, Mell, Joshua C., additional, Post, J. Christopher, additional, Hu, Fen Z., additional, Ehrlich, Garth D., additional, and Janto, Benjamin A., additional

Published

2016

3. In Vivo Capsular Switch in Streptococcus pneumoniae – Analysis by Whole Genome Sequencing

Author

Hu, Fen Z., primary, Eutsey, Rory, additional, Ahmed, Azad, additional, Frazao, Nelson, additional, Powell, Evan, additional, Hiller, N. Luisa, additional, Hillman, Todd, additional, Buchinsky, Farrel J., additional, Boissy, Robert, additional, Janto, Benjamin, additional, Kress-Bennett, Jennifer, additional, Longwell, Mark, additional, Ezzo, Suzanne, additional, Post, J. Christopher, additional, Nesin, Mirjana, additional, Tomasz, Alexander, additional, and Ehrlich, Garth D., additional

Published

2012

4. In vivo capsular switch in Streptococcus pneumoniae--analysis by whole genome sequencing

Author

Hu, Fen Z., Eutsey, Rory A., Ahmed, Azad, Frazão, Nelson, Powell, Evan, Hiller, Natalia, Hillman, Todd, Farrel J. Buchinsky, Boissy, Robert, Janto, Benjamin A., Kress-Bennett, Jennifer, Longwell, Mark, Ezzo, Suzanne, J. Christopher Post, Nesin, Mirjana, Tomasz, Alexander, and Ehrlich, Garth D.

Subjects

FOS: Biological sciences, 69999 Biological Sciences not elsewhere classified, 3. Good health

Abstract

Two multidrug resistant strains of Streptococcus pneumoniae - SV35-T23 (capsular type 23F) and SV36-T3 (capsular type 3) were recovered from the nasopharynx of two adult patients during an outbreak of pneumococcal disease in a New York hospital in 1996. Both strains belonged to the pandemic lineage PMEN1 but they differed strikingly in virulence when tested in the mouse model of IP infection: as few as 1000 CFU of SV36 killed all mice within 24 hours after inoculation while SV35-T23 was avirulent.Whole genome sequencing (WGS) of the two isolates was performed (i) to test if these two isolates belonging to the same clonal type and recovered from an identical epidemiological scenario only differed in their capsular genes? and (ii) to test if the vast difference in virulence between the strains was mostly - or exclusively - due to the type III capsule. WGS demonstrated extensive differences between the two isolates including over 2500 single nucleotide polymorphisms in core genes and also differences in 36 genetic determinants: 25 of which were unique to SV35-T23 and 11 unique to strain SV36-T3. Nineteen of these differences were capsular genes and 9 bacteriocin genes.Using genetic transformation in the laboratory, the capsular region of SV35-T23 was replaced by the type 3 capsular genes from SV36-T3 to generate the recombinant SV35-T3* which was as virulent as the parental strain SV36-T3* in the murine model and the type 3 capsule was the major virulence factor in the chinchilla model as well. On the other hand, a careful comparison of strains SV36-T3 and the laboratory constructed SV35-T3* in the chinchilla model suggested that some additional determinants present in SV36 but not in the laboratory recombinant may also contribute to the progression of middle ear disease. The nature of this determinants remains to be identified.

5. In vivo capsular switch in Streptococcus pneumoniae--analysis by whole genome sequencing

Author

Hu, Fen Z., Eutsey, Rory A., Ahmed, Azad, Frazão, Nelson, Powell, Evan, Hiller, Natalia, Hillman, Todd, Farrel J. Buchinsky, Boissy, Robert, Janto, Benjamin A., Kress-Bennett, Jennifer, Longwell, Mark, Ezzo, Suzanne, J. Christopher Post, Nesin, Mirjana, Tomasz, Alexander, and Ehrlich, Garth D.

Subjects

FOS: Biological sciences, 69999 Biological Sciences not elsewhere classified, 3. Good health

Abstract

Two multidrug resistant strains of Streptococcus pneumoniae - SV35-T23 (capsular type 23F) and SV36-T3 (capsular type 3) were recovered from the nasopharynx of two adult patients during an outbreak of pneumococcal disease in a New York hospital in 1996. Both strains belonged to the pandemic lineage PMEN1 but they differed strikingly in virulence when tested in the mouse model of IP infection: as few as 1000 CFU of SV36 killed all mice within 24 hours after inoculation while SV35-T23 was avirulent.Whole genome sequencing (WGS) of the two isolates was performed (i) to test if these two isolates belonging to the same clonal type and recovered from an identical epidemiological scenario only differed in their capsular genes? and (ii) to test if the vast difference in virulence between the strains was mostly - or exclusively - due to the type III capsule. WGS demonstrated extensive differences between the two isolates including over 2500 single nucleotide polymorphisms in core genes and also differences in 36 genetic determinants: 25 of which were unique to SV35-T23 and 11 unique to strain SV36-T3. Nineteen of these differences were capsular genes and 9 bacteriocin genes.Using genetic transformation in the laboratory, the capsular region of SV35-T23 was replaced by the type 3 capsular genes from SV36-T3 to generate the recombinant SV35-T3* which was as virulent as the parental strain SV36-T3* in the murine model and the type 3 capsule was the major virulence factor in the chinchilla model as well. On the other hand, a careful comparison of strains SV36-T3 and the laboratory constructed SV35-T3* in the chinchilla model suggested that some additional determinants present in SV36 but not in the laboratory recombinant may also contribute to the progression of middle ear disease. The nature of this determinants remains to be identified.