Your search keyword '"Hasselrot, Tyra"' showing total 5 results

1. A topical rectal douche product containing Q-Griffithsin does not disrupt the epithelial border or alter CD4+ cell distribution in the human rectal mucosa

Author

Franzén Boger, Mathias, Benhach, Nora, Hasselrot, Tyra, Brand, Rhonda M., Rohan, Lisa C., Wang, Lin, McGowan, Ian, Edick, Stacey, Ho, Ken, Meyn, Leslie, Matoba, Nobuyuki, Palmer, Kenneth E., Broliden, Kristina, and Tjernlund, Annelie

Published

2023

2. Sustained immune activation and impaired epithelial barrier integrity in the ectocervix of women with chronic HIV infection.

Author

Franzén Boger, Mathias, Hasselrot, Tyra, Kaldhusdal, Vilde, Miranda, Gisele H. B., Czarnewski, Paulo, Edfeldt, Gabriella, Bradley, Frideborg, Rexaj, Genta, Lajoie, Julie, Omollo, Kenneth, Kimani, Joshua, Fowke, Keith R., Broliden, Kristina, and Tjernlund, Annelie

Subjects

*SEXUALLY transmitted diseases, *HIV infections, *TRANSCRIPTION factors, *HIV, *HIV infection transmission

Abstract

Chronic systemic immune activation significantly influences human immunodeficiency virus (HIV) disease progression. Despite evidence of a pro-inflammatory environment in the genital tract of HIV-infected women, comprehensive investigations into cervical tissue from this region remain limited. Similarly, the consequences of chronic HIV infection on the integrity of the female genital epithelium are poorly understood, despite its importance in HIV transmission and replication. Ectocervical biopsies were obtained from HIV-seropositive (n = 14) and HIV-seronegative (n = 47) female Kenyan sex workers. RNA sequencing and bioimage analysis of epithelial junction proteins (E-cadherin, desmoglein-1, claudin-1, and zonula occludens-1) were conducted, along with CD4 staining. RNA sequencing revealed upregulation of immunoregulatory genes in HIV-seropositive women, primarily associated with heightened T cell activity and interferon signaling, which further correlated with plasma viral load. Transcription factor analysis confirmed the upregulation of pro-inflammatory transcription factors, such as RELA, NFKB1, and IKZF3, which facilitates HIV persistence in T cells. Conversely, genes and pathways associated with epithelial barrier function and structure were downregulated in the context of HIV. Digital bioimage analysis corroborated these findings, revealing significant disruption of various epithelial junction proteins in ectocervical tissues of the HIV-seropositive women. Thus, chronic HIV infection associated with ectocervical inflammation, characterized by induced T cell responses and interferon signaling, coupled with epithelial disruption. These alterations may influence HIV transmission and heighten susceptibility to other sexually transmitted infections. These findings prompt exploration of therapeutic interventions to address HIV-related complications and mitigate the risk of sexually transmitted infection transmission. Author summary: Chronic immune activation is a key feature of human immunodeficiency virus (HIV) infection and is linked to various health issues, including sexually transmitted infections. The consequence of immune activation is becoming evident as age-related morbidities are appearing in younger people living with HIV. The female genital tract is a primary location for initial HIV infection and replication following sexual transmission. While we know that chronic HIV infection causes inflammation in the tissue, more detailed studies, especially focusing on mucosal epithelial tissue, are still needed. To understand how chronic HIV infection affects the female genital tract, we examined samples from HIV-positive and HIV-negative Kenyan female sex workers. We found that chronic HIV infection is associated with a sustained cervical inflammatory environment. We also noticed a decrease in genes responsible for maintaining the protective epithelial barrier in the tissue. Our results suggest a connection between HIV-induced immune responses in mucosal areas and the health of the tissue, which might explain why HIV infection may increase the risk of other sexually transmitted infections. This highlights the importance of enhancing mucosal health in people living with chronic HIV to reduce associated complications. [ABSTRACT FROM AUTHOR]

Published

2024

3. Vaginal candida infection is associated with host molecular signatures of neutrophil activation in the adjacent ectocervical mucosa in Kenyan sex workers

Author

Hasselrot, Tyra, Franzén Boger, Mathias, Kaldhusdal, Vilde, Åhlberg, Alexandra, Omollo, Kenneth, Lajoie, Julie, Kimani, Joshua, Tjernlund, Annelie, Fowke, Keith R., Czarnewski, Paulo, Broliden, Kristina, Hasselrot, Tyra, Franzén Boger, Mathias, Kaldhusdal, Vilde, Åhlberg, Alexandra, Omollo, Kenneth, Lajoie, Julie, Kimani, Joshua, Tjernlund, Annelie, Fowke, Keith R., Czarnewski, Paulo, and Broliden, Kristina

Abstract

Problem: Overgrowth of candida species in the human vaginal mucosa causes inflammation, which could render the mucosal barrier more susceptible to HIV infection. Here, we investigated whether this condition also affects the ectocervical mucosa, a potential site of HIV entry, in women at high risk of HIV infection. Method of study: Retrospective medical data and ectocervical tissue samples were obtained from a cohort of Kenyan sex workers. Among 108 women, seven had signs of vaginal candida infection by wet smear microscopy and/or the presence of characteristic discharge. Women lacking these two criteria served as controls. Host transcriptomic profiling and quantitative in situ image analysis of epithelial barrier markers and CD4+ cell distribution were performed. Results: The candida group had 162 differentially expressed genes out of 15 435 genes as compared with the control group. Among these 162 genes, 147 were upregulated and 15 were downregulated. Gene expression pathway analysis indicated associations with an upregulated inflammatory response, defined primarily by markers of neutrophil activation. Transcription factor analysis revealed upregulation of pathways related to RELA/REL/NFKB1, JUN and STAT1 in the candida group. In situ image analysis of ectocervical tissue samples showed no differences between groups in terms of epithelial height, expression of epithelial junction proteins (E-cadherin, claudin-1, zonula occludens 1, and desmoglein-1), or epithelial CD4+ cell distribution. Conclusions: Vaginal candida infection was associated with inflammation and neutrophil infiltration, but not with severe epithelial disruption or CD4+ cell infiltration, in the ectocervical mucosa.

Published

2024

4. Vaginal candida infection is associated with host molecular signatures of neutrophil activation in the adjacent ectocervical mucosa in Kenyan sex workers

Author

Hasselrot, Tyra, primary, Boger, Mathias Franzén, additional, Kaldhusdal, Vilde, additional, Åhlberg, Alexandra, additional, Omollo, Kenneth, additional, Lajoie, Julie, additional, Kimani, Joshua, additional, Tjernlund, Annelie, additional, Fowke, Keith R., additional, Czarnewski, Paulo, additional, and Broliden, Kristina, additional

Published

2024

5. A topical rectal douche product containing Q-Griffithsin does not disrupt the epithelial border or alter CD4+ cell distribution in the human rectal mucosa.

Author

Franzén Boger, Mathias, Benhach, Nora, Hasselrot, Tyra, Brand, Rhonda M., Rohan, Lisa C., Wang, Lin, McGowan, Ian, Edick, Stacey, Ho, Ken, Meyn, Leslie, Matoba, Nobuyuki, Palmer, Kenneth E., Broliden, Kristina, and Tjernlund, Annelie

Subjects

MUCOUS membranes, TOPICAL drug administration, HIV infection transmission, PRE-exposure prophylaxis, PRODUCT safety, CADHERINS, RECTUM

Abstract

To reduce HIV transmission, locally applied pre-exposure prophylaxis (PrEP) products for anorectal use will be important complements to oral and injectable PrEP products already available. It is critical to preserve an intact rectal epithelium and avoid an influx of mucosal HIV target cells with such product use. In this phase 1 clinical trial, we evaluated application of a topical rectal douche product containing Q-Griffithsin (Q-GRFT). Colorectal tissue samples were obtained via sigmoidoscopy at baseline, 1 and 24 h after single-dose exposure in 15 healthy volunteers. In situ staining for epithelial junction markers and CD4+ cells were assessed as an exploratory endpoint. A high-throughput, digitalized in situ imaging analysis workflow was developed to visualize and quantify these HIV susceptibility markers. We observed no significant differences in epithelial distribution of E-cadherin, desmocollin-2, occludin, claudin-1, or zonula occludens-1 when comparing the three timepoints or Q-GRFT versus placebo. There were also no differences in %CD4+ cells within the epithelium or lamina propria in any of these comparisons. In conclusion, the rectal epithelium and CD4+ cell distribution remained unchanged following topical application of Q-GRFT. In situ visualization of HIV susceptibility markers at mucosal sites could be useful to complement standard product safety assessments. [ABSTRACT FROM AUTHOR]

Published

2023