Your search keyword '"Zayats, Romaniya"' showing total 3 results

1. T cell migration potentiates HIV infection by enhancing viral fusion and integration

Author

Lopez, Paul, Ajibola, Oluwaseun, Pagliuzza, Amelie, Zayats, Romaniya, Koh, Wan Hon, Herschhorn, Alon, Chomont, Nicolas, and Murooka, Thomas T.

Abstract

T cells actively migrate along reticular networks within lymphoid organs in search for cognate antigen, but how these behaviors impact HIV entry and infection is unclear. Here, we show that migratory T cells in 3D collagen matrix display significantly enhanced infection and integration by cell-free R5-tropic lab adapted and transmitted/founder molecular HIV clones in the absence of exogenous cytokines or cationic polymers. Using two different collagen matrices that either support or restrict T cell migration, we observe high levels of HIV fusion in migratory T cells, whereas non-motile T cells display low viral entry and integration. Motile T cells were less sensitive to combination antiretroviral drugs and were able to freely migrate into regions with high HIV densities, resulting in high infection rates. Together, our studies indicate that the environmental context in which initial HIV-T cell encounters occur modulates HIV-1 entry and integration efficiencies.

Published

2022

2. Visualizing Cellular Dynamics and Protein Localization in 3D Collagen

Author

Koh, Wan Hon, Zayats, Romaniya, Lopez, Paul, and Murooka, Thomas T.

Abstract

Immune cells migrate and communicate through cell-to-cell interactions and cytokines to coordinate the specificity and timing of the immune response. While studying these events in cell culture are standard procedure, spatiotemporal dynamics of cell-to-cell interactions within three-dimensional (3D) environments are critical in generating appropriate effector functions. Here, we present a detailed protocol to study cells within an all-in-one 3D collagen matrix that is amenable to live-cell microscopy and immunohistochemistry. This approach facilitates analyses of dynamic cellular events in 3D settings.

Published

2020

3. The Long Pentraxin 3 (PTX3) Suppresses Immunity to Cutaneous Leishmaniasis by Regulating CD4+T Helper Cell Response

Author

Gupta, Gaurav, Mou, Zhirong, Jia, Ping, Sharma, Rohit, Zayats, Romaniya, Viana, Sayonara M., Shan, Lianyu, Barral, Aldina, Boaventura, Viviane S., Murooka, Thomas T., Soussi-Gounni, Abdel, de Oliveira, Camila I., and Uzonna, Jude E.

Abstract

The long pentraxin 3 (PTX3) plays a critical role in inflammation, tissue repair, and wound healing. Here, we show that PTX3 regulates disease pathogenesis in cutaneous leishmaniasis (CL). PTX3 expression increases in skin lesions in patients and mice during CL, with higher expression correlating with severe disease. PTX3-deficient (PTX3−/−) mice are highly resistant to L. majorand L. braziliensisinfections. This enhanced resistance is associated with increases in Th17 and IL-17A responses. The neutralization of IL-17A abolishes this enhanced resistance, while rPTX3 treatment results in decrease in Th17 and IL-17A responses and increases susceptibility. PTX3−/−CD4+T cells display increased differentiation to Th17 and expression of Th17-specific transcription factors. The addition of rPTX3 suppresses the expression of Th17 transcription factors, Th17 differentiation, and IL-17A production by CD4+T cells from PTX3−/−mice. Collectively, our results show that PTX3 contributes to the pathogenesis of CL by negatively regulating Th17 and IL-17A responses.

Published

2020