Your search keyword '"Kissick, Haydn Thomas"' showing total 3 results

1. Development of a peptide-based vaccine targeting TMPRSS2:ERG fusion-positive prostate cancer

Author

Kissick, Haydn Thomas, Sanda, Martin George, Dunn, Laura Kathleen, and Arredouani, Mohamed Simo

Published

2013

2. Immunophenotyping and Transcriptional Profiling of Human Plasmablasts in Dengue.

Author

Aggarwal, Charu, Saini, Keshav, Reddy, Elluri Seetharami, Singl, Mohit, Nayak, Kaustuv, Chawla, Yadya M., Maheshwari, Deepti, Singh, Prabhat, Sharma, Pragati, Bhatnagar, Priya, Kumar, Sanjeev, Gottimukkala, Kamalvishnu, Panda, Harekrushna, Gunisetty, Sivaram, Davis, Carl W., Kissick, Haydn Thomas, Kabr, Sushil Kumar, Lodha, Rakesh, Medigeshi, Guruprasad R., and Ahmed, Rafi

Subjects

*CHEMOKINE receptors, *ARBOVIRUS diseases, *DENGUE hemorrhagic fever, *DENGUE, *IMMUNOPHENOTYPING, *HEMORRHAGIC fever, *VIRUS diseases, *NEOVASCULARIZATION

Abstract

Plasmablasts represent a specialized class of antibody-secreting effector B cells that transiently appear in blood circulation following infection or vaccination. The expansion of these cells generally tends to be massive in patients with systemic infections such as dengue or Ebola that cause hemorrhagic fever. To gain a detailed understanding of human plasmablast responses beyond antibody expression, here, we performed immunophenotyping and RNA sequencing (RNA-seq) analysis of the plasmablasts from dengue febrile children in India. We found that plasmablasts expressed several adhesion molecules and chemokines or chemokine receptors that are involved in endothelial interactions or homing to inflamed tissues, including skin, mucosa, and intestine, and upregulated the expression of several cytokine genes that are involved in leukocyte extravasation and angiogenesis. These plasmablasts also upregulated the expression of receptors for several B-cell prosurvival cytokines that are known to be induced robustly in systemic viral infections such as dengue, some of which generally tend to be relatively higher in patients manifesting hemorrhage and/or shock than in patients with mild febrile infection. These findings improve our understanding of human plasmablast responses during the acute febrile phase of systemic dengue infection. IMPORTANCE Dengue is globally spreading, with over 100 million clinical cases annually, with symptoms ranging from mild self-limiting febrile illness to more severe and sometimes life-threatening dengue hemorrhagic fever or shock, especially among children. The pathophysiology of dengue is complex and remains poorly understood despite many advances indicating a key role for antibody-dependent enhancement of infection. While serum antibodies have been extensively studied, the characteristics of the early cellular factories responsible for antibody production, i.e., plasmablasts, are only beginning to emerge. This study provides a comprehensive understanding of the transcriptional profiles of human plasmablasts from dengue patients. [ABSTRACT FROM AUTHOR]

Published

2021

3. Characterization of Human CD8 T Cell Responses in Dengue Virus-Infected Patients from India.

Author

Chandele, Anmol, Sewatanon, Jaturong, Gunisetty, Sivaram, Singla, Mohit, Onlamoon, Nattawat, Akondy, Rama S., Kissick, Haydn Thomas, Nayak, Kaustuv, Reddy, Elluri Seetharami, Kalam, Haroon, Kumar, Dhiraj, Verma, Anil, Panda, HareKrushna, Siyu Wang, Angkasekwinai, Nasikarn, Pattanapanyasat, Kovit, Chokephaibulkit, Kulkanya, Medigeshi, Guruprasad R., Lodha, Rakesh, and Kabra, Sushil

Subjects

*DENGUE viruses, *IMMUNOPATHOLOGY, *T cells, *EPIDEMIOLOGY

Abstract

Epidemiological studies suggest that India has the largest number of dengue virus infection cases worldwide. However, there is minimal information about the immunological responses in these patients. CD8 T cells are important in dengue, because they have been implicated in both protection and immunopathology. Here, we provide a detailed analysis of HLA-DR+ CD38+ and HLA-DR- CD38+ effector CD8 T cell subsets in dengue patients from India and Thailand. Both CD8 T cell subsets expanded and expressed markers indicative of antigen-driven proliferation, tissue homing, and cytotoxic effector functions, with the HLADR + CD38+ subset being the most striking in these effector qualities. The breadth of the dengue-specific CD8 T cell response was diverse, with NS3-specific cells being the most dominant. Interestingly, only a small fraction of these activated effector CD8 T cells produced gamma interferon (IFN-γ) when stimulated with dengue virus peptide pools. Transcriptomics revealed downregulation of key molecules involved in T cell receptor (TCR) signaling. Consistent with this, the majority of these CD8 T cells remained IFN-γ unresponsive even after TCR-dependent polyclonal stimulation (anti-CD3 plus anti-CD28) but produced IFN-γ by TCR-independent polyclonal stimulation (phorbol 12-myristate 13-acetate [PMA] plus ionomycin). Thus, the vast majority of these proliferating, highly differentiated effector CD8 T cells probably acquire TCR refractoriness at the time the patient is experiencing febrile illness that leads to IFN-γ unresponsiveness. Our studies open novel avenues for understanding the mechanisms that fine-tune the balance between CD8 T cell-mediated protective versus pathological effects in dengue. [ABSTRACT FROM AUTHOR]

Published

2016