TY - JOUR
T1 - Modeling HIV multiple infection
AU - Guo, Ting
AU - Qiu, Zhipeng
AU - Kitagawa, Kosaku
AU - Iwami, Shingo
AU - Rong, Libin
N1 - Funding Information:
This work was finished when the first two authors visited the Department of Mathematics at University of Florida in 2018-2019. T. Guo was supported by the NSFC grant (12071217, 11971232), the Postgraduate Research and Practice Innovation Program of Jiangsu Province (KYCX20_0243), and the CSC (201806840119). Z. Qiu was supported by the NSFC grants (12071217, 11671206). L. Rong was supported by the NSF grants DMS-1758290 and DMS-1950254.
Publisher Copyright:
© 2020 Elsevier Ltd
PY - 2021/1/21
Y1 - 2021/1/21
N2 - Multiple infection of target cells by human immunodeficiency virus (HIV) may lead to viral escape from host immune responses and drug resistance to antiretroviral therapy, bringing more challenges to the control of infection. The mechanisms underlying HIV multiple infection and their relative contributions are not fully understood. In this paper, we develop and analyze a mathematical model that includes sequential cell-free virus infection (i.e. one virus is transmitted each time in a sequential infection of target cells by virus) and cell-to-cell transmission (i.e. multiple viral genomes are transmitted simultaneously from infected to uninfected cells). By comparing model prediction with the distribution data of proviral genomes in HIV-infected spleen cells, we find that multiple infection can be well explained when the two modes of viral transmission are both included. Numerical simulation using the parameter estimates from data fitting shows that the majority of T cell infections are attributed to cell-to-cell transmission and this transmission mode also accounts for more than half of cell's multiple infections. These results suggest that cell-to-cell transmission plays a critical role in forming HIV multiple infection and thus has important implications for HIV evolution and pathogenesis.
AB - Multiple infection of target cells by human immunodeficiency virus (HIV) may lead to viral escape from host immune responses and drug resistance to antiretroviral therapy, bringing more challenges to the control of infection. The mechanisms underlying HIV multiple infection and their relative contributions are not fully understood. In this paper, we develop and analyze a mathematical model that includes sequential cell-free virus infection (i.e. one virus is transmitted each time in a sequential infection of target cells by virus) and cell-to-cell transmission (i.e. multiple viral genomes are transmitted simultaneously from infected to uninfected cells). By comparing model prediction with the distribution data of proviral genomes in HIV-infected spleen cells, we find that multiple infection can be well explained when the two modes of viral transmission are both included. Numerical simulation using the parameter estimates from data fitting shows that the majority of T cell infections are attributed to cell-to-cell transmission and this transmission mode also accounts for more than half of cell's multiple infections. These results suggest that cell-to-cell transmission plays a critical role in forming HIV multiple infection and thus has important implications for HIV evolution and pathogenesis.
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U2 - 10.1016/j.jtbi.2020.110502
DO - 10.1016/j.jtbi.2020.110502
M3 - Article
C2 - 32998053
AN - SCOPUS:85092248006
SN - 0022-5193
VL - 509
JO - Journal of Theoretical Biology
JF - Journal of Theoretical Biology
M1 - 110502
ER -
