Abstract
Dengue virus (DENV) has four serotypes, which can cause from asymptomatic disease to severe dengue. Heterologous secondary infections have been associated to a greater risk of potentially fatal dengue due to non-neutralizing memory antibodies (Abs), which facilitate the infection, such as anti-precursor membrane (prM) Abs, among other mechanisms. Usually, class-switched memory Abs are generated mainly through germinal centers (GCs). However, the cellular events underlying these Ab responses to DENV, especially during repeated/secondary infections, have been poorly studied. We wanted to know whether there is involvement of GC reactions during cutaneous DENV infection and whether there is any sort of preferential Ab responses to defined viral proteins. Intradermal DENV inoculation at a relatively low dose efficiently infects immune-competent BALB/c mice, inducing higher quantities of DENV-specific GC B cells and larger GCs than the control conditions. Interestingly, GCs exhibited as much prM as envelope (E) and non-structural 3 viral proteins in situ. Intriguingly, despite the much larger abundance of E protein than of prM protein in the virions, infected animals showed similar amounts of circulating Abs and Ag-specific GC B cells both for prM and for E proteins, even significantly higher for prM. To the best of our knowledge, there are no reports of the GC responses during DENV infection. This relatively stronger anti-prM response could be triggered by DENV to preferentially promote Abs against certain viral proteins, which might favor infections by facilitating DENV invasion of host cells. It is thus conceivably that DENV might have evolved to induce this kind of Ab responses.
Highlights
Dengue virus (DENV) is one of the most significant human viral pathogens transmitted by mosquitoes and causes every year between 50 and 100 million infections worldwide, resulting in approximately 500,000 people with severe dengue (SD)
DENV Efficiently Infects Immune-Competent Mice via the Skin To explore whether the cutaneous route can be used to infect immune-competent BALB/c mice with DENV, animals were intradermally (i.d) inoculated either with active DENV (DENV2, obtained from a clinical isolate from the National Institute for Epidemiological References INDRE, Minister of Health Mexico), with UV-inactivated DENV, with supernatant from uninfected C6/36 mosquito cell line (C6/36, these are deemed the “gold standard” cells to propagate DENV), or with endotoxin-free phosphate buffered saline (PBS)
These results suggested that DENV is actively infecting immune-competent mice and inducing an immune response
Summary
Dengue virus (DENV) is one of the most significant human viral pathogens transmitted by mosquitoes and causes every year between 50 and 100 million infections worldwide, resulting in approximately 500,000 people with severe dengue (SD). It is believed that the vast majority of dengue infections are asymptomatic; a proportion manifests a non-specific febrile illness or progresses to classical dengue fever, characterized by fever and severe joint pain. Some of those infections can evolve to SD, dengue haemorrhagic fever (DHF), or dengue shock syndrome (DSS) [1]. Various mechanisms have been associated with SD disease, highlighting among them the heterologous secondary infection, due to pre-existing, sub-, or non-neutralizing memory antibodies (Abs) [2] This hypothesis was proposed decades ago, it is only recently that detailed experimental proofs were provided in humans. The prM is abundant on immature and noninfectious virions, but not in the mature particles [5,6,7]
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