AUTHOR=Parra Marcela , Yang Jiyeon , Weitner Megan , Derrick Steven , Yang Amy , Schmidt Thomas , Singh Balwan , Moreno Alberto , Akkoyunlu Mustafa 

TITLE=TACI Contributes to Plasmodium yoelii Host Resistance by Controlling T Follicular Helper Cell Response and Germinal Center Formation

JOURNAL=Frontiers in Immunology

VOLUME=9

YEAR=2018

URL=https://www.frontiersin.org/journals/immunology/articles/10.3389/fimmu.2018.02612

DOI=10.3389/fimmu.2018.02612

ISSN=1664-3224

ABSTRACT=<p>The delay in parasite-specific B cell development leaves people in malaria endemic areas vulnerable to repeated <italic>Plasmodium</italic> infections. Here, we investigated the role of transmembrane activator and calcium-modulator and cyclophilin ligand interactor (TACI), a molecule involved in the generation of antigen-specific antibody secreting cells, in host response to non-lethal <italic>Plasmodium yoelii</italic> infection. We found that TACI deficiency not only resulted in higher peak parasitemia levels in <italic>P. yoelii</italic> challenged mice, but also led to a delay in parasite clearance and anti-<italic>P. yoelii</italic> Merozoite Surface Protein 1(C-terminal 19-kDa fragment [rMSP-1<sub>19</sub>]) protein and anti-rMSP-1<sub>19</sub> and anti-<italic>P. yoelii</italic> IgG antibody development. There was also a delay in the generation of splenic high affinity antibody secreting cells that recognize rMSP-1<sub>19</sub> protein as compared to wild-type mice. Interestingly, coinciding with the delay in parasite clearance there was a delay in the resolution of T follicular helper (T<sub>FH</sub>) cell and germinal center (GC) B cell responses in TACI -/- mice. The persistence of T<sub>FH</sub> and GC B cells is likely a result of enhanced interaction between T<sub>FH</sub> and GC B cells because inducible costimulator ligand (ICOSL) expression was significantly higher on TACI -/- GC B cells than wild-type cells. The difference in the kinetics of GC reaction appeared to also impact the emergence of plasma cells (PC) because there was a delay in the generation of TACI -/- mice PC. Nevertheless, following the recovery from <italic>P. yoelii</italic> infection, TACI -/- and wild-type mice were both protected from a rechallenge infection. Establishment of protective B cell response was responsible for the resolution of parasitemia because B cells purified from recovered TACI -/- or wild-type mice were equally protective when introduced to naïve wild-type mice prior to <italic>P. yoelii</italic> challenge. Thus, despite the increased susceptibility of TACI -/- mice to <italic>P. yoelii</italic> infection and a delay in the development of protective antibody levels, TACI -/- mice are able to clear the infection and resist rechallenge infection.</p>