First, we wanted to know if SLR can be used as a post-exposure prophylaxis. Mice infected with lethal dose of SARS-CoV-2 were treated with SLR 4 hours after exposure. SLR-treated mice had no detectable infectious virus 5 days later and most survived. (3/)

Next, we asked whether interferon signaling is required for the SLR-mediated protection. Mice injected with blocking antibodies to IFNAR were no longer protected by SLR from SARS-CoV-2 infection. Thus, SLR-mediated protection depends on IFN-I signaling. (4/)

How late can we administer SLR to observe protection? Compared to robust protection at 4 hours, injection of SLR 24 h and 48 h post exposure protected only partially, and at 72 h, no protection was observed. (Note: mouse disease course is accelerated compared to humans)(5/)

We also tested SLR in a mouse model of immunodeficiency. Here, we used RAG-deficient mice (devoid of T or B cells) that become persistently infected. In immunocompromised patients, prolonged SARS-CoV-2 infection has been widely reported (see @Primary_Immune’s tweets) (6/)

What is remarkable is that a single injection of SLR in persistently infected animal was able to eliminate infectious virus in most of the treated mice. Thus, in the absence of adaptive immunity, robust IFN response is sufficient to eliminate persistent virus infection 🤯 (7/)

Is SLR effective against the VOCs? SLR injection 4 hours post exposure with P.1, B.1.526, B.1.351 or B.1.1.7 led to significant protection from disease & death. Difference in effectiveness might reflect the IFN-resistance of these variants.

biorxiv.org/content/10.110…

(8/)