Vaccines that reduce infection & disease are needed to combat the pandemic. Here, @tianyangmao @BenIsraelow et al. describe our new mucosal booster strategy, Prime and Spike, to induce such immunity via nasal delivery of unadjuvanted spike vaccine 🧵 (1/)

biorxiv.org/content/10.110…
Current COVID vaccines are given intramuscularly. This induces robust circulating antibodies and systemic T & B cell responses that block viral spread and disease. However, to better block infection, immunity has to be established at mucosal surfaces. (2/)
annualreviews.org/doi/10.1146/an…
To elicit mucosal immunity from scratch, live attenuated vaccines are often necessary, due to the need to introduce sufficient antigen and innate immune signals needed for priming via mucosal surfaces. Live vaccines are not safe for immunocompromised. (3/)
nature.com/articles/s4157…
Adjuvanted inactivated vaccines have had safety concerns, as shown for the the intranasal flu vaccine significantly increasing the risk for Bell's palsy. (4/)

nejm.org/doi/full/10.10…
How do we overcome these problems? Intranasal inert antigens are not immunogenic, but adding adjuvant is unsafe. The answer lies in taking advantage of the existing adaptive immunity and use it as natural adjuvant to boost immunity. Hack the immune system. (5/)
To do this, @tianyangmao @BenIsraelow tested variety of boosting agents and found that simple purified spike protein (in stabilized prefusion confirmation) was able to boost ⬆️ nasal, lung and serum IgA/IgG & resident memory B & ASC following an IM Pfizer mRNA prime (blue). (6/)
Further, in every respiratory compartment, lung parenchyma, lung lumen, nasal cavity, Prime and Spike led to increased CD4 tissue-resident memory (TRM) and spike-specific CD8 TRM (blue). Note that IN Spike without Prime (gray) does not induce Ab or T cells (7/)
This strategy is versatile, and instead of using a recombinant protein, we show that spike mRNA encapsulated in immune-silent nanoparticle called Poly(amine-co-ester)s (PACE) developed by @wmsaltzman lab (PACE-Spike) IN was also capable of inducing TRM, BRM and mucosal Abs. (8/)
So how well does Prime and Spike work compared to Prime alone? To mimic waning immunity, we gave very low dose of mRNA IM to prime the mice, then boosted nasally with Spike. 42 days later, they challenged mice with a lethal dose of SARS-CoV-2. (9/)
Prime (mRNA IM) and Spike (protein IN)(blue) protected all mice from disease and death. Moreover, Prime and Spike reduced both nasal and lung viral load. Prime alone (gray) was not able to protect mice from infection, disease or death. (10/)
Similarly, Prime (mRNA IM) and PACE-Spike (mRNA in PACE IN) (green) also protected mice from death and disease, when challenged 42 days post boost. (11/)
@tianyangmao @BenIsraelow took it one step further. Can Prime and SpikeX (a heterologous Spike) generate cross-reactive immunity against SpikeX? They set up Prime (mRNA IM) boost (mRNA IM) vs. Prime (mRNA IM) and Spike (protein IN) groups and compared. (12/)
Remarkably, when SARS-CoV-1 spike was used as booster IN (red), mice developed lots of TRM (reactive to both CoV-1 and CoV-2) as well as boosted mucosal and systemic IgA and IgG against both CoV-1 and CoV-2 without suffering original antigenic sin. (13/)
This study shows that unadjuvanted recombinant spike or PACE-mRNA-spike can be used to safely boost mucosal immunity in hosts primed with conventional mRNA vaccine to reduce infection and prevent disease. A heterologous spike boost can induce variant-specific T and Ab. (14/)
Because Prime and Spike also establishes tissue-resident memory T and B cells, this strategy is likely to confer long-lasting and cross-reactive memory that can be quickly restimulated to prevent viral spread. (15/)
The intranasal spike protein booster will also be much easier to administer (via nasal spray), quite stable (just protein) and is much more likely to be accepted by people who are hesitant of mRNA or those with needle phobia. (16/)
This work was led by two brilliant colleagues, @tianyangmao and @BenIsraelow, along with @wmsaltzman and his lab members, and @marioph13 @rjhomer57 🔬(17/)
This is the first step in making this a reality. After this proof of concept in mice, this strategy needs to be tested for safety and efficacy in larger animals and in clinical trials. Similar strategies can be used to combat other mucosal viral pathogens in the future. (End)

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More from @VirusesImmunity

Jan 16
So excited to be a part of this important study led by @michelle_monje on how significant longterm neurologic damage can occur after a mild respiratory-only SARS-CoV-2 infection. My own🧵on the findings of this study with relevance to #longCovid (1/)

biorxiv.org/content/10.110…
How can a mild respiratory SARS-CoV-2 infection lead to longterm neurological symptoms? Possibilities include 1) direct infection of 🧠, 2) autoimmunity, and 3) inflammatory impact of infection distal to the 🧠. In this study, we focused on 3) 👇🏽 (2/)
To achieve this goal, @peowenlu & @Ericsongg used a mouse model developed by @BenIsraelow & @ericsongg in which we can control where the infection happens. Using AAV-hACE2 intratracheally, we can confine the SARS-CoV-2 infection only to the lungs. (3/)

rupress.org/jem/article/21…
Read 17 tweets
Dec 30, 2021
CoronaVac is an inactivated SARS-CoV-2 vaccine approved for use in 48 countries. In collaboration with the Ministry of Health in Dominican Republic, we tested whether CoronaVac (2x) + Pfizer booster induces neutralizing Abs to Delta and Omicron. (1/)

medrxiv.org/content/10.110…
We analyzed plasma samples from 101 participants in Dominican Republic (DR) who received the BNT162b2 booster >4 weeks after the 2x of CoronaVac. We compared them to samples from people at Yale who received 2x of BNT162b2.
⬆️ ⬆️ Ab induced by heterologous prime & boost.(2/)
Next, @carolilucas & @ValterVSM analyzed NAb against ancestral vs. Delta variant. CoronaVac 2x followed by Pfizer mRNA vax booster robustly elevated NAb against both virus types, level similar to 2x Pfizer vaccine. (3/)
Read 11 tweets
Dec 20, 2021
This thread is about our new preprint on transposable element called long interspersed nuclear elements (LINE-1/L1). When expressed excessively in the cerebellum, L1 causes ataxia (impaired coordination).

A fascinating finding by @taka_takehiro 👇🏽 (1/)

biorxiv.org/content/10.110…
Human genome is occupied in large part by transposable elements or jumping genes. LINE-1 occupies ~20% of our genome, compared to only 1.1% by exons. Some evolutionarily young LINE-1 are still active and are a rare cause of genetic diseases. (2/)

nejm.org/doi/full/10.10…
In addition, L1 may even promote the process of aging & age-related diseases in humans. Until recently, research focused on their activity in the germline. Now, their activity in somatic tissues during a lifespan is being studied. Fascinating review👇🏽(3/)
nature.com/articles/s4158…
Read 15 tweets
Dec 11, 2021
Our new study by @JieunOh9 @ericsongg @MiyuMoriyama et al shows that immune priming via intranasal route provides superior protection against heterologous respiratory virus challenge. The key is in inducing local secretory IgA with broader coverage. (1/)

science.org/doi/10.1126/sc…
Mucosal surface epithelium expresses polymeric Ig receptor (pIgR), which transports dimeric IgA + J-chain secreted from plasma cells within the tissue, across to the luminal side. IgA dimer + J-Chain + part of pIgR is released as ‘secretory IgA’. Figure by @BioRender. (2/)
The secretory IgA can bind viruses, bacteria, toxin in the lumen of intestine and neutralize them. Advantages of secretory IgA is the extended longevity as well as having 4 Fab instead of 2 Fab (monomeric IgA) to bind to the antigen. Secretory IgA is well studied in the gut. (3/)
Read 14 tweets
Dec 1, 2021
Today is #WorldAidsDay2021

Sharing our new review on "Impact of Chronic HIV Infection on SARS-CoV-2 Infection, COVID-19 Disease and Vaccines” by @YYexin. A short thread (1/)

link.springer.com/article/10.100…
Despite a number of studies, whether HIV infected individuals are at higher risk of COVID-19 diagnosis, hospitalization, and mortality remains unclear due to variable results found in the population studies, cohort studies, and case series. (2/)
People with chronic HIV infection have distinct immune profiles, such as reduced IFN-I, chronic inflammation, CD4 ⬇️, CD8 exhaustion, poor B cell responses, which impair immune defense against SARS-CoV-2. (Beautiful figure 🎨 by @YYexin) (3/)
Read 6 tweets
Nov 23, 2021
A preprint by Michael Simon et al @ArcadiaHealthIT shows that COVID vaccines given before or AFTER infection can reduce incidence of #longCOVID, based on a retrospective analysis of the health record of 240,648 COVID-19-infected people. 🧵(1/)

medrxiv.org/content/10.110…
People who received at least one dose of any of the 3 COVID vaccines in the US prior to COVID diagnosis were 8.8x less likely to report >1 long COVID symptoms between 12-20 weeks after diagnosis. (2/)
This reduction in LC risk appears high, given other studies that found 50% reduction or no reduction by prior vaccination in LC among breakthrough infection. Perhaps this depends on how one measures and defines long covid. (3/)

nature.com/articles/d4158…
Read 9 tweets

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