Mara Aspinall, managing director, BlueStone Venture Partners; professor of the practice, biomedical diagnostics, Arizona State University; advisor, Rockefeller Foundation

The vast majority of people in the US have at least partial immunity to many forms of SARS-CoV-2, either from prior infection, vaccination, or both.

The past few weeks have shown us that the Omicron variant transmits faster than any of its predecessors. That essentially guarantees that the unvaccinated plus early vaccinees (last dose/boost more than 6 months ago) will contract COVID-19 over the next few weeks and months. 

Early reports from hospitals are telling us that people with Omicron infections are suffering less severe symptoms. If this phenomenon — the combination of airborne transmissibility and mild lower airway symptoms holds up over time — then it is likely that COVID-19 will join the common cold, Influenza and Respiratory Syncytial Virus (RSV) among endemic infectious diseases.

We aren’t going to eradicate COVID. We’re going to have to live with it.

Let’s consider a couple key questions in some depth:

• What evidence is there that we are entering a COVID endemic era in 2022?
• What will a COVID endemic world look like (especially for diagnostics)?

1. What evidence is there that we are entering a COVID endemic era?

Omicron has become the dominant variant of concern in an even shorter time than Delta, the previous record holder. Because of its plethora of mutations on the Spike protein, Omicron has effective resistance to most previously developed antibody drug cocktails and substantially reduces vaccine effectiveness.

On the good news front, Omicron is causing far fewer hospitalized, ICU or ventilated patients per infection. Laboratory work suggests several compelling hypotheses of why this might be so. Our confidence is mounting that Omicron has higher transmission but lower morbidity and mortality than prior variants of concern: perhaps to the level of seasonal flu. 

However encouraging that may be, influenza fatality rates can be tragically high (e.g. 61,000 deaths in 2017-18 in the US). A world with both flu and COVID circulating at the same time will inevitably increase respiratory distress mortality and morbidity, and put tremendous pressure on hospitals.

Is there real-world evidence of lower morbidity and mortality? Early indications: Yes

The best data on Omicron comes from South Africa and the UK, where Omicron developed the earliest and where surveillance has been the most comprehensive. The UK is running about 4 weeks behind South Africa, where the drop in Omicron’s death rate was particularly striking. 

The UK pre-existing Delta death rate was already much lower than South Africa, but that too has more than halved in the Omicron era. 

The rate of asymptomatic Omicron cases is much higher than prior variants, according to a Dec. 27 study from South African researchers and colleagues at the Fred Hutchinson Cancer Research Center. Researchers found that almost one-third (31 percent) of people with HIV who enrolled in a Moderna vaccine study in South Africa in December were found to already have COVID. That’s up from about 1-2 percent of people who showed up in a comparable vaccine study months ago, when the Beta variant was circulating. These asymptomatic carriers were shown to have high levels of viral shedding based on samples from nasal swabs.

This high rate of hidden cases, and the high levels of viral shedding, means that many people will inevitably transmit their infections to others. Some of these people will end up with severe symptoms.

That’s a glimpse at the biology. Now let’s take a look at the clinical implications.

Researchers at Imperial College London looked at data from the first two weeks of December, when Omicron rose to prominence. The team reported 40-45% lower hospital admissions for Omicron versus Delta (Table 1: note UK “hospitalization” includes emergency department visits, admissions is more representative of severity). Prior infection and vaccination reduced the risk of Omicron hospital admission risk by ~70% (Table 2).

By the end of December, with more data coming in every day, the hospital admission rate in London was about 80 percent lower during this Omicron wave than the prior Delta wave.

How are the vaccines holding up?

The UK Health Security Agency has published an update on vaccine effectiveness after 198,348 UK Omicron cases (Omicron update 12/31/2021).  

Bottom-line, a two-dose mRNA vaccination series confers essentially no protection against Omicron infection after 6 months, whereas the two-dose mRNA vaccine retained ~60% effectiveness against Delta (down from 98% initially). A subsequent booster increases Omicron immunity at the 9-10 week point from a rapidly declining ~40% back up to ~50% (Pfizer boost), or ~70% (Moderna boost).

There has not yet been enough time to evaluate longer term effectiveness versus Omicron. 

Prior infection, current vaccines and boosters do reduce severity, but cannot be considered effective against infection beyond 6 months. The saving grace of the vaccines, however, can be seen in the hospitalization data referenced above. They are keeping people out of the hospitals.

There hasn’t been enough time yet to fully evaluate the US clinical experience, at least compared with the UK and South Africa. But all the signs are that it will be consistent here (for an always helpful US perspective, see Paul Sax MD’s blog of Dec. 30)

Evidence from the Laboratory to Explain Reduced Disease Severity

Over the past month, there have been many excellent studies (I have 16 on file currently and more arrive every day) examining the pathology of Omicron infection in animal models and human cell cultures. There are two arenas contributing to a consensus on why Omicron is demonstrating lower morbidity and mortality (see Eric Topol’s excellent “Ground Truths” newsletter on Substack):

Omicron infects primarily the upper respiratory tract – especially the nose and throat. That’s likely causing more coughing and viral aerosol dispersion and transmission. The virus appears to be less able to migrate further the lower respiratory tract, deep into the lungs where prior variants dramatically damage the cells – alveoli – responsible for clearing carbon dioxide and transferring essential oxygen to the bloodstream. This is an evolutionarily favorable path for viral mutation, as evidenced by Omicron’s competitive advantage over Delta, which is more efficient at getting deep into the lungs. This does not preclude a more virulent future path for Omicron, but it does reduce its likelihood.

See the following studies below for more detail:

• • Lungs have 1,000x lower viral load and no damage (12/26/21 animal model)
  • Omicron 70x higher virus in Bronchus; 10x less in lung (12/15/21 human tissue)
  • Omicron viral load and damage lower in lung (12/29/21 human tissue)
  • Cell fusion reduces white cell effectiveness, only evident in severe cases (5/12/21 Commentary/Review)
  • Damaging cell fusion (syncytia) are common in viral diseases (9/21/21 math model)
  • Omicron causes lower cell fusion closely related to pathogenicity ( animal model)
  • Lower lung absence of cleavage protein (TMPRSS) inhibits lung infection (12/22/21 cellular model)
  • Less lung infection and inflammation from Omicron (12/28/21 humanized mouse model)
  • Milder infection in all tissues, limited pathology (12/28/21 animal model)
  • Broader set of tissues infected, but less in the lungs (1/3/22 human cells)

Although neutralizing antibody counts from prior infection or vaccination do decline toward zero after 6 months, memory B cells (the cells that produce these antibodies) and memory T cells (that mobilize the immune system and attack pathogens directly) both become more broadly effective against unencountered variants after repeated prior exposures.

Generally speaking: the more exposure the better, especially with longer delays between encounters (implies minimum 12-16 week spacing of each initial and booster dose). One of the key early findings of the Omicron wave is that T-cell immunity from prior infection and vaccination appears to be longer-lasting, and this second-line of immune defense is likely a big reason why so many people are getting mild infections that don’t end up sending them to the hospital.

See a few key studies that look beyond neutralizing antibody assays below:

• • Longer infection/vaccination intervals increase resistance (1/1/22 multi-country)
  • Enhanced memory B cell effectiveness on repeated exposure (1/1/22 patient cells)
  • 70-80% of T cell effectiveness is retained across all variants (12/28/21 patient samples)
  • Omicron infection provides cross-immunity to prior variants (12/27/21 patient samples)
  • Broad immune escape but little lung damage (1/3/22 cells and epidemiology)

2. What will a COVID endemic world look like (especially for diagnostics)?

First, let’s look at this in the short term to mitigate the damage from an ongoing airborne threat.

• In the US, we need to persist in efforts to vaccinate the remaining 40% of the population that remains unvaccinated (including children). The vaccination push should require boosters at 6 months. Efforts should continue to revise vaccines for novel-variants and conserved epitopes. If successful, these updated vaccines could be available by late 2022/early 2023
• Continue masking in, and/or avoidance of, enclosed spaces
• Continue and systematize surveillance through viral genomic sequencing (and PCR)
• Empower individuals and institutions with widely available and inexpensive self-tests

There has been massive demand in the US for rapid testing. Individuals have become more familiar with self-testing. This is not about to decline. The industry needs to develop expanded availability of rapid tests to allow self-diagnosis to distinguish among the broad range of respiratory diseases – tests that can discriminate among both bacterial and viral respiratory infections – COVID-19, Influenza, RSV, tuberculosis, pneumonias etc.

Without adequate testing and surveillance, it’s hard to answer a key question — how will we know if it is “over” (at least in its current form)? 

Official counts of cases are becoming less reliable. Few of the rapid self-test results are reported to public health authorities who manage the official databases. Omicron’s increased asymptomatic cases will largely go untested — people will have COVID and walk around infecting other people without ever knowing they were positive.

In this context, reported case numbers understate the reality, even as the total number is rising exponentially. Given this reality, some have suggested we should primarily track hospital admissions since this is generally a reliable indicator of serious disease (although COVID deniers are advocating ignoring the hospitalized with COVID and only counting the hospitalized for COVID).  

Unfortunately, we now know that viral loads and hence transmission can be just as high in the asymptomatic – we cannot afford to lose track of the total number of cases.

A continuing unknown is the long-term effect of past infection. We do know that virus is found in many organs on autopsy; a trend likely exacerbated by Omicron as a result of its reduced ACE2/TMPRSS dependency. A 1/2/2022 University of Waterloo Canadian paper suggests that executive function is significantly affected during post-acute COVID-19 recovery, but we do not yet know what circumstances drive vulnerability to Long COVID-19, nor what types of infection cause it.

This is one of the big research questions that will take time to answer – to what extent does Omicron infection lead to various forms of Long COVID? What biological phenomena are driving the chronic symptoms? How many people will be affected, and for how long? What kind of symptoms will they have to endure?

It will take time to gather data to help us understand what’s going on.

It has been 100 years since the devastating 1918-1921 Influenza pandemic. That avian H1N1 virus infected one-third of the global population, with nearly 5% mortality among younger adults. We have been fortunate that COVID-19 has had a relatively low mortality rate of 1-2%, but it is clear that 21^st century travel and COVID-19 show that infection can spread quickly to more than just one third of the global population – by the time this pandemic is over, 70-80% of the global population will have been exposed, infected and/or vaccinated.

We have been negligent preparing for inevitable waves of epidemic infections. We have few effective viral therapies in hand. We are rapidly exhausting the antibiotics that have protected us from bacteria scourges for the past 70 years. 

Given that it is highly unlikely that COVID-19 disappears, we are beginning the transition to an influenza-like endemic COVID: a continuing threat of more virulent mutation-fueled outbreaks driving ever-present danger to the respiratory impaired and those with compromised immunity. 

The last 50 years have taught us that animal reservoir pathogens can mutate and spread without warning — we cannot allow ourselves to fall under the spell of complacency ever again.

Mara Aspinall, managing director, BlueStone Venture Partners; professor of the practice, biomedical diagnostics, Arizona State University

Over the past week I have been reflecting on what we know now, two years into a seemingly unending pandemic.

One of the biggest failures has been with testing.

At first, our only effective defenses were masking and social distancing. We were slow to ramp up testing, unable to give most people the timely information they could use to isolate and curb the spread.

As the first year went on, we got better and better at testing. First came PCR, then rapid antigen tests.

At the start of 2021, we began to think that testing was less necessary. Vaccination, many hoped, would bring the end of COVID all on its own. Masking became inconsistent and despised. Testing declined – to the extent that a major US rapid test antigen company began to wind down a manufacturing plant in the summer of 2021. 

Now at the end of 2021, it is clear that the virus has continued to evolve in dangerous ways.

It has kept pace, and in some ways is outpacing our best efforts. Rapid antigen tests are now reportedly in short supply in many parts of the country, right at the time they are needed most. New more transmissible variants are emerging every ~100 days. The newly emergent Omicron variant contains all the best/worst mutations of earlier variants that contribute to transmissibility and immune escape, plus an unprecedented number of mutations of which we know little or nothing.

Today, the CDC reported that Omicron makes up about 73 percent of new US cases. It took two weeks to reach that threshold. Delta needed four weeks to reach that level, and Alpha took 12 weeks. [Clarification, 12:40 pm PT Dec. 28: On Dec. 28, the CDC revised this estimate of Omicron incidence downward from 73 percent to 23 percent of new cases for the week ending Dec. 18.–LT]

In 2022, we will add effective treatments for the more seriously ill. But instead of putting all our eggs in one basket, we must mobilize all the tools at our disposal to return to “normal”, whatever that will turn out to be. Masking, vaccination, improved indoor ventilation, and the fast, low-cost and frequent self-testing that empowers individuals to manage their own health, their family health, and their community health.

Effective testing depends on how, when and where the virus replicates and the natural progression of resulting infections. A major challenge to our early understanding was that all our data came only from the sickest patients in hospital. 

How did testing become so much easier, simpler and cheaper? 

We have decent answers to four key scientific questions that put us in much better position than we were in two years ago:

1. How is the virus transmitted? Primarily aerosols, less so bodily fluids, and rarely fomites.
2. From where can we acquire a valid sample? Upper respiratory tract tissue secretions: mucus and saliva. There’s no need for more invasive or difficult to obtain biopsies or bronchoscopy.
3. Which infection products are reliable analytes? mRNA and N proteins, much less so immune response markers such as IgM from blood or volatile metabolic by-products from breath.
4. Are there easy to observe symptoms that are sufficiently reliable to act as a proxy for the infection itself? Unfortunately, no, not this time around, the only unique symptom is loss of smell or taste, but this is not universal. Temperature monitoring that worked well for SARS-CoV-1 in 2003 is largely futile “hygiene theater” for COVID-19. It’s not sensitive and not specific enough to be useful even as a screening test.

Stopping the chain of transmission requires tests that identify the infectious subset of the infected. If the upper respiratory viral load is high enough, secondary aerosol transmission can occur, especially in closed spaces where vocalization is happening (e.g. choirs, basketball arenas, bars and restaurants). 

High viral loads have been identified in all infectees: vaccinated or not; asymptomatic, pre-symptomatic, peak symptomatic, or early post symptomatic. This is to be expected, as the vaccines were designed to stimulate systemic immunity to save lives – they weren’t designed to prevent infection and transmission (although some scientists hoped they might do it all).

Optimizing the testing protocols for increasingly available rapid antigen tests depend on studies of the end-to-end natural history of disease in the same individuals over time (i.e. longitudinal, not cross-sectional) — from pre-infection, first positive test, peak infection, through viral clearance across all degrees of illness severity. This data is harder to find, mainly because it’s harder to collect than cross-sectional data.

But we do have some data to help guide us here.

A July 2021 Singapore study of hospitalized patients with Delta variant infections, who were previously given mRNA vaccines, showed that peak viral loads were similar between vaccinated and unvaccinated patients, but that the vaccinated had less severe illness and cleared the virus consistently faster (see adapted study Fig. 1).

Fig. 1. Virological and serological kinetics of SARS-CoV-2 Delta variant vaccine-breakthrough infections: a multi-center cohort study. MedRxiv. July 31, 2021. (Barnaby Edward Young et al National Center for Infectious Diseases, Singapore).

One caveat: only the seriously symptomatic were included in this study.

A December 2021 letter in the New England Journal of Medicine confirms these insights in the National Basketball Association’s 2020/2021 longitudinal screening program in a group of 173 healthy individuals (60% players/40% staff), PCR tested 19,941 times (before Omicron emerged):

• On average, from first contact through viral clearance takes an average of 13 days for the vaccinated and 15 days for the non-vaccinated – 4 days from contact to 1^st PCR+; 3.2-3.5 days to peak viral load; 5.5-7.5 more days for the unvaccinated to clear the virus. These estimates combine the results of a comprehensive study of a May/June 2021 Delta outbreak in Guangdong, China (30 million unvaccinated community PCR tests and 100% contact tracing of all 167 cases) that found that infectious contact to 1^st PCR+ in the 25% who developed COVID took an average 4 pre-symptomatic days. These data from China are consistent with the NBA study results of 1^st to last PCR dynamics, published in the NEJM. The NBA study found that 1^st PCR+ to peak timing was similar for both vaccinated and unvaccinated but that the vaccinated cleared the virus 2.3 days faster, with less patient-to-patient variation (see adapted Fig 1D & E). Several unvaccinated patients (Figure S7) had particularly long clearance times with PCR-detectable virus up to 30 days post-peak.

Adapted Fig. 1 and 2. Viral Dynamics of SARS-CoV-2 Variants in Vaccinated and Unvaccinated Persons. NEJM. Dec. 1, 2021.

• Peak viral load tops out around 100 million to 1 billion viral copies per ml (10⁸ – 10⁹cp/ml) and “…found no meaningful difference…” across all sub-groups sampled: vaccinated or not, and across variants (Wuhan A/B, Alpha or Delta – Figure 1F). However, through the wonder of exponential scales, it is worth noting that the 10^8.0 cp/ml in the vaccinated is still 20% less virus than the 10^8.1 cp/ml in the unvaccinated. In contrast to the NBA study, two earlier studies found greater differences in viral load: year-end 2020 Alpha surge data from Israel (May 2021 Nature Medicine) estimated 2.8-4.5x lower viral load in vaccinated patients (perhaps because mRNA vaccination was more effective at clearing Alpha variant infection?); and the Guangdong, China study found Delta peak viral load to be ~1,000x (10³) that of the initial Wuhan A/B D614G strain (24 cycle threshold (Ct) versus 34Ct). Either way, there is no doubt today that we have to assume that all infected individuals can reach similar viral loads and be infectious whether vaccinated or not, and whether asymptomatic or not. In other words – test, test, test to detect infection early so people can isolate in a timely manner.
• Rapid antigen tests are sensitive enough to detect transmissible individuals. A May 2021 study published in The Lancet showed there is a consensus that viral load drives transmission: the secondary attack rate (% contacts infected) was 24% if the index case viral load was >10¹⁰ cp/ml but only 12% if <10⁶ cp/ml. The Roche Cobas PCR test used in the NBA data has a limit of detection of ~25 cp/ml (10^1.4 cp/ml), corresponding to ~35 cycle threshold (Ct) (see the study’s methodology in supplementary data). Rapid antigen tests are typically 10,000x less sensitive, i.e. are antigen positive >10^5.4 cp/ml. Laboratory culture of virus is typically unsuccessful <10⁶ which implies a negative antigen test represents inability to transmit between humans, at the time of the test. This is evidence that the rapid tests are giving us valuable information – they tell us whether we are infectious at a given moment.
• Frequent testing is essential because viral load increases fast. In the NBA group, each new variant has shortened the time from 1^st PCR+ to peak viral load. The ramp-up is remarkably fast. The Wuhan D614G variant took an average of 4.2 days from 1^st PCR positive to peak viral load; Alpha 3.4 days; and Delta 3.0 days. It is likely that Omicron will prove faster still – if so, the good news is a shorter pre-symptomatic but transmissible delay, but the bad news is that it enables faster surge growth. Billy Quilty, a researcher at the London School of Hygiene & Tropical Medicine demonstrated this by taking a rapid antigen test 4 times in 24 hours, which was likely Delta, but might have been Omicron (no sequencing or PCR SGTF was performed to confirm the presence of Omicron).

Based on these data, we can conclude a few things.

Vaccines are still extremely valuable tools, but they are one layer of protection out of many.

To curb the rate of spread and keep our hospitals from being overwhelmed, we need to massively increase both the number of people who test, and how often we test, while being highly diligent in masking – even for the vaccinated and boosted. Otherwise, we’ll continue to fly blind during another very long and painful winter.