https://www.ucsf.edu/magazine/covid-body
We Thought It Was Just a Respiratory Virus
We were
wrong.
By Ariel Bleicher and Katherine Conrad UCSF Magazine Summer 2020
Illustration: Anna & Elena Balbusso
In late January, when hospitals in the United States confirmed the
presence of the novel coronavirus, health workers knew to watch for
precisely three symptoms: fever, cough, and shortness of breath. But as
the number of infections climbed, the symptom list began to grow. Some
patients lost their sense of smell and taste. Some had nausea or
diarrhea. Some had arrhythmias or even heart attacks. Some had damaged
kidneys or livers. Some had headaches, blood clots, rashes, swelling, or
strokes. Many had no symptoms at all.
By June, clinicians were swapping journal papers, news stories, and
tweets describing more than three dozen ways that COVID-19, the disease
the coronavirus causes, appears to manifest itself. Now researchers at UC
San Francisco and around the world have begun taking a closer look at
this dizzying array of symptoms to get at the disease’s root causes. They
are learning from people inside the hospital and out; people on the brink
of death and only mildly sick; people newly exposed and recovered; people
young and old, Black, brown, and white. And they are beginning to piece
together the story of a virus unlike any known before.
How infection sets in
Viruses lead a curious purgatorial
existence of being neither fully alive nor dead. Enveloped in a protein
cloak, a virus consists almost entirely of genetic material – DNA or RNA,
the blueprints for all of life. But it can’t reproduce on its own. To
survive, it must break into a cell and co-opt the cell’s gene-copying
machinery.
The novel coronavirus, an RNA virus named SARS-CoV-2, has become
notorious for its skill at breaking and entering human cells. Its tools
of choice are the protein spikes protruding from its surface – a feature
that distinguishes all coronaviruses. The spikes of SARS-CoV-2 are the
crème de la crème: By the luck of the evolutionary draw, they are able to
easily grab hold of protein gates on human cells known as ACE2 receptors
and, like jackknives, pry these gates open.
Spikes on the virus’s surface act like jackknives to break and enter
human cells.
“You can think of an ACE2 receptor like a docking site,” says
Faranak Fattahi,
PhD, a UCSF
Sandler Fellow. When the coronavirus pandemic hit San Francisco,
Fattahi repurposed her laboratory to study this key receptor, which
normally plays a role in regulating blood pressure. “When the virus lands
on it,” she says, “it initiates a molecular process that brings the virus
inside the cell.”
If you’re exposed to SARS-CoV-2 – say, from a cough or sneeze – the virus
will likely first encounter ACE2 receptors on cells in your nose or
throat. But these receptors also populate your heart, gut, and other
organs. Fattahi’s team has found evidence suggesting that male sex
hormones such as testosterone may increase the number of ACE2 receptors
that cells produce, which could help explain
why SARS-CoV-2
seems to wreak greater havoc on men than on women and why kids rarely
get sick. “The fewer ACE2 receptors, the less risk of infection – that’s
the idea,” she says, adding that this hypothesis for the disease’s gender
gap is only one of several.
Once inside a few initial host cells, the virus sets them to work
churning out copies of itself. Within hours, thousands of new virus
particles begin bursting forth, ready to infect more cells. Although
SARS-CoV-2 is less deadly than the original SARS virus, which emerged in
2002, it replicates more rapidly. Also unlike SARS, which primarily
infects the lungs, SARS-CoV-2 replicates throughout the airway, including
in the nose and throat, making it highly contagious – like the common
cold.
SARS-CoV-2 replicates throughout the airway, making it highly contagious,
like the common cold.
However, infection with SARS-CoV-2 usually doesn’t feel like a cold.
Fewer than 20% of infected people who eventually show up at a hospital
report having had a sore throat or runny nose. During the first few days
of being infected, you’re more likely to have a fever, dry cough or,
peculiarly, lose your sense of smell or taste.
Most likely, though, you won’t feel sick at all. When UCSF researchers
tested people for SARS-CoV-2 in San Francisco’s Mission District,
53% of those infected never had any symptoms. “That’s much higher
than expected,” says
Monica Gandhi, MD,
MPH, a UCSF professor of medicine with expertise in HIV. Surveys of
outbreaks in nursing homes and prisons show similar or even higher
numbers. “If we did a mass testing campaign on 300 million Americans
right now, I think the rate of asymptomatic infection would be somewhere
between 50% and 80% of cases,” Gandhi says. Millions of people may be
spreading the virus without knowing it, she points out, making
asymptomatic transmission the
Achilles’
heel of efforts to control the pandemic – and highlighting the
importance of universal masking.
“The majority of people who have COVID-19 are out in the community, and
they are either asymptomatic or only mildly ill,” says
Sulggi Lee, MD, PhD, a
UCSF assistant professor of medicine. When the coronavirus pandemic hit
San Francisco in early March, Lee conceived a study to investigate why.
She scrambled to assemble a team and
procure funding and
equipment. She borrowed a colleague’s
mobile clinic –
a van outfitted with an exam table and a phlebotomy chair – so that her
team could drive around the city, collecting samples from infected
people. Lee hopes data from the study, called CHIRP (COVID-19 Host Immune
Response Pathogenesis), will show how people’s immune systems respond as
SARS-CoV-2 starts to gain a foothold in their bodies.
“A lot is riding on that initial response,” she says. If Lee and her
collaborators can figure out the biological processes that allow some
infected people to stay relatively well, they can perhaps use that
knowledge to prevent others from falling severely ill.
Battling in the lungs
True to its name, SARS-CoV-2 (which
stands for severe acute respiratory syndrome coronavirus 2) is first and
foremost a bad respiratory virus. If your immune system doesn’t defeat it
at its landing site in your nose or throat, it will advance down your
windpipe, infiltrating the cells lining your lungs’ branching air tubes.
At the tubes’ ends, tiny air sacs called alveoli pass oxygen to your
blood. As the virus multiplies, the alveoli may fill with fluid, shutting
down this critical gas exchange. Your blood-oxygen level may drop and,
typically about six days into an infection, you may start feeling short
of breath.
What causes this mayhem? “Some of it is definitely caused by the virus
itself,” says Michael
Matthay, MD, a UCSF professor of medicine who has studied acute
respiratory diseases for more than 30 years. Inevitably, a
fast-replicating virus will kill or injure many of the lung cells it
infects; the more cells it infects, the more ruin it will leave in its
wake.
The virus’s fatality rate seems to be roughly 10 times that of the
flu.
But SARS-CoV-2 doesn’t appear to be a savage destroyer of cells. Although
it’s too early to know for sure, the virus’s fatality rate seems to be
roughly 10 times that of the flu. “You would think that’s because it’s
just a killing machine,” says
Max Krummel, PhD,
UCSF’s Smith Professor of Experimental Pathology and chair of the Bakar
ImmunoX initiative. So far, however, the science suggests
otherwise.
“One of the weirder things about this new coronavirus is it doesn’t seem
to be incredibly cytopathic, by which we mean cell-killing,” Krummel
says. “Flu is really cytopathic; if you add it to human cells in a petri
dish, the cells burst within 18 hours.” But when UCSF researchers
subjected human cells to SARS-CoV-2, many of the infected cells never
perished. “It’s pretty compelling data that maybe we’re not dealing with
a hugely aggressive virus,” Krummel says.
The bigger provocation, he suspects, may be your own immune system. Like
any pathogen, SARS-CoV-2 will trigger an immune attack within minutes of
entering your body. This counterstrike is extraordinarily complex,
involving many tactics, cells, and molecules. In a
UCSF study called COMET
(COVID-19 Multi-Phenotyping for Effective Therapies), Krummel and other
scientists have been observing this immune warfare in more than 30 people
admitted to UCSF hospitals with COVID-19 and other respiratory
infections. “What we’re doing is looking at patients’ blood, their genes,
and the secretions from their noses and lungs, and we’re asking, ‘What’s
your army? What’s your response strategy?’”
An early analysis of COMET data, Krummel says, suggests that the immune
systems of many hospitalized patients mobilize differently – and more
aggressively – against SARS-CoV-2 than against influenza viruses, which
cause the flu. Their lungs are ravaged, these data suggest, not by the
virus alone but by the detritus of an immunological battle gone awry.
This rogue immune response could explain why, around day 11 of a COVID-19
infection, patients often develop a severe pneumonia known as acute
respiratory distress syndrome, or ARDS.
Ultimately, COMET seeks to find COVID-19 therapies that can rein in an
overeager immune system in order to prevent or treat ARDS. But that feat
won’t be easy, says
Carolyn Calfee, MD,
MAS ’09, an ARDS expert, UCSF professor of medicine, and co-leader of
the study. Too much or the wrong kind of intervention, she explains,
could cripple a person’s immune system to the point where it can’t clear
an infection. “It’s a fine line between therapeutic and deleterious,”
Calfee says. “We’re trying to find that balance.”
Typically, people who die from COVID-19 ARDS die around day 19. Reported
rates of mortality have varied widely, with the highest rates being where
the pandemic has hit hardest, overwhelming hospital resources and staff.
At UCSF hospitals – likely due to the city’s early shelter-in-place
orders, which prevented an initial surge of COVID-19 cases – so far only
10 of 85 critically ill patients have died.
“The good news is that we’ve been doing clinical trials of best-care
practices for ARDS since 1998,” Matthay says. Thanks to
research by him and
others, for example, clinicians have long known which ventilator
settings result in the fewest deaths and how to flip patients onto their
stomachs – a technique known as proning – to best help them breathe. If
public health measures can keep hospital admissions low so that frontline
providers can make good use of the skills and knowledge they already
have, we may find that we have less to fear from SARS-CoV-2 than we
thought.
On the other hand, the virus behaves in ways that are still
mysterious.
![[]](https://img.genial.ly/5ce856bdf46a770ff83513c2/a5277e6e-cded-4e76-848b-ec6d637b922d.png)
GO TO WEBSITE FOR INTERACTIVE GRAPHIC
Text upper left: From Head to “COVID Toes” underlined. Text below
underline: People with COVID-19 exhibit from none to many of these
symptoms. Some symptoms (such as fever, cough, and loss of smell) are
common, while others (such as sore throat, pink eye, and stroke) are
rare. Middle of page: Illustration of human body. From the top: Brain
with one plus sign that opens to text reading: Headaches, brain fog,
dizziness, delirium, stroke, and another plus sign that opens to text
reading: Pink eye. Throat area with plus sign that opens to text reading:
Loss of smell or taste, runny nose, sneezing, sore throat. Heart with
plus sign that opens to box reading: Arrhythmia, weakened cardiac muscle,
heart attack. Lower left lung with plus sign that opens to text reading:
Cough, shortness of breath, lung injury. Kidney with plus sign that opens
to text reading: Kidney injury, elevated liver enzymes. Intestines with
plus sign that opens to text reading: Nausea, stomachache, vomiting,
diarrhea. Upper thigh with plus sign that opens to text reading: Fever,
fatigue, muscle aches, inflammation, blood clots, vascular injury. Toe
with with plus sign that opens to text reading: Skin rash, numbness or
swelling in feet or hands. Bottom of illustration: rectangle filled with
faded-back coronaviruses and text at far right reading: illustration
Stephanie Koch. Left of body illustration: small illustration of
coronavirus. Top and right of illustration: small illustration of
coronavirus.
Concept credit: Jennifer Babik, MD, PhD
Heart failure
In April, Susan Parson, MD, a Bay Area
medical examiner, made a startling discovery. For nearly two months,
officials had believed that the first people in the U.S. to die from
COVID-19 had died of respiratory failure in Washington state in late
February. At the time, the U.S. Centers for Disease Control and
Prevention limited testing to people who had respiratory symptoms and had
recently traveled to China or otherwise been exposed to the virus. Those
restrictions, however, turned out to be misguided.
As a medical examiner for California’s Santa Clara County, Parson had
done a routine autopsy on a 57-year-old woman named Patricia Dowd, who
had died suddenly at home on February 6. In Dowd’s tissues, Parson found
the cause of her death: SARS-CoV-2. But the virus hadn’t wrecked Dowd’s
lungs. In fact, she had only mild pneumonia. Instead, SARS-CoV-2 had
ruptured her heart.
Meanwhile, epidemiologists began learning that preexisting heart disease
and related conditions put people at greater risk of suffering and dying
from COVID-19. “We’re finding that many patients who have more severe
forms of the illness are obese, they are diabetic, they are
hypertensive,” says cardiologist
Nisha Parikh, MD, a
UCSF associate professor who specializes in population health research.
Such risk factors, she says, are unusual. “They’re not ones that really
stood out in prior epidemics.”
Clinicians, too, were seeing surprising numbers of COVID-19 patients
develop heart problems – muscle weakness, inflammation, arrhythmias, even
heart attacks. “We’re not used to respiratory viruses having such dire
consequences on the heart in such apparently high numbers,” says
cardiologist Gregory
Marcus, MD, MAS ’08, UCSF’s Endowed Professor of Atrial Fibrillation
Research. Many patients whose hearts acted up also had failing lungs. But
others had no other symptoms or, like Dowd, only mild ones.
Since March, Marcus has co-led one of the largest community surveys to
better understand the spread of SARS-CoV-2 and its myriad effects. The
study, dubbed COVID-19 Citizen Science, has so far enrolled more than
27,000 people; anyone with a smartphone
can participate. Marcus
plans to also start collecting data from wearable devices, including
Fitbits and Zio patches, which wirelessly monitor heart rhythms. “There
may be large numbers of people who are suffering from cardiovascular
effects of COVID-19 in the absence of other symptoms,” Marcus says. “I’m
worried we’re missing those cases.”
It stands to reason that SARS-CoV-2 affects the heart. After all, heart
cells are flush with ACE2 receptors, the virus’s vital port of entry.
And, indeed, laboratory experiments suggest that the virus can enter and
replicate in cultured human heart cells, says
Bruce Conklin, MD,
a professor of medicine and an expert in heart-disease genetics at UCSF
and the Gladstone Institutes.
But Conklin doesn’t think SARS-CoV-2 necessarily kills heart cells
outright. Rather, in the process of copying itself, the virus steals
pieces of the genetic instructions that tell the heart cells how to do
their job. “It’s hauling away and hijacking stuff that’s necessary for
the heart to beat,” he says. He is currently testing this hypothesis
using human heart cells grown in cup-sized vessels in the lab of
Todd McDevitt, PhD,
a bioengineer at UCSF and the Gladstone Institutes.
It’s also possible, however, that an infected person’s own immune system
may do the majority of the damage in the heart, as it appears to do in
the lungs. “The heart probably gets infected by a lot of other viruses,
and they don’t have a lethal effect,” Conklin says. “What makes this one
different?”
Graph with three bars. Bar at left has 80% at top and Non-Severe at
bottom. Bar in middle has 15% at top and Severe at bottom Bar at right
has 5% at top and Critical at bottom. Text below graph reads: Most
symptomatic cases of COVID-19 are mild. To left of graph, small circle
with the letter “i” in the middle opens to text reading: Graph Data: Wu
et al., JAMA 2020. Livingston et al., JAMA 2020. Garg et al, MMWR 2020.
Stoke et al., MMWR 2020. Left of graph: illustration of a
coronavirus.
Most symptomatic cases of COVID-19 are mild.
Stranger things
Toward the end of March, as San Francisco
began to warm up, Sonia got cold feet. She put on wool socks and turned
up her heater. Still, her feet felt frozen. Three days later, her soles
turned splotchy purple. Red dots appeared on her toes. At night, her cold
feet itched and burned. Walking hurt. And she was exhausted, napping
through afternoon Zoom meetings. “It was so bizarre,” says Sonia, a San
Francisco resident. A week later, her symptoms were gone.
“Yes, COVID,” wrote Lindy
Fox, MD, a UCSF professor of dermatology, replying to an email
describing Sonia’s case. Sonia wasn’t surprised. Anyone, like her, who’s
been following news of the pandemic has probably heard about “COVID
toes,” a painful or itchy skin rash that sometimes pops up in young
adults with otherwise mild or asymptomatic cases of COVID-19. “It looks
like what we call pernio, or chilblains,” Fox says, “which is a pretty
common phenomenon when somebody goes out in cold weather – they start to
get purple or pink bumps on their fingers or toes.”
Many people with rashes like Sonia’s don’t test positive for COVID-19,
Fox says, which has made some clinicians skeptical of the connection;
when patients have both, it’s just a coincidence, they believe. But Fox
doesn’t think so. For one thing, “the time of year is wrong,” she says.
“Pernio usually shows up in the dead of winter.” Even more compelling,
dermatologists around the world are “getting crazy numbers of calls about
it,” Fox says. “In the last three weeks, I’ve had somewhere between 10
and 12 patients.
Normally, I have four a year.”
20%-40% of people with COVID-19 experience diarrhea, nausea, or vomiting
before other symptoms.
And it’s not just dermatologists who are adding their observations to
COVID-19’s ever-expanding symptom list. Gut specialists are finding that
20% to 40% of people with the disease experience diarrhea, nausea, or
vomiting before other symptoms, says gastroenterologist
Michael Kattah, MD,
PhD, a UCSF assistant professor. If you swallow virus particles, he
says, there’s a good chance they will infect cells lining your stomach,
small intestine, or colon. As in the lungs and heart, these cells are
studded with vulnerable ACE2 portals.
Especially disconcerting, Kattah says, is how long the virus seems to
persist in the gut. About 50% of patients with COVID-19 have virus
particles in their stools, often for weeks after their nose swabs test
negative, he points out. Laboratory studies show that these particles are
often still alive and can infect cells in a petri dish. Whether fecal
transmission occurs between people, however, is an open question. If the
answer is yes, people recovering from COVID-19 may need to stay
quarantined even after they feel well, and the rest of us will need to be
as meticulous about bathroom hygiene as we’ve become about handwashing
and mask-wearing.
Other specialists are also raising flags. Neurologists worry about
reports of COVID-19 patients with headaches, “brain fog,” loss of the
sense of smell, dizziness, delirium, and, in rare cases, stroke.
Nephrologists worry about kidney stress and failure. Hepatologists worry
about liver injuries. Ophthalmologists worry about pink eye.
Pediatricians, meanwhile, worry about a peculiar
COVID-related inflammatory
syndrome that’s showing up in kids and young adults.
Researchers are still sorting out the causes for this constellation of
effects. If you come down with a particular symptom, is it because the
virus is attacking your cells? Because your immune system is
overreacting? Or just because you’re very sick? In any severe illness,
for example, the kidneys must work extra hard to filter waste and control
nutrients and fluid; if overtaxed, they may begin to fail. Similarly,
cognitive problems can result from increased blood toxins due to stressed
kidneys or from low oxygen due to respiratory distress. “There’s a lot of
smoke,” says Michael
Wilson, MD ’07, MAS ’16, the Rachleff Distinguished Professor at
UCSF’s Weill Institute for Neurosciences. “We need to figure out where
the fire is coming from.”
Recently, there’s been speculation that some of COVID-19’s seemingly
disparate symptoms may stem from trouble in the blood. Blood clots, for
example, are showing up in cases of COVID-19 frequently enough for
clinicians to take notice. “There’s something unique about the
coagulation system in these patients,” says nephrologist
Kathleen Liu, MD ’99,
PhD ’97, MAS ’07, a UCSF professor of medicine. In caring for
COVID-19 patients on dialysis machines, she’s been surprised to see blood
clots block dialysis tubes more than usual. Clotted tubes are common, she
says, “but this is extreme.”
Evidence suggests SARS-CoV-2 can infect cells in the walls of blood
vessels that help regulate clotting.
That may be because, as growing evidence suggests, SARS-CoV-2 can infect
cells in the walls of blood vessels that help regulate blood flow and
coagulation, or clotting. If true, this behavior could explain some of
the virus’s weirder (and rarer) manifestations, such as heart attacks,
strokes, and even “COVID toes.”
“Our vasculature is a contiguous system,” says cardiologist Parikh. “Thus
injury in one area, such as blood vessels in the lungs, can set off
clotting cascades that affect multiple organs.” Some of that trouble
likely results from inflammation triggered by the immune system, she
points out, although another culprit may be the body’s RAAS, or
renin-angiotensin-aldosterone system, a hormone system that controls
blood pressure and fluid balance. Because RAAS involves ACE2 receptors,
Parikh suspects it may become disrupted when the virus infects cells
through these receptors, thus triggering coagulation and other downstream
effects. Her lab is now studying this system in COVID-19 patients to
better understand how SARS-CoV-2 infection affects it.
Inevitably, some ailments may turn out to be red herrings. During a
pandemic, when people are flocking to hospitals with infections,
clinicians will also see a rise in other health problems, simply by the
rules of statistics, points out
S. Andrew Josephson,
MD, the Francheschi-Mitchell Professor, chair of UCSF’s neurology
department, and a member of the Weill Institute for Neurosciences. “If
the prevalence of infection is high, then almost any condition – a broken
leg, if you will – you might conclude is associated with COVID-19.”
“As clinicians, we want to get information to our medical community and
to the public as quickly as possible,” Josephson says, “but we have to be
cautious about not making too big a deal of a little blip.”
The long tail
As with any infection, how long a bout of
COVID-19 lasts
varies from person to person. If you’re ill enough to need critical
care, you can expect the disease to take at least a few weeks to run its
course. In some cases, symptoms persist for months. For a typical milder
case, though, you should feel better within a couple weeks.
At that point, the question foremost on your mind will be: Am I immune?
There are now more than a dozen antibody tests on the market, but most
are unreliable,
according to UCSF research. And even the best tests can’t tell you
whether you have enough of the right kinds of antibodies to protect you
against reinfection. “There is a lot of hope and belief that we’ll have
an antibody test that actually informs us of immunity, but we’re not
quite there yet,” says
Chaz Langelier, MD,
PhD, a UCSF assistant professor of medicine who is working to improve
diagnostic tools for COVID-19.
What we have in the meantime are a lot of unknowns: If you do become
immune to SARS-CoV-2, when and how does that occur? Will you gain
immunity from a mild or asymptomatic case, as well as a severe one? How
long will that immunity last?
“The answers will have huge implications for social distancing and
masking and for getting the economy back up and running,” says
Michael Peluso,
MD, a clinical fellow who came to UCSF three years ago to help fight
HIV. Now he’s co-leading a new
study called LIINC (Long-term Impact of Infection with Novel
Coronavirus), which is enrolling people who have been infected with
SARS-CoV-2 and will follow them for two years. Besides illuminating
changes in immunity over time, LIINC is investigating chronic effects of
infection on the immune system, lungs, heart, brain, blood, and other
parts of the body.
“I hope people will recover and immunity will be protective and
long-lasting, and that will be that,” Peluso says.
It’s what we all hope. We hope we will beat an infection swiftly – or,
better yet, avoid the virus until there is a vaccine. We hope that if we
do fall gravely ill, we will be cared for by the best providers and
tended to by people we love. The reality, as we already know, is more
complicated. And even if COVID-19 doesn’t batter our bodies, the pandemic
will surely leave scars – on our psyches, our livelihoods, our
institutions, and our health – that we are only beginning to fathom. In
truth, we don’t know how our cards will fall, as individuals or as a
people. Only time – and data – will tell.