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#CovidIsNotOver

48 posts42 participants3 posts today

“Wake Up and Smell the C*VID: An evening without Eric Bogosian”: new play takes aim at NYC mask ban and more

thecanary.co/global/world-news

"As New York State’s budget deadline looms, so too does the specter of a proposed mask ban …"

"Wake Up and Smell the C*VID isn’t a typical play—it’s an intervention. A rupture. A refusal.

It refuses the erasure of an ongoing mass disabling event."

Canary · “Wake Up and Smell the C*VID: An evening without Eric Bogosian”: new play takes aim at NYC mask ban and more“Wake Up and Smell the C*VID: An evening without Eric Bogosian”: new play takes aim at NYC mask ban and more from Canary on 31 March 2025

Someone asked me yesterday, "When was it that we came out of the pandemic?"

I replied, "Uh, we didn't."

They didn't like that.

I think what they meant was: When did the powers-that-be make us "return to normal" to save the economy? Because that's when they caught their first case of COVID (for which they are still physically paying). ☹️

medrxiv.org/content/10.1101/20 (preprint)

Between November 2023 and March 2024, coastal Kenya experienced a new wave of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infections detected through our continued genomic surveillance. Herein, we report the clinical and genomic epidemiology of SARS-CoV-2 infections from 179 individuals (total 185 positive samples) residing in the Kilifi Health and Demographic Surveillance (KHDSS) area (∼900 km2). Sixteen SARS-CoV-2 lineages within three sub-variants (XBB.2.3-like (58.4%), JN.1-like (40.5%) and XBB.1-like (1.1%)) were identified. Symptomatic infection rate was estimated at 16.0% (95% CI 11.1%-23.9%) based on community testing regardless of symptom status, and did not differ across the sub-variants (p = 0.13)

For most of the community surveillance positive cases, the infection episodes remained asymptomatic (n = 124, 83.2%)

medRxiv · Genomic and clinical epidemiology of SARS-CoV-2 in coastal Kenya: Insights into variant circulation, reinfection, and multiple lineage importations during a post-pandemic waveBetween November 2023 and March 2024, coastal Kenya experienced a new wave of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infections detected through our continued genomic surveillance. Herein, we report the clinical and genomic epidemiology of SARS-CoV-2 infections from 179 individuals (total 185 positive samples) residing in the Kilifi Health and Demographic Surveillance (KHDSS) area (∼900 km2). Sixteen SARS-CoV-2 lineages within three sub-variants (XBB.2.3-like (58.4%), JN.1-like (40.5%) and XBB.1-like (1.1%)) were identified. Symptomatic infection rate was estimated at 16.0% (95% CI 11.1%-23.9%) based on community testing regardless of symptom status, and did not differ across the sub-variants ( p = 0.13). The most common infection symptoms in community cases were cough (49.2%), fever (27.0%), sore throat (7.3%), headache (6.9%), and difficulty in breathing (5.5%) and one case succumbed to the infection. Genomic analysis of the virus from serial positives samples confirmed repeat infections among five participants under follow-up (median interval 21 days, range 16-95 days); in four participants, the same virus lineage was responsible in both the first and second infections, while one participant had a different lineage in the second infection compared to the first. Phylogenetic analysis including >18,000 contemporaneous global sequences estimated that at least 38 independent virus introduction events occurred into the KHDSS area during the wave, the majority likely originating in North America and Europe. Our study highlights coastal Kenya, like most other localities, continues to face new SARS-CoV-2 infection waves characterized by the circulation of new variants, multiple lineage importations and reinfections. Locally the virus may circulate unrecognized as most infections are asymptomatic in part due to high population immunity after several waves of infection. Our findings highlight the need for sustained SARS-CoV-2 surveillance to inform appropriate public health responses such as scheduled vaccination for risk populations. Author summary Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) has transitioned to an endemic respiratory pathogen causing seasonal outbreaks. We examined the epidemiological and genomic patterns of a wave of SARS-CoV-2 infections in coastal Kenya that occurred between November 2023 and March 2024. By analyzing genetic and epidemiological data from positive cases in Kilifi, we inferred the origins of the new strains, documented repeat infections and the virus’ ongoing evolution. Our data revealed several variants circulating in the community, indicating multiple new virus introductions probably before and during local outbreaks. Many infected individuals were asymptomatic, highlighting unnoticed transmission within the population. Despite low vaccination rates among the cases (∼7.0%), high population immunity has previously been reported locally. The common symptoms among those who were symptomatic included cough, fever, and sore throat. A few participants experienced repeat infections during the wave, often involving closely related strains. The virus lineages detected were most closely related to those sampled in Europe. Our findings emphasize that, despite the end of the emergency phase, SARS-CoV-2 remains a significant public health issue, necessitating ongoing monitoring and responsive measures e.g. target vaccinations, masking and good hygiene practices to protect those at risk of severe infection. ### Competing Interest Statement The authors have declared no competing interest. ### Funding Statement This research was funded by Wellcome through (a) a Career Development Award to CNA (Ref. #226002/A/22/Z & Ref. #226002/Z/22/Z) and (b) 226130/Z/22/Z from the Wellcome Covid19: understanding the biological significance of SARS CoV 2 variants application to IO. SD acknowledges support from the Fonds National de la Recherche Scientifique (F.R.S.FNRS, Belgium; grant nF.4515.22), from the Research Foundation, Flanders (Fonds voor Wetenschappelijk Onderzoek, Vlaanderen, FWO, Belgium; grant nG098321N), and from the European Union Horizon 2020 projects MOOD (grant agreement n874850) and LEAPS (grant agreement n101094685). E.C.H. is supported by a National Health and Medical Research Council (Australia) Investigator Grant (GNT2017197). AWL was supported by the Sub-Saharan African Network for TB/HIV Research Excellence (SANTHE) which is funded by the Science for Africa Foundation [Del22007] with support from Wellcome Trust and the UK Foreign, Commonwealth & Development Office and is part of the EDCPT2 programme supported by the European Union; the Bill & Melinda Gates Foundation [INV033558]; and Gilead Sciences Inc., [19275]. All content contained within is that of the authors and does not necessarily reflect positions or policies of any SANTHE funder. For the purpose of Open Access, the author has applied a CC-BY public copyright license to any author accepted manuscript version arising from this submission. ### Author Declarations I confirm all relevant ethical guidelines have been followed, and any necessary IRB and/or ethics committee approvals have been obtained. Yes The details of the IRB/oversight body that provided approval or exemption for the research described are given below: Ethics committee/IRB of KEMRI Scientific Ethics and Research Unit (SERU), Nairobi Kenya gave ethical approval for this work. Each surveillance platform (community, outpatient, and inpatient) that provided samples analysed here had a dedicated research protocol. The protocols consenting and sample collection process were reviewed and approved by KEMRI Scientific Ethics and Research Unit (SERU), Nairobi Kenya (protocol numbers #3178, #3103 and 4724). Samples were collected following consent from a parent or guardian for participants aged <18 year olds (with assent for children aged between 13 to 18 year olds). Individual written informed consent was sought for participants aged >18 years. I confirm that all necessary patient/participant consent has been obtained and the appropriate institutional forms have been archived, and that any patient/participant/sample identifiers included were not known to anyone (e.g., hospital staff, patients or participants themselves) outside the research group so cannot be used to identify individuals. Yes I understand that all clinical trials and any other prospective interventional studies must be registered with an ICMJE-approved registry, such as ClinicalTrials.gov. I confirm that any such study reported in the manuscript has been registered and the trial registration ID is provided (note: if posting a prospective study registered retrospectively, please provide a statement in the trial ID field explaining why the study was not registered in advance). Yes I have followed all appropriate research reporting guidelines, such as any relevant EQUATOR Network research reporting checklist(s) and other pertinent material, if applicable. Yes The final consensus genomes from the SARS-CoV-2 samples sequenced in this study have been deposited in the Global Initiative on Sharing all Influenza Data (GISAID) database and can be accessed at <https://doi.org/10.55876/gis8.250116pz>. Epidemiological data and scripts for data analysis are available on the Harvard dataverse <https://doi.org/10.7910/DVN/BMCJTI>.

I just had a guy get angry at me for saying we’re still in a pandemic. He said it was fear mongering and “silly” to continue to take precautions.

He then went on to say his wife has Long Covid and he’s had Covid “at least 4-5 times”.

This attitude is why we’re in this mess. His own wife was disabled by Covid, and rather than adapt his behaviour he’s exposed her 4-5 additional times.

Repeat infections are devastating to those with Long Covid. Not to mention each infection does cumulative damage, and eventually you will be left disabled.

Even if you’re someone who believes it’s “just a flu”… surely you recognize people didn’t get the flu 4-5 times in a four year period? Being sick that often is an aberration, and a darn good reason to take precautions.

You know who hasn’t had COVID 4-5 times? People who are taking precautions.

Bonus tip: If you’re masking and you become infected anyways, you’ve reduced your viral load AND you’ve made sure not to infect anyone else. That’s community care & compassion and it’s worth doing.

It took me over a decade to realize I was disabled.

Internalized ableism is no joke. It can lead us to push our bodies and deny our reality.

I was a sickly child my whole life - but we didn’t discover the reasons until I turned 30. It was validating to finally have answers. A name for my conditions, explanations for why I never felt well & why my body couldn’t do what other people could.

Despite my now having validation and multiple diagnoses of chronic illness and disability - I didn’t identify as disabled. I was still working, still supporting myself…
So surely that meant I wasn’t right? I was scared of what it would mean if I said I was disabled.

Would people judge me? Think less of me? Would my non disabled friends distance themselves and would disabled people think I wasn’t “disabled enough”? I recognize now these were questions that were mainly due to my own internalized ableism.

I was worried about these things
because I didn’t understand dynamic disability.

I was also grieving my health. Even though I was sick before the diagnosis - once they had a name and no cure I had to come to terms with the fact that I was never going to get better.

I was likely the most functional I would ever be - and would probably lose function as I aged. That reality hit me like a ton of bricks and it took me a long time to reach a point of acceptance.

An injury followed by a viral infection took my remaining function away from me and left me completely housebound.

It wasn’t until a caring and compassionate doctor explained the concept of dynamic disability that I realized I WAS disabled and that I had been for many years.

This good doctor encouraged me to write about my experiences to help others - and while it took me time to become confident enough to speak out - I’m so glad I did.

The fact that I had so much fear of judgement, so much difficulty accepting reality only served to show me why we need more disability advocates. We need people telling their stories. It helps with acceptance of chronic illness & educates others on dynamic disability

If Covid has taught us anything it’s that a large number of people still see the disabled as “expendable”.

How many times have we heard “Covid is mild unless you have pre-existing conditions”. This has been the party line for the entire pandemic

Many folks don’t realize that it’s rooted in ableism. To say it’s only dangerous for those who are already sick is to say that we don’t matter. That killing or maiming us is acceptable as long as the non disabled can continue to live life as though we’ve gone back to 2019

As a result many disabled and high risk individuals have been isolating for five years. Have been quietly exited from society to protect themselves. We started to re-enter the world when high quality respirators became easily available - but even that is problematic

We get bullied from the “covid is over” crowd. They want us at home. They want us to not exist. Because we are a constant reminder of their own mortality and the fact that they are risking disability every time they get a Covid infection.

But here’s the incredible thing I’ve seen happen in the last few years. The disability community are organizing. They may be isolated at home but they’ve found community online. They’ve galvanized around inspiring leaders with strong voices and are creating a movement.

Not just for Covid caution & Long Covid but for the rights of disabled people across the world. For better access to healthcare, more inclusion and recognition of diversity and minority groups. Hashtags, campaigns and artwork have started taking off. We are getting louder

Activism is more important now than ever before, as we face existential threats due to the changing political landscape.

It’s a powerful moment for intersectionality. All of us who are marginalized can and should be working together to bring about change

It’s a scary time, but I have hope whenever I see people speaking out. Sharing stories. Refusing to go gently.

I’m glad to have finally stepped up and found my voice - and I hope that by sharing my story I play a small role in making the world safer

If you’re disabled or chronically ill (or even if you aren’t sure) and you’re afraid to speak up - please don’t be. Speak up. Reach out. Share your story. There’s an incredible community waiting for you and we will lift you up and help you find your voice.

Activism is important right now, but so is pacing. We must work to save our spoons amidst the torrent of bad news & stress we’re inundated with.

“We are a community. We carry each other through the tough times. Our love and support knows no borders, so when a group of us are hurting we all hurt”

disabledginger.com/p/spoon-sav

"Province continues to ensure people are protected from COVID-19, measles" says the press release

simultaneously they removed the mask mandate from healthcare settings, haven't yet made C19 vaccines available (and are tepid at best that "non-vulnerable people" (ha ha only morbid) can or should get boosted), C19 vaccination protection still wanes incredibly fast.

:unsure_fry:

Mask bans are ableist, discriminatory ugly laws.

Disabled advocates have been warning for years that if people didn’t help normalize masking, bans would follow

Please call legislators in New York and tell them No mask bans!

Medical exemptions aren’t enough, everyone needs the legal right to mask

The police are not doctors. They can’t determine who’s “sick enough” to wear a mask.

Many people with invisible illnesses struggle to get healthcare workers to take us seriously. We don’t want to be questioned by police.

Everyone should be allowed to mask up to prevent covid.

the thing about echo chambers, is they reflect back what is put into them, "with character" - think of how a choir sounds in a cathedral, versus outside

nonsense in, nonsense with character out

BUT

glorious, coordinated, beautiful voices in? Reverberating, amplified, beauty out!

what I'm getting at is: yeah, places within Mastodon & Fediverse are clearly echo chambers

but the voices in this concert hall are beautiful singly, and in harmony, and in dissonance. Songs that reflect the human condition, and broader reality.

It's not misleading to be in an echo chamber where "2+2=4"[*] and "what does the evidence say" are mantras.

I'm sure this is not an original thought, thanks to whoever (in this echo chamber!) planted it in my brain however long ago.

[*] #masksWork and #CovidIsNotOver !

Replied in thread

Some highlights from @ducky 's weekly roundup at covidbc.webfoot.com/2025/03/28

SARS-CoV-2 can interact with / activate the CD147 receptor to get into lymphocytes (T-cells and B-cells). (sciencedirect.com/science/arti)

women are 13.4 times more likely to get Long COVID if they are 🤰pregnant than if they are 🚫🤰not, with the danger highest if they catch COVID-19 in the third trimester. (sciencedirect.com/science/arti)

the rate of cases of postural orthostatic tachycardia syndrome (POTS) has gone up more than fourteen times compared to pre-pandemic (academic.oup.com/ehjqcco/advan)

covidbc.webfoot.com2025-03-28 General – Pandemics in British Columbia

Fantastic news! Long Covid research grants restored due to the efforts of advocates all over the country.

Never let anyone silence you or convince you that your voice doesn’t matter.

We all have power, and even those of us who are disabled can make a difference in our own way.

Speak up, demand accountability and work together. Change is possible!

thesicktimes.org/2025/03/28/up

The Sick Times - Chronicling the Long Covid crisis · UPDATE: RECOVER Long COVID pathobiology grants restored - The Sick TimesLong COVID research grants from the National Institutes of Health’s RECOVER program will be restored following news stories about their abrupt cancellations and advocacy to restore the funding, according to patient representatives in the initiative.