NIH

How should I generally go about treating my non-ICU hospitalized patient with newly diagnosed Covid-19 and who doesn’t require more than conventional O2?

FA Manian MD, MPH, , , , , , , , , , , , , , , Leave a comment

Much of the management of Covid-19 hospitalized patients who don’t require ICU care and need no more than conventional 02 (ie, high-flow or mechanical/non-mechanical ventilatory support) depends on the severity of their disease: “mild/moderate” (eg, SpO2≥94% on room air) vs “severe” (eg, Sp02<94% on room air) disease; respiration rate ≥30/min and lung infiltrates on chest radiograph>50% may also be considered, but I personally find these parameters less reliable.  Generally, patients hospitalized with Covid-19-related symptoms (respiratory or otherwise) require specific treatment to keep them from progressing or succumbing to their disease (see Figure below). 1-5

In patients with mild/moderate Covid-19, the first step is to determine whether they are at low risk (ie, NO risk factors) or high risk (ie, ≥1 risk factors) of progression to severe disease.  Recall that there are numerous risk factors for progression, including age (eg, ≥50 y) and many comorbidities, such as diabetes, chronic kidney disease, obesity, smoking (current or former), disability (eg, wheelchair dependence), and mental health disorders (eg, depression), just to name a few.1 If your patient with mild/moderate Covid-19 has ANY Covid-related symptoms and ANY risk factors for progression, you should strongly consider IV remdesivir. If your patient’s admission has nothing to do with Covid-19 but qualify for anti-Covid treatment, an oral anti-viral regimen (eg, nirmatrelvir-ritonavir [Paxlovid]) used for ambulatory patients may also be considered (see related pearl on P4P). If your patient has NO risk factors for progression to severe disease, symptomatic treatment is all that’s needed.

If your patient has severe disease but no need for 02 supplementation, IV remdesivir and prophylactic heparin (either fractionated [eg, enoxaparin] or unfractionated) should be considered; no need for dexamethasone or systemic steroids in this situation.

If your patient has severe Covid-19 and needs supplemental 02, you should consider initiation of remdesivir, dexamethasone and, at the minimum, prophylactic anticoagulation with either a fractionated or unfractionated heparin product as soon as possible.  Use of therapeutic anticoagulation in this setting (ie, outside of ICU) is controversial with NIH guidelines recommending therapeutic heparin for those with elevated D-dimer without increased bleeding risk (CIIa, “weak” with moderate supportive evidence).2,6,7  You may also be able to forgo systemic steroids in your patient with minimal 02 requirement (ie, 1-2 L) per NIH, particularly if immunocompromised, as hypoxia in such patients may be more related to viral infection itself and not significant inflammatory reaction.

If your patient with severe Covid-19 gets progressively worse requiring high-flow oxygen or non-invasive ventilation outside of ICU, you should consider adding baricitinib as a first line immunomodulator (tocilizumab or others in NIH guidelines as an alternative)2 in patients who are not already immunocompromised or do not already have and are not at high risk of secondary infections.

The duration of remdesivir treatment in hospitalized patients is usually 5 days (or until discharge) for severe Covid-19, and 3 days for those with mild/moderate disease. The ultimate duration should be individualized in patients at risk of ongoing viral replication.  One retrospective study in immunocompromised patients hospitalized for Covid-19 found remdesivir to be effective in reducing hospitalization and mortality when initiated within 2 days of hospitalization and given for a median of 5 days, even among those not requiring 02 supplementation or requiring only low flow 02.

Couple more things to keep in mind when managing severe Covid-19. When indicated, remdesivir should be given ideally as early as possible and no later than 10 days after onset of symptoms and dexamethasone should be given for up to 10 days or until discharge.  Anticoagulation, prophylactic or therapeutic, should only be prescribed in the absence of any contraindications for bleeding (see Figure footnote) and continued until discharge for no more than 14 days total.

As with all drugs, please make sure you are thoroughly familiar with the dosing, adverse effects and contraindications to above-referenced medications before prescribing them.

Figure. Management of SARS-CoV-2 positive hospitalized patients requiring no or only conventional 02 due to Covid-19

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References

  1. CDC. Interim Clinical Considerations for COVID-19 Treatment in Outpatients | CDC. Accessed Feb 1, 2024
  2. NIH. Clinical Spectrum | COVID-19 Treatment Guidelines (nih.gov). Accessed Feb 1, 2024
  3. Uptodate. Coived-19 management in hospitalized patients. https://www.uptodate.com/contents/covid-19-management-in-hospitalized-adults. Accessed Feb 5, 2024.
  4. Bash K, Sacha G, Latifi M. Covid-19: A management update. Clev Clin J Med 2023;90:677-683. https://www.ccjm.org/content/90/11/677
  5. Mozaffari E, Chandak A, Gottlieb RL, et al. Remdesivir reduced mortality in immunocompromised patients hospitalized for Covid-19 across variant waves: Findings from routine clinical practice. Clin Infect Dis 2023; 77;1626-34. https://pubmed.ncbi.nlm.nih.gov/37556727/
  6. Merz LE, Fogerty AE. The conundrum of anticoagulation for hospitalized patient with Covid-19. NEJM Evidence 2023;2 (2).  https://evidence.nejm.org/doi/full/10.1056/EVIDe2200329
  7. ATTACC, CTIV-4a, REMAP-CAP Investigators. Therapeutic anticoagulation with heparin in noncritically patients with Covid-19. N Engl J Med 2021; 385:790-802. https://pubmed.ncbi.nlm.nih.gov/34351721/

Disclosures/Disclaimers: The listed questions and answers are solely the responsibility of the author and do not necessarily represent the official views of Mercy Hospital-St. Louis, Massachusetts General Hospital, Harvard Catalyst, Harvard University, their affiliate academic healthcare centers, or its contributors. Although every effort has been made to provide accurate information, the author is far from being perfect. The reader is urged to verify the content of the material with other sources as deemed appropriate and exercise clinical judgment in the interpretation and application of the information provided herein. No responsibility for an adverse outcome or guarantees for a favorable clinical result is assumed by the author. Thank you!

How should I generally go about treating my non-ICU hospitalized patient with newly diagnosed Covid-19 and who doesn’t require more than conventional O2?

Who should get tested after a holiday indoor gathering with family members?

FA Manian MD, MPH, , , , , , , , , , , , Leave a comment

Whether you should get tested after holiday gatherings depends a lot on factors such as the level of transmission of Covid-19 within your region, the vaccination status of all the attendees, the likelihood of Covid-19 in any of the attendees, and your threshold for risk of either contracting or transmitting of Covid-19 to others, particularly immunocompromised persons. 

The following discussion assumes a scenario that is common to most indoor holiday gatherings: 1. You are getting together with people outside of your household; 2.  You or your family members don’t wear a face mask at all or certainly not all the time during the gathering; and 3. You find it impossible or don’t wish to socially distance from others during the get-together.1,2

First, let’s start with 2 situations where you should get tested following a holiday get-together, irrespective of your (or the attendees’) vaccination status: 1. if you have symptoms of Covid-19; and 2. If you were in close contact of an infected person (ie, commonly defined as within 6 feet of that person for a minimum of 15 minute during a 24-hour period).3

In the absence of known exposure or symptoms, you should consider getting tested if you are not fully immunized since you will be at higher risk of contracting and transmitting Covid-19 to others as long as there is still significant Covid-19 transmission in the region.  In contrast, if you and other attendees are fully immunized already, routine testing for Covid-19 after the gathering is hard to justify given the effectiveness of FDA-authorized Covid-19 vaccines and the costs and impracticalities associated with routine testing of millions of fully vaccinated persons.  

It goes without saying that holiday gatherings with family members outside of one’s immediate houseshold is not a zero-risk proposition for contracting or transmitting Covid-19 because people can have no symptoms and be infectious and vaccinated individuals can on occasion become infected.   Even the tests are not perfect. However, if you are concerned that you might have been exposed to Covid-19  and knowledge of a negative Covid-19 test (with its inherent limitations) gives you peace of mind, you should consider getting tested. The over-the-counter rapid Covid-19 tests may be particularly useful in assessing the likelihood of being contagious.4

For further recommendations on when you should consider getting tested for Covid-19 in general, I highly recommend an NIH-sponsored online calculator called “When to Test”.  This calculator is based on mathematical modelling that takes into account an individual’s vaccination status, transmission rates in the geographic area, and mitigation behaviors (eg, masks and social distancing).1

Bonus Pearl: Did you know that persons with Covid-19 are considered infectious 2 days before they develop symptoms or 2 days before the date of their positive test if they don’t have symptoms?5

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References:

  1. When to test offers free online tool to help individuals make informed Covid-19 testing decisions. https://www.nih.gov/news-events/news-releases/when-test-offers-free-online-tool-help-individuals-make-informed-covid-19-testing-decisions. Accessed November 26, 2021.
  2. Covid-19 testing overview. https://www.cdc.gov/coronavirus/2019-ncov/symptoms-testing/testing.html. Accessed November 26, 2021.
  3. Covid-19. https://www.cdc.gov/coronavirus/2019-ncov/php/contact-tracing/contact-tracing-plan/appendix.html#contact. Accessed November 26, 2021.
  4. Schuit E, Venekamp RP, Pas SD, et al. Diagnostic accuracy of rapid antigen tests in asymptomatic and presymptomatic close contacts of individuals with confirmed SARS-CoV-2 infection: cross sectional study. BMJ 2021;374:n1676.  https://www.bmj.com/content/374/bmj.n1676
  5. Quarantine and isolation. https://www.cdc.gov/coronavirus/2019-ncov/your-health/quarantine-isolation.html#:~:text=Get%20tested%205%2D7%20days%20after%20their%20first%20exposure.,the%20person%20with%20COVID%2D19. Accessed November 26, 2021.

Disclosures: The listed questions and answers are solely the responsibility of the author and do not necessarily represent the official views of Mercy Hospital-St. Louis, Massachusetts General Hospital, Harvard Catalyst, Harvard University, their affiliate academic healthcare centers, or its contributors. Although every effort has been made to provide accurate information, the author is far from being perfect. The reader is urged to verify the content of the material with other sources as deemed appropriate and exercise clinical judgment in the interpretation and application of the information provided herein. No responsibility for an adverse outcome or guarantees for a favorable clinical result is assumed by the author. Thank you!

 

Who should get tested after a holiday indoor gathering with family members?

Should patients previously immunized against Covid-19 receive selected monoclonal antibodies when diagnosed with a breakthrough infection?

FA Manian MD, MPH, , , , , , , , , , , , , , , , , , , , , , , , Leave a comment

Although published studies supporting monoclonal antibody therapy in mild to moderate Covid-19 preceded availability of Covid-19 vaccines and the emergence of new variants of concern,1,2 given the possibility of severe breakthrough Covid-19 in high risk vaccinated patients with suboptimal immunity and the retained activity of certain monoclonal antibody products (ie, casirivimab and imdevimab-Regeneron-Cov and sotrovimab) against common variants of SARS-CoV-2 , their use is recommended even in vaccinated individuals with mild to moderate Covid-19.3-5

In fact, the CDC states that “For people who have received one or more doses of Covid-19 vaccine and subsequently experience SARS-CoV-2 infection, prior receipt of a Covid-19 vaccine should not affect treatment decisions (including use of monoclonal antibodies, convalescent plasma, antiviral treatment, or corticosteroid administration) or timing of such treatment.”3

In its July 30, 2021 Emergency Authorization Use (EUA) letter regarding use of casirivimab and imdevimab – REGEN-COV), the FDA does not distinguish between vaccinated and unvaccinated individuals for its indications,4 similar to those of guidelines posted by the Department of Health and Human Services and the NIH.5-6

When indicated, high risk vaccinated individuals with Covid-19 should be offered  an FDA approved (under EUA currently) monoclonal antibody product (such as  casirivimab and imdevimab antibody cocktail or sotrovimab) soon after diagnosis and certainly no later than 10 days.

Vaccinated individuals with mild to moderate Covid-19 not requiring hospitalization and for whom monoclonal antibody treatment may be indicated include older patients and those with risk factors for severe disease, such as obesity, pregnancy, chronic kidney disease, chronic lung disease (including COPD), immunocompromised state, serious heart conditions (eg, heart failure, coronary artery disease, cardiomyopathies), sickle cell disease and type 2 diabetes.7

Of note, casirivimab and imdevimab is indicated for adults (weighing at least 40 kg) and children 12 years or older and is administered by IV infusion or subcutaneously, if IV infusion is not feasible and would lead to delay in treatment.4

Bonus Pearl: Did you know that in phase III trials, casirivimab and imdevimab  antibody cocktail reduced hospitalization or death by 70% in non-hospitalized patients with Covid-19?2

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References

  1. Interim clinical considerations for use of Covid-19 vaccines currently authorized in the United States. 2021. Available at https://www.cdc.gov/vaccines/covid-19/info-by-product/clinical-considerations.html. Accessed August 22, 2021.
  2. March 23, 2021 https://www.roche.com/media/releases/med-cor-2021-03-23.htm
  3. Dougan M, Nirula A, Azizad M, et al. Bamlanivimab plus Etesevimab in mild or moderate Covid-19. N Engl J Med, July 14, 2021. https://www.nejm.org/doi/10.1056/NEJMoa2102685
  4. Letter, EUA REGEN-COV, July 30, 2021. https://www.fda.gov/media/145610/download
  5. Department of Health and Human Services. High risk Covid-19 outpatients may avoid hospitalization with monoclonal antibody treatment. July 16, 2021. https://combatcovid.hhs.gov/sites/default/files/documents/High-Risk-COVID-19-Outpatients-072021.pdf
  6. Anti-SARS Cov-2 monoclonal antibodies. Accessed August 22, 2021. https://www.covid19treatmentguidelines.nih.gov/therapies/anti-sars-cov-2-antibody-products/anti-sars-cov-2-monoclonal-antibodies/
  7. Science brief: evidence used to update the list of underlying medical conditions that increase a person’s risk of severe illness from Covid-19. Accessed August 22, 2021. https://www.cdc.gov/coronavirus/2019-ncov/science/science-briefs/underlying-evidence-table.html

Disclosures: The listed questions and answers are solely the responsibility of the author and do not necessarily represent the official views of Mercy-St. Louis, Massachusetts General Hospital, Harvard Catalyst, Harvard University, their affiliate healthcare centers, or its contributors. Although every effort has been made to provide accurate information, the author is far from being perfect. The reader is urged to verify the content of the material with other sources as deemed appropriate and exercise clinical judgment in the interpretation and application of the information provided herein. No responsibility for an adverse outcome or guarantees for a favorable clinical result is assumed by the author. Thank you!

Should patients previously immunized against Covid-19 receive selected monoclonal antibodies when diagnosed with a breakthrough infection?