Camostat Mesylate May Reduce Severity of Coronavirus Disease 2019 Sepsis: A First Observation

Hofmann-Winkler, Heike; Moerer, Onnen; Alt-Epping, Sabine; Bräuer, Anselm; Büttner, Benedikt; Müller, Martin; Fricke, Torben; Grundmann, Julian; Harnisch, Lars-Olav; Heise, Daniel; Kernchen, Andrea; Pressler, Meike; Stephani, Caspar; Tampe, Björn; Kaul, Artur; Gärtner, Sabine; Krämer, Stefanie D.; Pöhlmann, Stefan; Winkler, Martin Sebastian

doi:10.1097/cce.0000000000000284

Cited by 43 publications

(43 citation statements)

References 13 publications

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“…These clinical trials are running in Denmark (CamoCO‐19, NCT04321096), USA (RECOVER, NCT04470544, NCT04353284, NCT04524663, NCT04374019), UK (NCT04455815), Mexico (NCT04530617), Israel (COSTA, NCT04355052), Germany (NCT04338906), South Korea (NCT04521296) and Japan (NCT04451083) and should provide valuable insight into the potential utility of camostat mesylate in treating COVID‐19. A recent open‐label case‐control study with camostat mesylate on COVID‐19 intensive care patients shows promise for these ongoing trials 58 …”

Section: Discussionmentioning

confidence: 99%

Camostat mesylate against SARS‐CoV‐2 and COVID‐19—Rationale, dosing and safety

Breining

Frølund

Højen

et al. 2020

Basic Clin Pharma Tox

123

105

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SARS-CoV-2 is a new coronavirus with epicentre in the Hubei-region in China from where it spread globally in late 2019. 1-3 As of 11 March 2020, WHO declared the situation a pandemic. 4 Infection with SARS-CoV-2 leads to COVID-19, a disease ranging from mild respiratory illness to fatal pneumonia with acute respiratory distress syndrome (ARDS). 2,5 SARS-CoV-2 has proven highly contagious and has put an immense strain on healthcare systems worldwide.

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Section: Discussionmentioning

confidence: 99%

Camostat mesylate against SARS‐CoV‐2 and COVID‐19—Rationale, dosing and safety

Breining

Frølund

Højen

et al. 2020

Basic Clin Pharma Tox

123

105

View full text Add to dashboard Cite

show abstract

“…An alternative and probably safer, versus ACE2 inhibition, approach would be the use of TMPRSS2 inhibitors. TMPRSS2 is druggable and camostat mesylate partially blocked SARS-CoV-2 cell infection [ 4 ] while preliminary reports showed that it reduced the severity of COVID-19 sepsis [ 86 ]; thus, several clinical trials are currently ongoing to test whether camostat mesylate could be repurposed and utilized to combat the current pandemic [ 87 ]. TMPRSS2 inhibition could also reduce viral tropism at the initial site of SARS-CoV-2 infection and enhance anti-viral humoral immune responses of the host [ 88 , 89 ].…”

Section: Targeting the Life Cycle Of The Virusmentioning

confidence: 99%

Insights to SARS-CoV-2 life cycle, pathophysiology, and rationalized treatments that target COVID-19 clinical complications

et al. 2021

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Background Gaining further insights into SARS-CoV-2 routes of infection and the underlying pathobiology of COVID-19 will support the design of rational treatments targeting the life cycle of the virus and/or the adverse effects (e.g., multi-organ collapse) that are triggered by COVID-19-mediated adult respiratory distress syndrome (ARDS) and/or other pathologies. Main body COVID-19 is a two-phase disease being marked by (phase 1) increased virus transmission and infection rates due to the wide expression of the main infection-related ACE2, TMPRSS2 and CTSB/L human genes in tissues of the respiratory and gastrointestinal tract, as well as by (phase 2) host- and probably sex- and/or age-specific uncontrolled inflammatory immune responses which drive hyper-cytokinemia, aggressive inflammation and (due to broad organotropism of SARS-CoV-2) collateral tissue damage and systemic failure likely because of imbalanced ACE/ANGII/AT1R and ACE2/ANG(1–7)/MASR axes signaling. Conclusion Here we discuss SARS-CoV-2 life cycle and a number of approaches aiming to suppress viral infection rates or propagation; increase virus antigen presentation in order to activate a robust and durable adaptive immune response from the host, and/or mitigate the ARDS-related “cytokine storm” and collateral tissue damage that triggers the severe life-threatening complications of COVID-19.

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“… Akin to Kumar and colleagues, the essential role of transmembrane protease serine 2 (TMPRSS2) co-expression in mediating the SARS-CoV-2 cellular entry, has captivated the attention of the fraternity [3] , [4] , [5] , [6] . In this context, the TMPRSS2 inhibitors such as camostat mesylate (CM) and nafamostat mesylate (NM) are being currently envisaged as promising repurposed drugs (approved for treating pancreatitis in Japan) in COVID-19 for their anti-inflammatory and antiviral properties owing to serine protease inhibition and resultant viral cellular entry block [3] , [4] , [5] , [6] . A few researchers cite an incremental value to the therapeutic inclusion of a critical host factor blocker like TMPRSS2 inhibitor over an isolated antiviral regimen, in conferring a subsequent resilience to the rapidly developing viral resistance.…”

mentioning

confidence: 99%

“…They opine that the isolated viral point mutations are unlikely to accommodate for such a critical host component block [7] . A recent retrospective observational case-series by Hofmann-Winkler et al outlined an attenuation of the COVID-19 disease severity marked by lower sepsis-related organ failure assessment (SOFA) scores paralleled by an ameliorated inflammatory profile in the six ICU patients who received CM compared to the five ICU patients treated with hydroxychloroquine [3] . The maximum CM dose administered in their evaluation amounted to 2 × 100 mg pills three times daily for 5 days which was in accordance with the protocol of a large Denmark randomized controlled trial (RCT, CamoCo-19, NCT04321096).…”

mentioning

confidence: 99%