A Study to Evaluate the Safety and Effectiveness of Antithrombotics to Treat Hospitalized COVID-19 Patients

Mayo Clinic Location	Status	Contact
Scottsdale/Phoenix, Ariz. Mayo Clinic principal investigator Leslie Padrnos, M.D.	Closed for enrollment	Contact information: Amanda Palacios B.S. (480) 342-6236

Effect of Crizanlizumab, a P-Selectin Inhibitor, in COVID-19: A Placebo-Controlled, Randomized Trial. Leucker TM. Thorsten M; Osburn WO. William O; Reventun P. Paula; Smith K. Kimberley; Claggett B. Brian; Kirwan BA. Bridget-Anne; de Brouwer S. Sophie; Williams MS. Marlene S; Gerstenblith G. Gary; Hager DN. David N; Streiff MB. Michael B; Solomon SD. Scott D; Lowenstein CJ. Charles J. JACC. Basic to translational science. 2021. Dec; 6(12):935-945

COVID-19 is characterized by vascular inflammation and thrombosis, including elevations in P-selectin, a mediator of inflammation released by endothelial cells. We tested the effect of P-selectin inhibition on biomarkers of thrombosis and inflammation in patients with COVID-19. Hospitalized patients with moderate COVID-19 were randomly assigned to receive either placebo or crizanlizumab, a P-selectin inhibitor, in a double-blind fashion. Crizanlizumab reduced P-selectin levels by 89%. Crizanlizumab increased D-dimer levels by 77% and decreased prothrombin fragment. There were no significant differences between crizanlizumab and placebo for clinical endpoints. Crizanlizumab was well tolerated. Crizanlizumab may induce thrombolysis in the setting of COVID-19. (Crizanlizumab for Treating COVID-19 Vasculopathy [CRITICAL]; NCT04435184). Read More on PubMed

Thrombo-inflammatory biomarkers and D-dimer in a biracial cohort study. Kamin Mukaz D. Debora; Gergi M. Mansour; Koh I. Insu; Zakai NA. Neil A; Judd SE. Suzanne E; Sholzberg M. Michelle; Baumann Kreuziger L. Lisa; Freeman K. Kalev; Colovos C. Christos; Olson NC. Nels C; Cushman M. Mary. Research and practice in thrombosis and haemostasis. 2021. Dec; 5(8):e12632

Higher D-dimer is a risk factor for cardiovascular diseases and venous thromboembolism. In the general population, D-dimer and other thrombo-inflammatory biomarkers are higher among Black individuals, who also have higher risk of these conditions compared to White people. Read More on PubMed

Dapagliflozin in patients with cardiometabolic risk factors hospitalised with COVID-19 (DARE-19): a randomised, double-blind, placebo-controlled, phase 3 trial. Kosiborod MN. Mikhail N; Esterline R. Russell; Furtado RHM. Remo H M; Oscarsson J. Jan; Gasparyan SB. Samvel B; Koch GG. Gary G; Martinez F. Felipe; Mukhtar O. Omar; Verma S. Subodh; Chopra V. Vijay; Buenconsejo J. Joan; Langkilde AM. Anna Maria; Ambery P. Philip; Tang F. Fengming; Gosch K. Kensey; Windsor SL. Sheryl L; Akin EE. Emily E; Soares RVP. Ronaldo V P; Moia DDF. Diogo D F; Aboudara M. Matthew; Hoffmann Filho CR. Conrado Roberto; Feitosa ADM. Audes D M; Fonseca A. Alberto; Garla V. Vishnu; Gordon RA. Robert A; Javaheri A. Ali; Jaeger CP. Cristiano P; Leaes PE. Paulo E; Nassif M. Michael; Pursley M. Michael; Silveira FS. Fabio Serra; Barroso WKS. Weimar Kunz Sebba; Lazcano Soto JR. José Roberto; Nigro Maia L. Lilia; Berwanger O. Otavio. The lancet. Diabetes & endocrinology. 2021. Sep; 9(9):586-594

COVID-19 can lead to multiorgan failure. Dapagliflozin, a SGLT2 inhibitor, has significant protective benefits for the heart and kidney. We aimed to see whether this agent might provide organ protection in patients with COVID-19 by affecting processes dysregulated during acute illness. Read More on PubMed

Therapeutic Anticoagulation with Heparin in Noncritically Ill Patients with Covid-19. . ; . ; . ; Lawler PR. Patrick R; Goligher EC. Ewan C; Berger JS. Jeffrey S; Neal MD. Matthew D; McVerry BJ. Bryan J; Nicolau JC. Jose C; Gong MN. Michelle N; Carrier M. Marc; Rosenson RS. Robert S; Reynolds HR. Harmony R; Turgeon AF. Alexis F; Escobedo J. Jorge; Huang DT. David T; Bradbury CA. Charlotte A; Houston BL. Brett L; Kornblith LZ. Lucy Z; Kumar A. Anand; Kahn SR. Susan R; Cushman M. Mary; McQuilten Z. Zoe; Slutsky AS. Arthur S; Kim KS. Keri S; Gordon AC. Anthony C; Kirwan BA. Bridget-Anne; Brooks MM. Maria M; Higgins AM. Alisa M; Lewis RJ. Roger J; Lorenzi E. Elizabeth; Berry SM. Scott M; Berry LR. Lindsay R; Aday AW. Aaron W; Al-Beidh F. Farah; Annane D. Djillali; Arabi YM. Yaseen M; Aryal D. Diptesh; Baumann Kreuziger L. Lisa; Beane A. Abi; Bhimani Z. Zahra; Bihari S. Shailesh; Billett HH. Henny H; Bond L. Lindsay; Bonten M. Marc; Brunkhorst F. Frank; Buxton M. Meredith; Buzgau A. Adrian; Castellucci LA. Lana A; Chekuri S. Sweta; Chen JT. Jen-Ting; Cheng AC. Allen C; Chkhikvadze T. Tamta; Coiffard B. Benjamin; Costantini TW. Todd W; de Brouwer S. Sophie; Derde LPG. Lennie P G; Detry MA. Michelle A; Duggal A. Abhijit; Džavík V. Vladimír; Effron MB. Mark B; Estcourt LJ. Lise J; Everett BM. Brendan M; Fergusson DA. Dean A; Fitzgerald M. Mark; Fowler RA. Robert A; Galanaud JP. Jean P; Galen BT. Benjamin T; Gandotra S. Sheetal; García-Madrona S. Sebastian; Girard TD. Timothy D; Godoy LC. Lucas C; Goodman AL. Andrew L; Goossens H. Herman; Green C. Cameron; Greenstein YY. Yonatan Y; Gross PL. Peter L; Hamburg NM. Naomi M; Haniffa R. Rashan; Hanna G. George; Hanna N. Nicholas; Hegde SM. Sheila M; Hendrickson CM. Carolyn M; Hite RD. R Duncan; Hindenburg AA. Alexander A; Hope AA. Aluko A; Horowitz JM. James M; Horvat CM. Christopher M; Hudock K. Kristin; Hunt BJ. Beverley J; Husain M. Mansoor; Hyzy RC. Robert C; Iyer VN. Vivek N; Jacobson JR. Jeffrey R; Jayakumar D. Devachandran; Keller NM. Norma M; Khan A. Akram; Kim Y. Yuri; Kindzelski AL. Andrei L; King AJ. Andrew J; Knudson MM. M Margaret; Kornblith AE. Aaron E; Krishnan V. Vidya; Kutcher ME. Matthew E; Laffan MA. Michael A; Lamontagne F. Francois; Le Gal G. Grégoire; Leeper CM. Christine M; Leifer ES. Eric S; Lim G. George; Lima FG. Felipe Gallego; Linstrum K. Kelsey; Litton E. Edward; Lopez-Sendon J. Jose; Lopez-Sendon Moreno JL. Jose L; Lother SA. Sylvain A; Malhotra S. Saurabh; Marcos M. Miguel; Saud Marinez A. Andréa; Marshall JC. John C; Marten N. Nicole; Matthay MA. Michael A; McAuley DF. Daniel F; McDonald EG. Emily G; McGlothlin A. Anna; McGuinness SP. Shay P; Middeldorp S. Saskia; Montgomery SK. Stephanie K; Moore SC. Steven C; Morillo Guerrero R. Raquel; Mouncey PR. Paul R; Murthy S. Srinivas; Nair GB. Girish B; Nair R. Rahul; Nichol AD. Alistair D; Nunez-Garcia B. Brenda; Pandey A. Ambarish; Park PK. Pauline K; Parke RL. Rachael L; Parker JC. Jane C; Parnia S. Sam; Paul JD. Jonathan D; Pérez González YS. Yessica S; Pompilio M. Mauricio; Prekker ME. Matthew E; Quigley JG. John G; Rost NS. Natalia S; Rowan K. Kathryn; Santos FO. Fernanda O; Santos M. Marlene; Olombrada Santos M. Mayler; Satterwhite L. Lewis; Saunders CT. Christina T; Schutgens REG. Roger E G; Seymour CW. Christopher W; Siegal DM. Deborah M; Silva DG. Delcio G; Shankar-Hari M. Manu; Sheehan JP. John P; Singhal AB. Aneesh B; Solvason D. Dayna; Stanworth SJ. Simon J; Tritschler T. Tobias; Turner AM. Anne M; van Bentum-Puijk W. Wilma; van de Veerdonk FL. Frank L; van Diepen S. Sean; Vazquez-Grande G. Gloria; Wahid L. Lana; Wareham V. Vanessa; Wells BJ. Bryan J; Widmer RJ. R Jay; Wilson JG. Jennifer G; Yuriditsky E. Eugene; Zampieri FG. Fernando G; Angus DC. Derek C; McArthur CJ. Colin J; Webb SA. Steven A; Farkouh ME. Michael E; Hochman JS. Judith S; Zarychanski R. Ryan. The New England journal of medicine. 2021. Aug; 385(9):790-802

Thrombosis and inflammation may contribute to the risk of death and complications among patients with coronavirus disease 2019 (Covid-19). We hypothesized that therapeutic-dose anticoagulation may improve outcomes in noncritically ill patients who are hospitalized with Covid-19. Read More on PubMed

Therapeutic Anticoagulation with Heparin in Critically Ill Patients with Covid-19. . ; . ; . ; Goligher EC. Ewan C; Bradbury CA. Charlotte A; McVerry BJ. Bryan J; Lawler PR. Patrick R; Berger JS. Jeffrey S; Gong MN. Michelle N; Carrier M. Marc; Reynolds HR. Harmony R; Kumar A. Anand; Turgeon AF. Alexis F; Kornblith LZ. Lucy Z; Kahn SR. Susan R; Marshall JC. John C; Kim KS. Keri S; Houston BL. Brett L; Derde LPG. Lennie P G; Cushman M. Mary; Tritschler T. Tobias; Angus DC. Derek C; Godoy LC. Lucas C; McQuilten Z. Zoe; Kirwan BA. Bridget-Anne; Farkouh ME. Michael E; Brooks MM. Maria M; Lewis RJ. Roger J; Berry LR. Lindsay R; Lorenzi E. Elizabeth; Gordon AC. Anthony C; Ahuja T. Tania; Al-Beidh F. Farah; Annane D. Djillali; Arabi YM. Yaseen M; Aryal D. Diptesh; Baumann Kreuziger L. Lisa; Beane A. Abi; Bhimani Z. Zahra; Bihari S. Shailesh; Billett HH. Henny H; Bond L. Lindsay; Bonten M. Marc; Brunkhorst F. Frank; Buxton M. Meredith; Buzgau A. Adrian; Castellucci LA. Lana A; Chekuri S. Sweta; Chen JT. Jen-Ting; Cheng AC. Allen C; Chkhikvadze T. Tamta; Coiffard B. Benjamin; Contreras A. Aira; Costantini TW. Todd W; de Brouwer S. Sophie; Detry MA. Michelle A; Duggal A. Abhijit; Džavík V. Vladimír; Effron MB. Mark B; Eng HF. Heather F; Escobedo J. Jorge; Estcourt LJ. Lise J; Everett BM. Brendan M; Fergusson DA. Dean A; Fitzgerald M. Mark; Fowler RA. Robert A; Froess JD. Joshua D; Fu Z. Zhuxuan; Galanaud JP. Jean P; Galen BT. Benjamin T; Gandotra S. Sheetal; Girard TD. Timothy D; Goodman AL. Andrew L; Goossens H. Herman; Green C. Cameron; Greenstein YY. Yonatan Y; Gross PL. Peter L; Haniffa R. Rashan; Hegde SM. Sheila M; Hendrickson CM. Carolyn M; Higgins AM. Alisa M; Hindenburg AA. Alexander A; Hope AA. Aluko A; Horowitz JM. James M; Horvat CM. Christopher M; Huang DT. David T; Hudock K. Kristin; Hunt BJ. Beverley J; Husain M. Mansoor; Hyzy RC. Robert C; Jacobson JR. Jeffrey R; Jayakumar D. Devachandran; Keller NM. Norma M; Khan A. Akram; Kim Y. Yuri; Kindzelski A. Andrei; King AJ. Andrew J; Knudson MM. M Margaret; Kornblith AE. Aaron E; Kutcher ME. Matthew E; Laffan MA. Michael A; Lamontagne F. Francois; Le Gal G. Grégoire; Leeper CM. Christine M; Leifer ES. Eric S; Lim G. George; Gallego Lima F. Felipe; Linstrum K. Kelsey; Litton E. Edward; Lopez-Sendon J. Jose; Lother SA. Sylvain A; Marten N. Nicole; Saud Marinez A. Andréa; Martinez M. Mary; Mateos Garcia E. Eduardo; Mavromichalis S. Stavroula; McAuley DF. Daniel F; McDonald EG. Emily G; McGlothlin A. Anna; McGuinness SP. Shay P; Middeldorp S. Saskia; Montgomery SK. Stephanie K; Mouncey PR. Paul R; Murthy S. Srinivas; Nair GB. Girish B; Nair R. Rahul; Nichol AD. Alistair D; Nicolau JC. Jose C; Nunez-Garcia B. Brenda; Park JJ. John J; Park PK. Pauline K; Parke RL. Rachael L; Parker JC. Jane C; Parnia S. Sam; Paul JD. Jonathan D; Pompilio M. Mauricio; Quigley JG. John G; Rosenson RS. Robert S; Rost NS. Natalia S; Rowan K. Kathryn; Santos FO. Fernanda O; Santos M. Marlene; Santos MO. Mayler O; Satterwhite L. Lewis; Saunders CT. Christina T; Schreiber J. Jake; Schutgens REG. Roger E G; Seymour CW. Christopher W; Siegal DM. Deborah M; Silva DG. Delcio G; Singhal AB. Aneesh B; Slutsky AS. Arthur S; Solvason D. Dayna; Stanworth SJ. Simon J; Turner AM. Anne M; van Bentum-Puijk W. Wilma; van de Veerdonk FL. Frank L; van Diepen S. Sean; Vazquez-Grande G. Gloria; Wahid L. Lana; Wareham V. Vanessa; Widmer RJ. R Jay; Wilson JG. Jennifer G; Yuriditsky E. Eugene; Zhong Y. Yongqi; Berry SM. Scott M; McArthur CJ. Colin J; Neal MD. Matthew D; Hochman JS. Judith S; Webb SA. Steven A; Zarychanski R. Ryan. The New England journal of medicine. 2021. Aug; 385(9):777-789

Thrombosis and inflammation may contribute to morbidity and mortality among patients with coronavirus disease 2019 (Covid-19). We hypothesized that therapeutic-dose anticoagulation would improve outcomes in critically ill patients with Covid-19. Read More on PubMed

Incidence of venous thromboembolism in hospitalized patients with COVID-19. Middeldorp S. Saskia; Coppens M. Michiel; van Haaps TF. Thijs F; Foppen M. Merijn; Vlaar AP. Alexander P; Müller MCA. Marcella C A; Bouman CCS. Catherine C S; Beenen LFM. Ludo F M; Kootte RS. Ruud S; Heijmans J. Jarom; Smits LP. Loek P; Bonta PI. Peter I; van Es N. Nick. Journal of thrombosis and haemostasis : JTH. 2020. Aug; 18(8):1995-2002

Coronavirus disease 2019 (COVID-19) can lead to systemic coagulation activation and thrombotic complications. Read More on PubMed

Megakaryocytes and platelet-fibrin thrombi characterize multi-organ thrombosis at autopsy in COVID-19: A case series. Rapkiewicz AV. Amy V; Mai X. Xingchen; Carsons SE. Steven E; Pittaluga S. Stefania; Kleiner DE. David E; Berger JS. Jeffrey S; Thomas S. Sarun; Adler NM. Nicole M; Charytan DM. David M; Gasmi B. Billel; Hochman JS. Judith S; Reynolds HR. Harmony R. EClinicalMedicine. 2020. Jul; 24():100434

There is increasing recognition of a prothrombotic state in COVID-19. Post-mortem examination can provide important mechanistic insights. Read More on PubMed

Assessing differential impacts of COVID-19 on black communities. Millett GA. Gregorio A; Jones AT. Austin T; Benkeser D. David; Baral S. Stefan; Mercer L. Laina; Beyrer C. Chris; Honermann B. Brian; Lankiewicz E. Elise; Mena L. Leandro; Crowley JS. Jeffrey S; Sherwood J. Jennifer; Sullivan PS. Patrick S. Annals of epidemiology. 2020. Jul; 47():37-44

Given incomplete data reporting by race, we used data on COVID-19 cases and deaths in U.S. counties to describe racial disparities in COVID-19 disease and death and associated determinants. Read More on PubMed

Incidence of thrombotic complications in critically ill ICU patients with COVID-19. Klok FA. F A; Kruip MJHA. M J H A; van der Meer NJM. N J M; Arbous MS. M S; Gommers DAMPJ. D A M P J; Kant KM. K M; Kaptein FHJ. F H J; van Paassen J. J; Stals MAM. M A M; Huisman MV. M V; Endeman H. H. Thrombosis research. 2020. Jul; 191():145-147

COVID-19 may predispose to both venous and arterial thromboembolism due to excessive inflammation, hypoxia, immobilisation and diffuse intravascular coagulation. Reports on the incidence of thrombotic complications are however not available. Read More on PubMed

COVID-19 and coagulation: bleeding and thrombotic manifestations of SARS-CoV-2 infection. Al-Samkari H. Hanny; Karp Leaf RS. Rebecca S; Dzik WH. Walter H; Carlson JCT. Jonathan C T; Fogerty AE. Annemarie E; Waheed A. Anem; Goodarzi K. Katayoon; Bendapudi PK. Pavan K; Bornikova L. Larissa; Gupta S. Shruti; Leaf DE. David E; Kuter DJ. David J; Rosovsky RP. Rachel P. Blood. 2020. Jul; 136(4):489-500

Patients with coronavirus disease 2019 (COVID-19) have elevated D-dimer levels. Early reports describe high venous thromboembolism (VTE) and disseminated intravascular coagulation (DIC) rates, but data are limited. This multicenter retrospective study describes the rate and severity of hemostatic and thrombotic complications of 400 hospital-admitted COVID-19 patients (144 critically ill) primarily receiving standard-dose prophylactic anticoagulation. Coagulation and inflammatory parameters were compared between patients with and without coagulation-associated complications. Multivariable logistic models examined the utility of these markers in predicting coagulation-associated complications, critical illness, and death. The radiographically confirmed VTE rate was 4.8% (95% confidence interval [CI], 2.9-7.3), and the overall thrombotic complication rate was 9.5% (95% CI, 6.8-12.8). The overall and major bleeding rates were 4.8% (95% CI, 2.9-7.3) and 2.3% (95% CI, 1.0-4.2), respectively. In the critically ill, radiographically confirmed VTE and major bleeding rates were 7.6% (95% CI, 3.9-13.3) and 5.6% (95% CI, 2.4-10.7), respectively. Elevated D-dimer at initial presentation was predictive of coagulation-associated complications during hospitalization (D-dimer >2500 ng/mL, adjusted odds ratio [OR] for thrombosis, 6.79 [95% CI, 2.39-19.30]; adjusted OR for bleeding, 3.56 [95% CI, 1.01-12.66]), critical illness, and death. Additional markers at initial presentation predictive of thrombosis during hospitalization included platelet count >450 × 109/L (adjusted OR, 3.56 [95% CI, 1.27-9.97]), C-reactive protein (CRP) >100 mg/L (adjusted OR, 2.71 [95% CI, 1.26-5.86]), and erythrocyte sedimentation rate (ESR) >40 mm/h (adjusted OR, 2.64 [95% CI, 1.07-6.51]). ESR, CRP, fibrinogen, ferritin, and procalcitonin were higher in patients with thrombotic complications than in those without. DIC, clinically relevant thrombocytopenia, and reduced fibrinogen were rare and were associated with significant bleeding manifestations. Given the observed bleeding rates, randomized trials are needed to determine any potential benefit of intensified anticoagulant prophylaxis in COVID-19 patients. Read More on PubMed

Hospitalization and Mortality among Black Patients and White Patients with Covid-19. Price-Haywood EG. Eboni G; Burton J. Jeffrey; Fort D. Daniel; Seoane L. Leonardo. The New England journal of medicine. 2020. Jun; 382(26):2534-2543

Many reports on coronavirus disease 2019 (Covid-19) have highlighted age- and sex-related differences in health outcomes. More information is needed about racial and ethnic differences in outcomes from Covid-19. Read More on PubMed

COVID-19 and Thrombotic or Thromboembolic Disease: Implications for Prevention, Antithrombotic Therapy, and Follow-Up: JACC State-of-the-Art Review. Bikdeli B. Behnood; Madhavan MV. Mahesh V; Jimenez D. David; Chuich T. Taylor; Dreyfus I. Isaac; Driggin E. Elissa; Nigoghossian C. Caroline Der; Ageno W. Walter; Madjid M. Mohammad; Guo Y. Yutao; Tang LV. Liang V; Hu Y. Yu; Giri J. Jay; Cushman M. Mary; Quéré I. Isabelle; Dimakakos EP. Evangelos P; Gibson CM. C Michael; Lippi G. Giuseppe; Favaloro EJ. Emmanuel J; Fareed J. Jawed; Caprini JA. Joseph A; Tafur AJ. Alfonso J; Burton JR. John R; Francese DP. Dominic P; Wang EY. Elizabeth Y; Falanga A. Anna; McLintock C. Claire; Hunt BJ. Beverley J; Spyropoulos AC. Alex C; Barnes GD. Geoffrey D; Eikelboom JW. John W; Weinberg I. Ido; Schulman S. Sam; Carrier M. Marc; Piazza G. Gregory; Beckman JA. Joshua A; Steg PG. P Gabriel; Stone GW. Gregg W; Rosenkranz S. Stephan; Goldhaber SZ. Samuel Z; Parikh SA. Sahil A; Monreal M. Manuel; Krumholz HM. Harlan M; Konstantinides SV. Stavros V; Weitz JI. Jeffrey I; Lip GYH. Gregory Y H; . . Journal of the American College of Cardiology. 2020. Jun; 75(23):2950-2973

Coronavirus disease-2019 (COVID-19), a viral respiratory illness caused by the severe acute respiratory syndrome-coronavirus-2 (SARS-CoV-2), may predispose patients to thrombotic disease, both in the venous and arterial circulations, because of excessive inflammation, platelet activation, endothelial dysfunction, and stasis. In addition, many patients receiving antithrombotic therapy for thrombotic disease may develop COVID-19, which can have implications for choice, dosing, and laboratory monitoring of antithrombotic therapy. Moreover, during a time with much focus on COVID-19, it is critical to consider how to optimize the available technology to care for patients without COVID-19 who have thrombotic disease. Herein, the authors review the current understanding of the pathogenesis, epidemiology, management, and outcomes of patients with COVID-19 who develop venous or arterial thrombosis, of those with pre-existing thrombotic disease who develop COVID-19, or those who need prevention or care for their thrombotic disease during the COVID-19 pandemic. Read More on PubMed

Anticoagulant treatment is associated with decreased mortality in severe coronavirus disease 2019 patients with coagulopathy. Tang N. Ning; Bai H. Huan; Chen X. Xing; Gong J. Jiale; Li D. Dengju; Sun Z. Ziyong. Journal of thrombosis and haemostasis : JTH. 2020. May; 18(5):1094-1099

A relatively high mortality of severe coronavirus disease 2019 (COVID-19) is worrying, and the application of heparin in COVID-19 has been recommended by some expert consensus because of the risk of disseminated intravascular coagulation and venous thromboembolism. However, its efficacy remains to be validated. Read More on PubMed

Ethnic and socioeconomic differences in SARS-CoV-2 infection: prospective cohort study using UK Biobank. Niedzwiedz CL. Claire L; O'Donnell CA. Catherine A; Jani BD. Bhautesh Dinesh; Demou E. Evangelia; Ho FK. Frederick K; Celis-Morales C. Carlos; Nicholl BI. Barbara I; Mair FS. Frances S; Welsh P. Paul; Sattar N. Naveed; Pell JP. Jill P; Katikireddi SV. S Vittal. BMC medicine. 2020. May; 18(1):160

Understanding of the role of ethnicity and socioeconomic position in the risk of developing SARS-CoV-2 infection is limited. We investigated this in the UK Biobank study. Read More on PubMed

Clinical course and risk factors for mortality of adult inpatients with COVID-19 in Wuhan, China: a retrospective cohort study. Zhou F. Fei; Yu T. Ting; Du R. Ronghui; Fan G. Guohui; Liu Y. Ying; Liu Z. Zhibo; Xiang J. Jie; Wang Y. Yeming; Song B. Bin; Gu X. Xiaoying; Guan L. Lulu; Wei Y. Yuan; Li H. Hui; Wu X. Xudong; Xu J. Jiuyang; Tu S. Shengjin; Zhang Y. Yi; Chen H. Hua; Cao B. Bin. Lancet (London, England). 2020. Mar; 395(10229):1054-1062

Since December, 2019, Wuhan, China, has experienced an outbreak of coronavirus disease 2019 (COVID-19), caused by the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2). Epidemiological and clinical characteristics of patients with COVID-19 have been reported but risk factors for mortality and a detailed clinical course of illness, including viral shedding, have not been well described. Read More on PubMed

Black, Asian and Minority Ethnic groups in England are at increased risk of death from COVID-19: indirect standardisation of NHS mortality data. Aldridge RW. Robert W; Lewer D. Dan; Katikireddi SV. Srinivasa Vittal; Mathur R. Rohini; Pathak N. Neha; Burns R. Rachel; Fragaszy EB. Ellen B; Johnson AM. Anne M; Devakumar D. Delan; Abubakar I. Ibrahim; Hayward A. Andrew. Wellcome open research. 2020. ; 5():88

: International and UK data suggest that Black, Asian and Minority Ethnic (BAME) groups are at increased risk of infection and death from COVID-19. We aimed to explore the risk of death in minority ethnic groups in England using data reported by NHS England. : We used NHS data on patients with a positive COVID-19 test who died in hospitals in England published on 28th April, with deaths by ethnicity available from 1st March 2020 up to 5pm on 21 April 2020. We undertook indirect standardisation of these data (using the whole population of England as the reference) to produce ethnic specific standardised mortality ratios (SMRs) adjusted for age and geographical region. : The largest total number of deaths in minority ethnic groups were Indian (492 deaths) and Black Caribbean (460 deaths) groups. Adjusting for region we found a lower risk of death for White Irish (SMR 0.52; 95%CIs 0.45-0.60) and White British ethnic groups (0.88; 95%CIs 0.86-0.0.89), but increased risk of death for Black African (3.24; 95%CIs 2.90-3.62), Black Caribbean (2.21; 95%CIs 2.02-2.41), Pakistani (3.29; 95%CIs 2.96-3.64), Bangladeshi (2.41; 95%CIs 1.98-2.91) and Indian (1.70; 95%CIs 1.56-1.85) minority ethnic groups. Our analysis adds to the evidence that BAME people are at increased risk of death from COVID-19 even after adjusting for geographical region, but was limited by the lack of data on deaths outside of NHS settings and ethnicity denominator data being based on the 2011 census. Despite these limitations, we believe there is an urgent need to take action to reduce the risk of death for BAME groups and better understand why some ethnic groups experience greater risk. Actions that are likely to reduce these inequities include ensuring adequate income protection, reducing occupational risks, reducing barriers in accessing healthcare and providing culturally and linguistically appropriate public health communications. Read More on PubMed

Empirical systemic anticoagulation is associated with decreased venous thromboembolism in critically ill influenza A H1N1 acute respiratory distress syndrome patients. Obi AT. Andrea T; Tignanelli CJ. Christopher J; Jacobs BN. Benjamin N; Arya S. Shipra; Park PK. Pauline K; Wakefield TW. Thomas W; Henke PK. Peter K; Napolitano LM. Lena M. Journal of vascular surgery. Venous and lymphatic disorders. 2019. May; 7(3):317-324

An association between increased venous thromboembolism (VTE) events and influenza A H1N1 (H1N1) was noted in the first 10 patients with severe acute respiratory distress syndrome (ARDS). An empirical systemic anticoagulation protocol (heparin intravenous infusion) was initiated when autopsy of patients with severe hypoxemia confirmed multiple primary pulmonary thrombi and emboli. The purpose of this study was to examine the relationship between H1N1 and VTE events and to assess the efficacy of empirical systemic heparin anticoagulation in preventing VTE and death in H1N1 severe ARDS patients. Read More on PubMed

Understanding Infection-Induced Thrombosis: Lessons Learned From Animal Models. Beristain-Covarrubias N. Nonantzin; Perez-Toledo M. Marisol; Thomas MR. Mark R; Henderson IR. Ian R; Watson SP. Steve P; Cunningham AF. Adam F. Frontiers in immunology. 2019. ; 10():2569

Thrombosis is a common consequence of infection that is associated with poor patient outcome. Nevertheless, the mechanisms by which infection-associated thrombosis is induced, maintained and resolved are poorly understood, as is the contribution thrombosis makes to host control of infection and pathogen spread. The key difference between infection-associated thrombosis and thrombosis in other circumstances is a stronger inflammation-mediated component caused by the presence of the pathogen and its products. This inflammation triggers the activation of platelets, which may accompany damage to the endothelium, resulting in fibrin deposition and thrombus formation. This process is often referred to as thrombo-inflammation. Strikingly, despite its clinical importance and despite thrombi being induced to many different pathogens, it is still unclear whether the mechanisms underlying this process are conserved and how we can best understand this process. This review summarizes thrombosis in a variety of models, including single antigen models such as LPS, and infection models using viruses and bacteria. We provide a specific focus on Typhimurium infection as a useful model to address all stages of thrombosis during infection. We highlight how this model has helped us identify how thrombosis can appear in different organs at different times and thrombi be detected for weeks after infection in one site, yet largely be resolved within 24 h in another. Furthermore, we discuss the observation that thrombi induced to Typhimurium are largely devoid of bacteria. Finally, we discuss the value of different therapeutic approaches to target thrombosis, the potential importance of timing in their administration and the necessity to maintain normal hemostasis after treatment. Improvements in our understanding of these processes can be used to better target infection-mediated mechanisms of thrombosis. Read More on PubMed

Acute Myocardial Infarction after Laboratory-Confirmed Influenza Infection. Kwong JC. Jeffrey C; Schwartz KL. Kevin L; Campitelli MA. Michael A; Chung H. Hannah; Crowcroft NS. Natasha S; Karnauchow T. Timothy; Katz K. Kevin; Ko DT. Dennis T; McGeer AJ. Allison J; McNally D. Dayre; Richardson DC. David C; Rosella LC. Laura C; Simor A. Andrew; Smieja M. Marek; Zahariadis G. George; Gubbay JB. Jonathan B. The New England journal of medicine. 2018. Jan; 378(4):345-353

Acute myocardial infarction can be triggered by acute respiratory infections. Previous studies have suggested an association between influenza and acute myocardial infarction, but those studies used nonspecific measures of influenza infection or study designs that were susceptible to bias. We evaluated the association between laboratory-confirmed influenza infection and acute myocardial infarction. Read More on PubMed

Review: Viral infections and mechanisms of thrombosis and bleeding. Goeijenbier M. M; van Wissen M. M; van de Weg C. C; Jong E. E; Gerdes VE. V E A; Meijers JC. J C M; Brandjes DP. D P M; van Gorp EC. E C M. Journal of medical virology. 2012. Oct; 84(10):1680-96

Viral infections are associated with coagulation disorders. All aspects of the coagulation cascade, primary hemostasis, coagulation, and fibrinolysis, can be affected. As a consequence, thrombosis and disseminated intravascular coagulation, hemorrhage, or both, may occur. Investigation of coagulation disorders as a consequence of different viral infections have not been performed uniformly. Common pathways are therefore not fully elucidated. In many severe viral infections there is no treatment other than supportive measures. A better understanding of the pathophysiology behind the association of viral infections and coagulation disorders is crucial for developing therapeutic strategies. This is of special importance in case of severe complications, such as those seen in hemorrhagic viral infections, the incidence of which is increasing worldwide. To date, only a few promising targets have been discovered, meaning the implementation in a clinical context is still hampered. This review discusses non-hemorrhagic and hemorrhagic viruses for which sufficient data on the association with hemostasis and related clinical features is available. This will enable clinicians to interpret research data and place them into a perspective. Read More on PubMed

Recent respiratory infection and risk of venous thromboembolism: case-control study through a general practice database. Clayton TC. Tim C; Gaskin M. Marion; Meade TW. Tom W. International journal of epidemiology. 2011. Jun; 40(3):819-27

The association between respiratory infection and risk of heart attacks and strokes is well established. However, less evidence exists for an association between respiratory infection and venous thromboembolism (VTE). In this article, we describe the associations between respiratory infection and VTE. Read More on PubMed

Autopsy findings in eight patients with fatal H1N1 influenza. Harms PW. Paul W; Schmidt LA. Lindsay A; Smith LB. Lauren B; Newton DW. Duane W; Pletneva MA. Maria A; Walters LL. Laura L; Tomlins SA. Scott A; Fisher-Hubbard A. Amanda; Napolitano LM. Lena M; Park PK. Pauline K; Blaivas M. Mila; Fantone J. Joseph; Myers JL. Jeffrey L; Jentzen JM. Jeffrey M. American journal of clinical pathology. 2010. Jul; 134(1):27-35

A novel H1N1 influenza A virus emerged in April 2009, and rapidly reached pandemic proportions. We report a retrospective observational case study of pathologic findings in 8 patients with fatal novel H1N1 infection at the University of Michigan Health Systems (Ann Arbor) compared with 8 age-, sex-, body mass index-, and treatment-matched control subjects. Diffuse alveolar damage (DAD) in acute and organizing phases affected all patients with influenza and was accompanied by acute bronchopneumonia in 6 patients. Organizing DAD with established fibrosis was present in 1 patient with preexisting granulomatous lung disease. Only 50% of control subjects had DAD. Peripheral pulmonary vascular thrombosis occurred in 5 of 8 patients with influenza and 3 of 8 control subjects. Cytophagocytosis was seen in all influenza-related cases. The autopsy findings in our patients with novel H1N1 influenza resemble other influenza virus infections with the exception of prominent thrombosis and hemophagocytosis. The possibility of hemophagocytic syndrome should be investigated in severely ill patients with H1N1 infection. Read More on PubMed

Risk of deep vein thrombosis and pulmonary embolism after acute infection in a community setting. Smeeth L. Liam; Cook C. Claire; Thomas S. Sara; Hall AJ. Andrew J; Hubbard R. Richard; Vallance P. Patrick. Lancet (London, England). 2006. Apr; 367(9516):1075-1079

Acute infection increases the risk of arterial cardiovascular events, but effects on venous thromboembolic disease are less well established. Our aim was to investigate whether acute infections transiently increase the risk of venous thromboembolism. Read More on PubMed

Haematological manifestations in patients with severe acute respiratory syndrome: retrospective analysis. Wong RS. Raymond S M; Wu A. Alan; To KF. K F; Lee N. Nelson; Lam CW. Christopher W K; Wong CK. C K; Chan PK. Paul K S; Ng MH. Margaret H L; Yu LM. L M; Hui DS. David S; Tam JS. John S; Cheng G. Gregory; Sung JJ. Joseph J Y. BMJ (Clinical research ed.). 2003. Jun; 326(7403):1358-62

To evaluate the haematological findings of patients with severe acute respiratory syndrome (SARS). Read More on PubMed

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