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HP:0005521: Disseminated intravascular coagulation

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HP:0005521: Disseminated intravascular coagulation

Developed by Shray Alag, The Harker School
Sections: Correlations, Clinical Trials, and HPO

Correlations computed by analyzing all clinical trials.

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Correlated Drug Terms (12)

	Name (Synonyms)	Correlation
drug860	Cash transfer Wiki	0.50
drug3186	Quantra System Wiki	0.50
drug4009	Thrombin Generation Assay (TGA) Wiki	0.50

	Name (Synonyms)	Correlation
drug4207	Venous Draw & Testing Wiki	0.50
drug4011	Thrombomodulin Modified Thrombin Generation Assay (TGA-TM) Wiki	0.50
drug845	Capillary Collection & Testing Wiki	0.50
drug359	Aspirin 81 mg Wiki	0.50
drug1529	Fibrin generation markers assays Wiki	0.50
drug4010	Thrombin generation test assay Wiki	0.50
drug2779	PLACEBO Wiki	0.35
drug841	Cannabidiol Wiki	0.35
drug4251	Vitamin D Wiki	0.17

Correlated MeSH Terms (7)

	Name (Synonyms)	Correlation
D004211	Disseminated Intravascular Coagulation NIH	1.00
D020141	Hemostatic Disorders NIH	0.39
D001778	Blood Coagulation Disorders NIH	0.39

	Name (Synonyms)	Correlation
D014808	Vitamin D Deficiency NIH	0.18
D016638	Critical Illness NIH	0.06
D014777	Virus Diseases NIH	0.05
D007239	Infection NIH	0.02

Correlated HPO Terms (2)

	Name (Synonyms)	Correlation
HP:0001928	Abnormality of coagulation HPO	0.39
HP:0100512	Low levels of vitamin D HPO	0.18

Clinical Trials

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There are 4 clinical trials

1 Coagulation Assays in the Critically Ill Patient: a New Approach Using the Thrombomodulin-modified Thrombin Generation Assay (TGA-TM)

Inflammation and abnormalities in laboratory coagulation tests are inseparably tied. For example, coagulation abnormalities are nearly universal in septic patients. Coagulation disorders have also been reported in many patients with severe courses of Coronavirus disease 2019 (Covid-19). But it is difficult to assess these changes. Global coagulation tests have been shown to incorrectly assess in vivo coagulation in patients admitted to intensive care units. But other tests are available. Thrombin generation assay (TGA) is a laboratory test which allows the assessment of an individual's potential to generate thrombin. But also in conventional TGA the protein C system is hardly activated because of the absence of endothelial cells (containing natural thrombomodulin) in the plasma sample. Therefore the investigators add recombinant human thrombomodulin to a conventional TGA. Thereby the investigators hope to be able to depict in vivo coagulation more closely than global coagulation tests do.

NCT04356144

Conditions

Disseminated Intravascular Coagulation
Critical Illness
Sars-CoV2
Viral Infection
Coagulation Disorder, Blood
Covid19

Interventions

Diagnostic Test: Thrombin Generation Assay (TGA)
Diagnostic Test: Thrombomodulin Modified Thrombin Generation Assay (TGA-TM)

MeSH:Infection Virus Diseases Hemostatic Disorders Blood Coagulation Disorders Disseminated Intravascular Coagulation Critical Illness

HPO:Abnormality of coagulation Abnormality of the coagulation cascade Disseminated intravascular coagulation

Primary Outcomes

Description: nM;

Measure: ETP (AUC) without rhThrombomodulin (rhTM)

Time: 6 months

Description: nM;

Measure: ETP (AUC) with rhThrombomodulin (rhTM)

Time: 6 months

Description: Ratio of endogenous thrombin potential (ETP) with rhTM to ETP without rhTM

Measure: ETP-ratio

Time: 6 months

Description: Comparison of ETP-ratios from ICU patients and ETP-ratios from citrated plasma samples from healthy donors

Measure: ETP-Normalisation

Time: 6 months

2 Analysis of the Coagulopathy Developed by COVID-19 Infected Patients: Thrombin Generation Potential in COVID-19 Infected Patients

Increased D-dimers at admission of COVID-19 infected patients entering hospital due to a severe disease is a risk factor for death. Understanding this acquired coagulopathy is a prerequisite before specific interventional studies. The study investigators aim to apply a normalized and automated thrombin generation test (TGT), developed for testing the thrombotic risk (triggered by 5 pM Tissue Factor, with a purified thrombomodulin (TM) challenge) and to study its association with survival.

NCT04356950

Conditions

Sepsis
Blood Coagulation Disorders
Thrombin
Disseminated Intravascular Coagulation
COVID-19

Interventions

Other: Thrombin generation test assay
Other: Fibrin generation markers assays

MeSH:Hemostatic Disorders Blood Coagulation Disorders Disseminated Intravascular Coagulation

HPO:Abnormality of coagulation Abnormality of the coagulation cascade Disseminated intravascular coagulation

Primary Outcomes

Description: Death yes/no during hopstilization, 28 days after admittence

Measure: 28-day survival rate

Time: 1 month

Description: Seconds; without (TM-) and with (TM+) purified thrombomodulin

Measure: Absolute thrombin generation test latent period

Time: Day 0

Description: %; without (TM-) and with (TM+) purified thrombomodulin

Measure: Relative thrombin generation test latent period compared to reference plasma

Time: Day 0

Description: nmol/s; without (TM-) and with (TM+) purified thrombomodulin

Measure: Absolute thrombin generation test initial velocity

Time: Day 0

Description: %; without (TM-) and with (TM+) purified thrombomodulin

Measure: Relative thrombin generation test initial velocity compared to reference plasma

Time: Day 0

Description: %; without (TM-) and with (TM+) purified thrombomodulin

Measure: Relative thrombin generation test peak thrombin compared to reference plasma

Time: Day 0

Description: nmol/L; without (TM-) and with (TM+) purified thrombomodulin

Measure: Absolute thrombin generation test peak thrombin

Time: Day 0

Description: Seconds; without (TM-) and with (TM+) purified thrombomodulin

Measure: Absolute thrombin generation test peak thrombin time

Time: Day 0

Description: %; without (TM-) and with (TM+) purified thrombomodulin

Measure: Relative thrombin generation test peak thrombin time compared to reference plasma

Time: Day 0

Description: seconds; without (TM-) and with (TM+) purified thrombomodulin

Measure: Absolute thrombin generation test total thrombin generation time

Time: Day 0

Description: %; without (TM-) and with (TM+) purified thrombomodulin

Measure: Relative thrombin generation test total thrombin generation time compared to reference plasma

Time: Day 0

Description: Seconds; without (TM-) and with (TM+) purified thrombomodulin

Measure: Absolute thrombin generation test endogenous thrombin potential

Time: Day 0

Description: %; without (TM-) and with (TM+) purified thrombomodulin

Measure: Relative thrombin generation test endogenous thrombin potential compared to reference plasma

Time: Day 0

Secondary Outcomes

Description: Death yes/no

Measure: 3-month survival rate

Time: 3 months

Description: Yes/no

Measure: Transfer to intensive care unit during hospitalization

Time: 3 months

Description: Yes/no (deep vein thrombosis, pulmonary embolism, atherothrombosis flare, arterial thrombosis)

Measure: Thrombotic complication during hospitalization

Time: 3 months

Description: µg / L, assayed by automated enzyme linked fluorescent assay (Vidas® D-dimers Exclusion ™ II)

Measure: Plasma concentrations of D-dimers

Time: Day 0

Description: mg / L, measured by automated immunoagglutination (STA®-Liatest® FM)

Measure: Plasma concentrations of soluble fibrin monomers

Time: Day 0

3 The LEAD COVID-19 Trial: Low-risk, Early Aspirin and Vitamin D to Reduce COVID-19 Hospitalizations

Although the novel SARS-CoV-2 virus (COVD-19) is classified as an acute respiratory infection, emerging data show that morbidity and mortality are driven by disseminated intravascular coagulopathy. Untreated CAC leads to microangiopathic thromboses, causing multiple systems organ failure and consuming enormous healthcare resources. Identifying strategies to prevent CAC are therefore crucial to reducing COVID-19 hospitalization rates. The pathogenesis of CAC is unknown, but there are major overlaps between severe COVID-19 and vitamin D insufficiency (VDI). We hypothesize that VDI is a major underlying contributor to CAC. Preliminary data from severe COVID-19 patients in New Orleans support this hypothesis. The purpose of the proposed multi-center, prospective, randomized controlled trial is to test the hypothesis that low-risk, early treatment with aspirin and vitamin D in COVID-19 can mitigate the prothrombotic state and reduce hospitalization rates.

NCT04363840

Conditions

COVID
Vitamin D Deficiency
Coagulopathy
Disseminated Intravascular Coagulation

Interventions

Drug: Aspirin 81 mg
Dietary Supplement: Vitamin D

MeSH:Disseminated Intravascular Coagulation Vitamin D Deficiency

HPO:Disseminated intravascular coagulation Low levels of vitamin D

Primary Outcomes

Description: Hospitalization for COVID-19 symptoms

Measure: Hospitalization

Time: 2 weeks

4 Exploratory Assessment of the Coagulation Changes Associated With Severe Inflammation in COVID-19 Patients

This study will study the potential utility of the Quantra QPlus System in patients inflicted with COVID-19 disease.

NCT04460664

Conditions

COVID
Disseminated Intravascular Coagulation
Coagulation Disorder

Interventions

Diagnostic Test: Quantra System