FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2890639221> ?p ?o ?g. }

• W2890639221 endingPage "34" @default.
• W2890639221 startingPage "23" @default.
• W2890639221 abstract "Hypermetabolism in traumatic brain injury (TBI) is caused by massive hormonal response to stress. Hyperglycemia in acute lesions of the brain (without the presence of diabetes) is considered as a factor that enhances the damaging processes like intracellular acidosis, accumulation of extracellular glutamate, the formation of cerebral edema, a breakthrough of blood-brain barrier, hemorrhagic transformation of cerebral infarction. The predominance of anaerobic glycolysis in TBI reduces the macroergic phosphate (phosphocreatine concentration of ATP) and increases AMP. Lactic acidosis with increased lactate in the brain tissue and cerebral spinal fluid develops. Glucose intolerance during TBI promotes to violation of its metabolism. In patients with severe TBI glucose level ore than 11 mmol/l is associated with poor outcome. Intensive monitoring of blood glucose levels and maintaining normoglycemia can be effective neuroprotective intervention. Despite the violation of energy and plastic substrates utilization in acute period, artificial nutrition is one of the tenets of intensive care. Early nutritional support is important for patients with traumatic brain injury, which is associated with the development hypercatabolism syndrome with significant demand for calories and proteins in these patients. Neurointensive care patients need a special type of nutritional support in connection with the intensification of catabolism and prolonged fasting. Enteral or mixed enteral and parenteral administration of formulas (if enteral nutrition does not provide more than 60 % as needed) is recommended. Summarizing the mentioned above, it should be noted that the problem of adequate correction of hypermetabolism-hypercatabolism syndrome in patients with acute cerebral insufficiency of different genesis requires further study." @default.
• W2890639221 created "2018-09-27" @default.
• W2890639221 creator A5000233241 @default.
• W2890639221 creator A5033008417 @default.
• W2890639221 creator A5035951967 @default.
• W2890639221 date "2015-01-01" @default.
• W2890639221 modified "2023-10-18" @default.
• W2890639221 title "Nutritional Support in Critical Condition Caused by Acute Cerebral Insufficiency" @default.
• W2890639221 hasPublicationYear "2015" @default.
• W2890639221 type Work @default.
• W2890639221 sameAs 2890639221 @default.
• W2890639221 citedByCount "0" @default.
• W2890639221 crossrefType "journal-article" @default.
• W2890639221 hasAuthorship W2890639221A5000233241 @default.
• W2890639221 hasAuthorship W2890639221A5033008417 @default.
• W2890639221 hasAuthorship W2890639221A5035951967 @default.
• W2890639221 hasConcept C118552586 @default.
• W2890639221 hasConcept C126322002 @default.
• W2890639221 hasConcept C165455791 @default.
• W2890639221 hasConcept C177713679 @default.
• W2890639221 hasConcept C2777464067 @default.
• W2890639221 hasConcept C2778553927 @default.
• W2890639221 hasConcept C2779306644 @default.
• W2890639221 hasConcept C2779493303 @default.
• W2890639221 hasConcept C2780317664 @default.
• W2890639221 hasConcept C2780668416 @default.
• W2890639221 hasConcept C2781017439 @default.
• W2890639221 hasConcept C2987404301 @default.
• W2890639221 hasConcept C42219234 @default.
• W2890639221 hasConcept C44315111 @default.
• W2890639221 hasConcept C71924100 @default.
• W2890639221 hasConcept C78722104 @default.
• W2890639221 hasConceptScore W2890639221C118552586 @default.
• W2890639221 hasConceptScore W2890639221C126322002 @default.
• W2890639221 hasConceptScore W2890639221C165455791 @default.
• W2890639221 hasConceptScore W2890639221C177713679 @default.
• W2890639221 hasConceptScore W2890639221C2777464067 @default.
• W2890639221 hasConceptScore W2890639221C2778553927 @default.
• W2890639221 hasConceptScore W2890639221C2779306644 @default.
• W2890639221 hasConceptScore W2890639221C2779493303 @default.
• W2890639221 hasConceptScore W2890639221C2780317664 @default.
• W2890639221 hasConceptScore W2890639221C2780668416 @default.
• W2890639221 hasConceptScore W2890639221C2781017439 @default.
• W2890639221 hasConceptScore W2890639221C2987404301 @default.
• W2890639221 hasConceptScore W2890639221C42219234 @default.
• W2890639221 hasConceptScore W2890639221C44315111 @default.
• W2890639221 hasConceptScore W2890639221C71924100 @default.
• W2890639221 hasConceptScore W2890639221C78722104 @default.
• W2890639221 hasOpenAccess W2890639221 @default.
• W2890639221 hasRelatedWork W139504539 @default.
• W2890639221 hasRelatedWork W140474599 @default.
• W2890639221 hasRelatedWork W1985478982 @default.
• W2890639221 hasRelatedWork W2001042783 @default.
• W2890639221 hasRelatedWork W2002465455 @default.
• W2890639221 hasRelatedWork W2007375497 @default.
• W2890639221 hasRelatedWork W2080138984 @default.
• W2890639221 hasRelatedWork W2106690929 @default.
• W2890639221 hasRelatedWork W2137328684 @default.
• W2890639221 hasRelatedWork W2141592375 @default.
• W2890639221 hasRelatedWork W2288570808 @default.
• W2890639221 hasRelatedWork W2408670304 @default.
• W2890639221 hasRelatedWork W2509494639 @default.
• W2890639221 hasRelatedWork W2584031526 @default.
• W2890639221 hasRelatedWork W2606772399 @default.
• W2890639221 hasRelatedWork W2731578721 @default.
• W2890639221 hasRelatedWork W2768030132 @default.
• W2890639221 hasRelatedWork W282565610 @default.
• W2890639221 hasRelatedWork W2921713631 @default.
• W2890639221 hasRelatedWork W2964556034 @default.
• W2890639221 isParatext "false" @default.
• W2890639221 isRetracted "false" @default.
• W2890639221 magId "2890639221" @default.
• W2890639221 workType "article" @default.