| Literature DB >> 25886997 |
Jean-Charles Preiser1, Arthur R H van Zanten2, Mette M Berger3, Gianni Biolo4, Michael P Casaer5, Gordon S Doig6, Richard D Griffiths7, Daren K Heyland8, Michael Hiesmayr9, Gaetano Iapichino10, Alessandro Laviano11, Claude Pichard12, Pierre Singer13, Greet Van den Berghe14, Jan Wernerman15, Paul Wischmeyer16, Jean-Louis Vincent17.
Abstract
The results of recent large-scale clinical trials have led us to review our understanding of the metabolic response to stress and the most appropriate means of managing nutrition in critically ill patients. This review presents an update in this field, identifying and discussing a number of areas for which consensus has been reached and others where controversy remains and presenting areas for future research. We discuss optimal calorie and protein intake, the incidence and management of re-feeding syndrome, the role of gastric residual volume monitoring, the place of supplemental parenteral nutrition when enteral feeding is deemed insufficient, the role of indirect calorimetry, and potential indications for several pharmaconutrients.Entities:
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Year: 2015 PMID: 25886997 PMCID: PMC4310041 DOI: 10.1186/s13054-015-0737-8
Source DB: PubMed Journal: Crit Care ISSN: 1364-8535 Impact factor: 9.097
Areas of uncertainty – opposing views
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| Optimal caloric intake | Early match of EE. | Less than EE during the early phase. |
| Supplemental PN | When EN provision is less than 60% in early course of ICU stay not contraindicated. | Not before day 8 in patients with a body mass index of at least 17. |
| Optimal protein intake | Equal to nitrogen losses, up to 1.5 g/kg per day. | Less than nitrogen losses. |
| Re-feeding syndrome | Slowly increase nutritional support to prevent re-feeding syndrome consequences even if this results in increased energy deficit. | Early nutritional support improves outcome also in malnourished patients; re-feeding syndrome consequences should be monitored and immediately treated if necessary. |
| Role of indirect calorimetry | Yes (patients staying more than 4 days). | No. |
| Autophagy | Provision of nutrients should be reduced so as not to reduce autophagy capacity as early nutrients provoke a phenotype of suppressed autophagy in human and animal experiments, with functional consequences that impair recovery. | Although experimentally autophagy may be reduced in early critical illness, pharmacological autophagy activation remains to be tested clinically. |
| Antioxidants | Supplement in case of low levels of antioxidants. | Use pharmacological dosages. |
| Glutamine | In all patients on PN. | High-dose glutamine increases mortality in critically ill patients, regardless of route of administration. |
| Omega-3 lipid formulations | Use continuous enteral administration and avoid bolus administration. | Not beneficial in acute respiratory distress syndrome. |
| High-dose selenium 800 to 4,000 μg/day | High-dose trials (1,000 μg) show greater improvement than low-dose trials. | Potential for toxicity. |
| In selenium-replete populations, 800 to 1,000 μg may be ineffective. | ||
| Probiotics | Safe. Avoid use in pancreatitis patients with multiple organ dysfunction syndrome. | May be harmful in ICU patients when given post-pyloric with fiber. |
| Monitoring GRV | Accept GRV of 250 up to 500 mL per 6 hours. | Abandon GRV monitoring in medical patients and consider in surgical patients. |
EE, energy expenditure; EN, enteral nutrition; GRV, gastric residual volume; PN, parenteral nutrition.
Areas of consensus (ICU patients with a more than 4-day length of stay)
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| Early enteral feeding | Consider in each patient without absolute contraindication; prevents mucosal atrophy |
| Risks of overfeeding | Early phase |
| Estimation of energy expenditure | Requires indirect calorimetry – cannot be predicted by equations |
| Arginine | Not recommended in sepsis; beneficial in perioperative patients outside the ICU |
| Vitamins, trace elements | Mandatory, in nutritional doses; particularly true in parenteral nutrition |