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The nutritional policy in acute severe pancreatitis changed dramatically in the last two decades. After years of recommendations
for nihil per os combined with total parenteral nutrition, the policy moved to enteral nutrition delivered by jejunostomy combined
with total parenteral nutrition, than changed to only (if possible) enteral nutrition. Than enteral nutrition by nasojejunal tube was
advocated. Lately intragastric nutrition in acute severe pancreatitis is under scrutiny.
The “classical” recommendation nihil per os aimed the pancreatic rest. Meanwhile the caloric needs should be delivered by total
parenteral nutrition. Fasting has a lot of deleterious consequences: villous atrophy, decreased splanhnic blood flow, loss of epithelial
tight junctions, decreased secretion of bile salts and IgA, decreased gut associated lymphoid tissue(GALT), bacterial overgrowth
and bacterial translocation. The impaired GALT alters the macrophage priming, promotes the release of cytokines, free oxygen
species and arahidonic acid metabolits, all of them resulting in enhanced inflammatory reaction and systemic inflammatory
response syndrome (1,4,6).
By contrast, enteral nutrition preserves the integrity and the barrier function of intestinal epithelium, enhances blood
flow, avoids bacterial overgrowth and bacterial epithelial adhesion and prevents bacterial translocation. It is important to
stress that infection of pancreatic necrosis is due to enteral bacteria (1,4,6). Thus, enteral nutrition is not only a support
intervention, but a therapeutic one because it may directly influence the evolution of the disease by preventing infection of
necrotic tissue. It also promotes bowel movements, shortening the duration of paralitic ileus and decreasing intra-abdominal
pressure.
Taking into account that 65% of total immune tissues and 80% of immunoglobulin producing tissues belong to the digestive
tract (gut-associated lymphoid tissue –GALT and mucosal-associated lymphoid tissue –MALT), enteral nutrition has an important effect upon the local and systemic immune response during acute severe pancreatitis. In conclusion, fasting promotes inflammation
and enteral nutrition promotes appropriate immune function.
Several studies and meta-analysis investigated different parameters (infection rate, morbidity, mortality, rate of surgery, ICUand
hospital length-of-stay, costs) in patients with acute pancreatitis comparing enteral versus parenteral nutrition (1,4,8,10). The
last (2008) Cochrane meta-analysis showed that rates of mortality, hospital length-of-stay, local or systemic infections and of other
complications favor enteral nutrition (19). Parameters of immune response also favor enteral nutrition, which results in lower rates
of SIRS, sepsis, multiple organ dysfunction syndrome and mortality.
All these evidences translated into guideline recommendations of the European Society of Enteral and Parenteral Nutrition (7).
Whenever possible in acute severe pancreatitis enteral nutrition should be used (grade A). If needed, parenteral nutrition may be
associated to support energy and nutrients requirements. Whenever possible, the oral route should be used, if not, the alternative
is endoscopically placed naso-jejunal feeding. Feeding jejunostomy may be performed during surgery. Standard enteral formula
are well tolerated.
Today a consensus has been reached considering early enteral nutrition as standard of care in acute severe pancreatitis due to
promotion of appropriate immune response, shortening and improvement of disease evolution, decreased infection and surgery rates
and diminished costs. However, despite knowledge and commitment, the application of these principles into the daily practice is not
an easy task. Enteral nutrition in acute severe pancreatitis is still associated with many questions, which are looking for answers. |
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