Sandbox cerebral palsy
Pathophysiology
Mucosal barrier
- The gastric mucosa is protected from the acidic environment by mucus, bicarbonate, prostaglandins, and blood flow.
- This mucosal barrier consists of three protective components which include:
- Layer of epithelial cells lining.
- Layer of mucus, secreted by surface epithelial cells and Foveolar cells.
- Bicarbonate ions, secreted by the surface epithelial cells.
Mechanism of Action
- The insoluble mucus forms a protective gel-like coating over the entire surface of the gastric mucosa.
- The mucus protects the gastric mucosa from autodigestion by e.g. pepsin and from erosion by acids and other caustic materials that are ingested.
- The bicarbonate ions act to neutralize harsh acids.
- If the balance of gastric acid secretion and mucosal defenses is disrupted, acid interacts with the epithelium to cause damage
Pathogenesis
- Regardless of etiology, if the balance of gastric acid secretion and mucosal defenses is disrupted, acid interacts with the epithelium to cause damage.
- Helicobacter pylori disrupts the mucosal barrier and causes inflammation of the mucosa of the stomach and duodenum.
- As the ulcer progresses beyond the mucosa to the submucosa the inflammation causes weakening and necrosis of arterial walls, leading to pseudoaneurysm formation followed by rupture and hemorrhage.
- NSAIDs inhibit cyclooxygenase, leading to impaired mucosal defenses by decreasing mucosal prostaglandin synthesis.
- During stress, there is acid hypersecretion; therefore, the breakdown of mucosal defenses leads to injury of the mucosa and subsequent bleeding.
- Mucosal defects along with dilated and tortuous vessels in dieulafoy lesion put them at risk for rupture because of necrosis of the arterial wall from exposure to gastric acid.
| NSAIDS | |||||||||||||||||||||||||||||||||||||||||||||||
| Inhibits cycloxygenase pathway | |||||||||||||||||||||||||||||||||||||||||||||||
| COX-1 | COX-2 | ||||||||||||||||||||||||||||||||||||||||||||||
| Reduced mucosal blood flow | Reduced mucosal and bicarbonate secreation | Impaired platelet aggregation | Reduced angiogenesis | Increased leucocyte adherence | |||||||||||||||||||||||||||||||||||||||||||
| Impaired defence Impaired healing | |||||||||||||||||||||||||||||||||||||||||||||||
| Mucosal Injury | |||||||||||||||||||||||||||||||||||||||||||||||
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Pathogenesis of Crohn's disease
- Genetic component
- Stress and environmental component
- Microbial component
- Inflammatory component
Genetic Component
Genes involved
- NOD2/CARD15 gene
- OCTN1 gene
- DLG5 gene
- TLR4 gene
| Genes | Chromosome | Function | Mutation | |
|---|---|---|---|---|
| NOD2/CARD15 | 16 | 16q12.1 | Encodes a scaffolding protein important for maintaining epithelial integrity | Disrupts normal epithelial integrity |
| OCTN1 | 05 | 5q31 | Ecodes an ion channel | Alters the function of cation transporters and cell-to-cell signaling |
| DLG5 | 10 | 10q22.3 | Interact additively with the NOD2/CARD15 gene | Iincrease susceptibility to CD along with CARD15 |
| TLR4 | 09 | 9q33.1 | Lipopolysaccharide signaling, bacterial recognition, and subsequent immune response | Altered immune response to pathogens and a subsequent increase in inflammation. |
Stress and Environmental Component
- Stress signals are perceived by the central nervous system (CNS), triggering the hypothalamic-pituitary-adrenal axis and the sympathetic-adrenal-medullary axis.
- Neuroendocrine mediators released in response to stress not only modulate secretory, absorptive, and barrier functions in the gut but also increase the gut permeability.
- Stress increases gut permeability along with other factors which inlude
- Corticotropin-releasing factor
- Autonomic nervous system
- Enteric nervous system
Microbial Component
The possible mechanisms for a bacterial etiology in the development of CD include:
- Initial immune response to a specific pathogen resulting in intestinal infection
- Alterations in normal bacterial flora of the intestinal tract
- Defective mucosal barrier and overwhelming exposure to resident bacteria and their antigens and endotoxins
- Alterations to the intestinal immune response
| Infectious Pathogens Implicated in Crohn’s Disease |
|---|
| Escherichia coli
Listeria monocytogenes Yersinia enterocolitica Mycobacterium avium subspecies paratuberculosis Measles virus |
Immune Component
- Altered immune response:
- An abnormal antibody response to an unspecified bacterial antigen is mainly responsible for inflammation in Crohn's disease.
- The inflammatory response is believed to be triggered when elimination of specified microbial antigen was unsuccessful leading to altered immune response
- Dysregulation of normal mucosal immune response results in failure of phagocytosis leading to antigen persistence.
- Antigen persistance leads to antibodies production against all the normal gut flora.
- Activation resulted in secretion of tumor necrosis factor-alpha (TNF-alpha) and subsequent epithelial changes.
- Cytokine response:
- The primary precipitating event in Crohn's disease is T-cell mediated immune response.
- Activated T cells are responsible for the release of cytokines.
- The production of inflammatory cytokines results in ulceration and increased intestinal permeability.
- The characteristic granulomatous lesion seen in Crohn’s disease is evidence of a cell-mediated immune response.
- The early lesions of Crohn's disease are characterized by elevations in interleukin-4 (IL-4) and decrease in IFN-gamma, a pattern more consistent with an overactive Th2 immune response.
- Chronic lesions are associated with high levels of interleukin-2 (IL-2), interferon gamma (IFN-gamma), TNF-alpha, and interleukin-12 and -18 (IL-12 and IL-18) consistent with an Th1 immune response.
- Tumor necrosis factor appears to play a significant role in the pathogenesis of CD.
- TNF-alpha induces expression of adhesion factors that allow for inflammatory cells to infiltrate and activates macrophages to promote release of other pro-inflammatory mediators such as IFN-gamma.
- Neutralization of TNF resulted in significant decrease in inflammation.
- TNF-alpha concentrations in the stool can be used to monitor disease activity in both CD and UC.