1 / 45

Metabolic Acidosis and Congenital Diarrhea

Metabolic Acidosis and Congenital Diarrhea. Dr. Amir Bar, Bnei-Zion Medical Center, Haifa. תיאור מקרה :. היריון תקין ניתוח קיסרי, חוסר התקדמות לידה, במועד (38+ 4) מים מקוניאלים מ.ל. – 3.310 אפגר 1010 בדיקה גופנית תקינה הורים צעירים ממוצא מוסלמי, קרובי משפחה - דרגה 1

watson
Télécharger la présentation

Metabolic Acidosis and Congenital Diarrhea

An Image/Link below is provided (as is) to download presentation Download Policy: Content on the Website is provided to you AS IS for your information and personal use and may not be sold / licensed / shared on other websites without getting consent from its author. Content is provided to you AS IS for your information and personal use only. Download presentation by click this link. While downloading, if for some reason you are not able to download a presentation, the publisher may have deleted the file from their server. During download, if you can't get a presentation, the file might be deleted by the publisher.

E N D

Presentation Transcript

  1. Metabolic Acidosis and Congenital Diarrhea Dr. Amir Bar, Bnei-Zion Medical Center, Haifa

  2. תיאור מקרה : • היריון תקין • ניתוח קיסרי, חוסר התקדמות לידה, במועד (38+ 4) • מים מקוניאלים • מ.ל. – 3.310 • אפגר 10\10 • בדיקה גופנית תקינה • הורים צעירים ממוצא מוסלמי, קרובי משפחה - דרגה1 • לידה ראשונה לאחר מספר הפלות טיבעיות (בשלבים מוקדמים) • האם סובלת מחסר פקטור 5 ליידן, טופלה בקלקסן בהיריון • אב סובל מאי-סבילות לחלב פרה

  3. תיאור מקרה -המשך • מועמדת לשחרור, ביום הרביעי לחייה: • שלשולים מרובים, צהבהבים, מימיים, בחלקם עם תוכן, ללא הקאות, בטן רכה, לא תפוחה ולא רגישה • סימנים חיוניים תקינים, ללא חום סיסטמי, עירנית וחיונית, ללא נשמת, סטורציה תקינה • סימני דהידרציה קלינית, טורגור שמור

  4. ע.ג - מעבדה: (3)

  5. שלשול וחמצת מטבולית • שלשול– זיהומי ?? • העדר חום סיסטמי, עירנית וחיונית, לא "ספטית" • ללא לוקוציטוזיס, CRP תקין • תרביות שליליות (דם וצואה כולל וירוסים) • חמצת מטבולית - מישנית לשלשול או הפרעה מטבולית ראשונית ?? • שיפור הדהידרציה וההפרעה האלקטרוליטרית, ללא שיפור משמעותי בחמצת המטבולית >> הפרעה מטבולית ראשונית • הורים קרובי משפחה דרגה 1 • אין סיפור משפחתי של מחלות מטבוליות

  6. Metabolic Acidosis • Normal AG Bicarbonate loss • Renal – RTA • GI – diarrhea • Increased AG Additional anion • Sepsis – lactate • Diabetes – ketones • Inborn errors of metab. (AG = 16) (Normal WBC & CRP, Normal lactate) (Normal glucose levels, No ketonuria) (No hyperammonemia, Negative organic & amino Ac)

  7. Renal tubular Acidosis (RTA) • Normal AG, hyperchloremic metabolic acidosis resulting from either impaired HCO3 reabsorption or impaired H+ excretion • Type 1 (Distal) • Type 2 (Proximal) • Type 3 (Mixed of type 1 and 2) • Primarily in Pt with inherited carbonic anhydrase def • Type 4 • Hyperkalemic, deficiency/resistance to Aldosteron

  8. Proximal RTA: dd • Isolated (Rare) • Sporadic • Hereditary (AD, AR) • Fanconi syn (more common) glycosuria, aminoaciduria, proteinuria (LMW), phosphaturia • Primary • Sporadic • Hereditary (AD, AR) • Cystinosis, Lowe syndrome, Galactosemia, Tyrosenemia, Fructosemia, Fanconi-Bickel syndrome, Wilson disease, Mitochondrial diseases • Secodary: • Heavy metals, Outdated tetracycline, Gentamicin, Ifosfamide, Cyclosporine, tacrolimus

  9. Peritubular fluid Na+ Na+ H+ H+ K+ H2CO3 H2O Na+ Carb. Anhyd. 85% HCO3- H2O+CO2 CO2+HO- HCO3- Carb. Anhyd. Proximal Tubule HCO3- Na+ HCO3-

  10. Proximal RTA: Dx (A) Serum HCO3 levels were in the range of 7-12 • Hyperchloremic/Hypokalemic metabolic acidosis • The serum HCO3 level falls until it reaches the PT-HCO3 threshold (15-16) >> urine excretion stops • Urine is acidified (pH < 5.5) when serum HCO3 < 16 (Normal distal H+ secretion) >> RTA-2, while alkaline urine implies RTA-1 • HCO3 provision – serum HCO3 will be increased but not to the normal range, and Ur-pH will increase gradually (C) Proximal RTA is rarely isolated !!! (B) HCO3=23

  11. Distal RTA: dd • Primary • Sporadic • Hereditary (AD, AR) • Secondary • Interstitial nephritis • Obstructive uropathy • Vesicoureteral reflux • Pyelonephritis • Transplant rejection • Sickle cell nephropathy • Ehlers-Danlos syndrome • Lupus nephritis • Nephrocalcinosis • Medullary sponge kidney • Hepatic cirrhosis • Toxins/Medications • Amphotericin B • Lithium • Toluene • Cisplatin

  12. Distal Tubule Collecting duct Peritubular fluid Na+ H+ H+ H2O Cl- 15% HCO3- CO2+HO- HCO3- + NH3 H+ NH3 Cl-/NH4+

  13. Distal RTA: Dx • Ur: Na-20, K-8.8, Cl-50.6 >> Ur-AG = ( - 21.8) • Hyperchloremic/Hypokalemic M.A. • “Urine AG” (Na+ + K+ - Cl-): • Normal subjects: Met. Ac. >> acidification of the urine via NH4/Cl excretion (only the Cl is presence in the equation) >> • Negative “Urine AG” • Low urine pH • Abnormal urine acidification, low NH4/Cl excretion >> zero or positive Urine AG and high urine pH (B) Urine pH=5.0

  14. Metabolic Acidosis • Increased AG • Additional anion • Sepsis – lactate • Diabetes – ketones • Inborn errors of metab. • Normal AG • Bicarbonate loss • Renal – RTA • GI – diarrhea (Normal WBC & CRP, Normal lactate) (Normal glucose levels) (No hyperammonemia, Negative organic & amino Ac) (AG = 16)

  15. Diarrhea: Pathophysiology • Secretory diarrhea • Osmotic diarrhea • Ion transport defects • Reduced surface area • Abnormal motility

  16. Hypochloremia/Hyponatremia/Alkalosis HCO3- H+ Villus Epithelial cell Na+ Cl- - • cAMP • cGMP • Ca+2 + Secretory diarrhea GI Lumen Cl- K+ Na+ Crypt Epithelial cell K- Na+-K+/Cl

  17. Osmotic diarrhea • Diarrhea under Neocate (lactase def) • Carbohydrate free diet (glucose-Galactose malabs.) • Diarrhea during NPO

  18. Hyponatremia Hyponatremia Amino Ac Na+ Glu Na+ Bile Ac Na+ Ions Transport Defects H+ Na+ Cl- HCO3- Hyponatremia Alkalosis

  19. Diarrhea: Pathophysiology • Secretory diarrhea • Osmotic diarrhea • Ion transport defects • Reduced surface area • Abnormal motility

  20. Intractable Diarrhea of Infancy (IDI) • 1968 - 1st described by the following features: • Diarrhea in an infant <3m • Lasting > 2 w • 3 or more negative stool cultures

  21. IDI / PDI: Causes • The list of causes can be divided into: • Normal villus-crypt axis • Villus atrophy

  22. IDI / PDI: CausesA. Normal Villus • Ion transport defects • Chloride-bicarbonate exchanger (chloride-losing d.) • Sodium-hydrogen exchanger (congenital sodium d.) • Ileal bile acid receptor defect • Sodium-glucose cotransporter (glucose-galactose mal) • Micronutrient deficiency • Acrodermatitis enteropathica (zinc def) • Enzyme deficiency • Enterokinase def • Congenital short bowel

  23. IDI / PDI: CausesB.Villus Atrophy • Microvillus inclusion disease (MVID) • Tufting enteropathy • Autoimmune enteropathy • IPEX syndrome • Infectious enteropathy • Post-infectious enteropathy • Allergic enteropathy • Idiopathic

  24. Microvillus Inclusion Disease • The 2nd most common identified cause of IDI/PDI beginning in the 1st week of life (After infection) • Various names: • Microvillus inclusion disease • (microvillus inclusions in enterocytes/colonocytes - the characteristic diagnostic feature on EM) • Congenital microvillus atrophy • Familial microvillous atrophy • Davidson’s syndrome

  25. Davidson’s syndrome • 1978, Davidson et al - 5 newborns with severe, persistent diarrhea • LM: thin mucosa, villous atrophy • EM: intra-cytoplasmic cysts made up of brush border and increased secretory granules • From this 1st clinical and histologic description, MVID has been established as a distinct disease within the syndrome of IDI

  26. MVID • Typical form - 1st days of life, a severe watery diarrhea (>250-300mL/kg/d), which can be mistaken for urine • Massive diarrhea >> Life-threatening >> dehydration, electrolyte imbalance, and metabolic acidosis within hours, persists despite GI rest • Atypical clinical presentation - predominant occlusive syndrome • “Late-onset” (>1m), less severe diarrhea, secretory granules and microvillous inclusions are present, but distributed differently

  27. MVID • Crypt cells – increase in secretory granules, otherwise appear near normal on EM, well-developed brush border • In contrast, in mid- to upper villous – rare/absent microvilli, the diagnostic presence of microvillous inclusions • The colon is involved, and although it may be easier to Bx the rectum, Dx features are not easily recognized

  28. MVID: Histology • Variable degree of villous atrophy, generally w/o any inflammatory infiltrate • Staining: • Periodic Acid Schiff (PAS) - positive secretory granules and abnormal brush border pattern • CD10

  29. PAS-Control PAS-MVID CD10 - control CD10 - MVID

  30. MVID: Pathogenesis • A defect in the membrane trafficking of immature / differentiating enterocytes • Enterocyte cytoskeleton • Autosomal recessive • Affected siblings • Consanguinity • No candidate genes have been identified

  31. MVID: Tx • It is recommended that once the diagnosis of typical MVID has been made, transplant should be considered • Conversely, Pt with a late-onset or atypical MVID should not be automatically scheduled for transplant

  32. Tufting Enteropathy/Intestinal epithelial Dysplasia • Chronic watery diarrhea on the 1st few months • Dysmorphic features - in some affected infants • The long-term prognosis is variable

  33. Tufting Enteropathy:Morphology – LM • The characteristic feature is the epithelial “tufts” (80-90% of epithelial surface, in contrast to other known enteropathies <15%) + other typical findings: • Total or partial villus atrophy • Crypt hyperplasia • Normal or slightly increased density of inflammatory cells in the lamina propria • No colonic involvement

  34. Tufting Enteropathy

  35. Tufting Enteropathy: Pathogenesis • The molecular basis for TE is unknown • Defect in adhesion molecules ? • A genetic defect ?? • Cluster of patients in Malta • Involved families can have many affected infants

  36. Autoimmune Enteropathy • Villus atrophy, infiltration of activated T cells into the lamina propria • In contrast to MVID and Tufting E.: • Extra-intestinal manifestations of autoimmunity (arthritis, Membranous GN, IDDM, hepatitis, hypothyroidism, hemolytic anemia, thronbocytopenia • Rarely had a family history of unexplained infantile diarrhea • Onset frequently > 2 m life • Responsive to immune suppression Tx

  37. Autoimmune Enteropathy:Morphology • The histopathology is similar to celiac disease, except that there is a relative paucity of intraepithelial lymphocytes • Most of the affected infants have no history of gluten ingestion before the onset of diarrhea

  38. Autoimmune Enteropathy:Morphology (Cont’) • Bx: total villus atrophy, crypt hyperplasia, crypt abscesses are identified in severely affected cases • The lesions are not confined to the small bowel; can be seen in the stomach and colon • Immunohistochemistry: increase in CD3-positive lymphocytes within the epithelium and lamina propria

  39. Autoimmune Enteropathy:Pathogenesis • Circulating systemic antibody against enterocytes • The villus atrophy and crypt hyperplasia are both considered 2nd features of an autoimmune-induced injury to the gut • Immune suppression Tx: • Antibody levels decline/disappear • The titer may correlate with the volume of stool output

  40. IPEX Syndrome • IPEX is characterized by: • Immune dysregulation • Polyendocrinopathy • Enteropathy • X-linkage • The syndrome has many intestinal manifestations in common with autoimmune enteropathy, including villus atrophy with a marked infiltration into the lamina propria of activated T cells

  41. IPEX Syndrome • The genetic basis is a mutation of the FOXP3 gene, a transcription factor involved in the proliferation of CD4+ T cells • Autoimmune enteropathy • IDDM, thyroid disease, eczematous ichthyosis hemolytic anemia

  42. IDI / PDI: CausesB.Villus Atrophy • Microvillus inclusion disease (MVID) • Tufting enteropathy • Autoimmune enteropathy • IPEX syndrome • Infectious enteropathy • Post-infectious enteropathy • Allergic enteropathy • Idiopathic

  43. Thank You!

More Related