Gastroesophageal Reflux in Preterm Neonate

1. Gastroesophageal Reflux (GER) in Preterm Neonates: An Evidence Based Therapeutic Approach & Case Presentation Tauhid Ahmed Bhuiyan, PharmD Pharmacy Practice Resident (R2) King Faisal Specialist Hospital & Research Center (KFSH&RC) An Application Based Activity King Faisal Specialist Hospital and Research Center (KFSHRC) is accredited by the Accreditation Council for Pharmacy Education as a provider of continuing pharmacy education. (UAN# 0833-0000-15-036-L01-P, 0833-0000-15-036-L01-T)

2. Objectives • To discuss the general overview of gastroesophageal reflux (GER) in preterm neonates • To identify possible diagnostic measures for diagnosing GER • To provide an evidenced based therapeutic approach for management of GER • To evaluate a topic related patient case I do not have financial relationship and no actual or potential conflict of interest in relation to this activity

3. Important Terminologies • Gestational age (or “menstrual age”) ▫ First day of the last normal menstruation to day of delivery • Chronological age (or “postnatal” age) ▫ time elapsed after birth • Prematurity: ▫ Gestational age <37 weeks • Birth weight: ▫ Normal: 2500 g + ▫ Low: <2500 g ▫ Very low: <1500 g AAP. Age Terminology. Pediatrics 2004; 114:1362–64

4. Definition • “Gastroesophageal reflux (GER) is the passage of gastric contents into the esophagus with or without regurgitation and vomiting” • “Gastroesophageal reflux disease (GERD), when reflux of gastric acid contents causes troublesome symptoms and/or complications” Vandenplas Y et al. J Pediatr Gastroenterol Nutr 2009; 49:498–547

5. Gastroesophageal Reflux (GER) • Common phenomenon in all newborn infants, especially in premature babies • Normal physiological process associated with transient relaxation of the lower esophageal sphincter (LES) • Associated factors in premature babies ▫ Posture ▫ Immature esophageal motility ▫ Abundant milk intake • “Regurgitation” and “spitting up” are the two most visible symptoms Lightdale JR et al. Pediatrics 2013; 131(5):e1684-95

6. Regurgitation • “Passage of refluxed gastric contents into the pharynx or mouth and sometimes expelled out of the mouth” • Regurgitation is generally assigned as effortless and non-projectile • Occurs daily in about 50%of the infants < 3 months of age • Resolves spontaneously in most healthy infants by 12 to 14 months of age Vandenplas Y et al. J Pediatr Gastroenterol Nutr 2009; 49:498–547

7. Epidemiology • Occurs in all healthy infants ≥30 times daily that lasts <3 mins (“happy spitters”) • Common: healthy preterm > term • Dhillon AS et al., one year multicenter observation study (77 NICU in England and Wales) using standard questionnaire ▫ The incidence of symptomatic GER in those babies born before 34 weeks of gestation ~22% ▫ Common treatment strategies:  Body positioning (98%)  Placement on a slope (96%)  H2-receptor antagonists (100%)  Feed thickeners (98%)  Antacids (96%)  Prokinetic agents (79%)  Proton-pump inhibitors (65%)  Dopamine-receptor antagonists (53%)

8. Incidence of GERD • Babies with history of regurgitation, the peak prevalence of GERD, ▫ ~50% at 4 months of age ▫ 5% to 10% of infants at 12 months • Prospective birth cohort study (n=693) in children who were followed for 2 years from birth and then contacted 8 to 11 years later ▫ Children with history of frequent regurgitation (defined as >90 days of "spilling out" during the first two years of life) were relatively 2.3 times higher likelihood of reporting GERD symptoms during follow-up years (95% CI 1.3-4.0) Dhillon AS et al. Acta Paediatr 2004;93(1):88-93 Martin AJ et al. Pediatrics. 2002;109(6):1061

9. Pathogenesis of GER in Premature Babies “Multifactorial” • Relaxation of lower esophageal sphincter (LES) ▫ Linked to 92-94% of the overall GER episodes • Gastric emptying ( ↑time ≈ ↓gestational age) • Esophageal motility • Respiratory disorders (e.g. BPD) • Gastric tube (e.g. naso/oro gastric tube) ▫ Cause ↑ LES relaxation and/or ↓ gastric emptying BPD: bronchopulmonary dysplasia

10. Complications • Frequent feeding problems • Failure to thrive • Esophagitis • Lung aspiration wheezing or pneumonia ▫ Can increase the length of hospitalization • Apnea & chronic lung disease; still controversial Corvaglia L et al. Gastroenterology Research and Practice 2013

12. Diagnostic Evaluations • Constant challenge • Symptoms are nonspecific and diagnostic tests are limited due to ▫ Sensitivity and Specificity ▫ Condition of the babies History & Physical Examination ▫ Nonspecific signs: regurgitation of milk, vomiting, irritability, unexplained crying, arching, grimace, desaturation, sleep disturbances, feeding refusal, or respiratory symptoms ▫ Differential diagnoses: bilious vomiting, gastrointestinal bleeding, diarrhea, constipation, fever, lethargy, abdominal tenderness and distension, and hepatosplenomegaly Martin R. et al. Gastroesophageal reflux in premature infants. Uptodate. Accessed on: May 13, 2015

13. Available Tests • Esophageal pH probe (most widely used in preterm) ▫ Detect reflux of gastric contents (pH <4) ▫ Trans-nasal passage of microelectrode to measure pH ▫ Limitation: detection of acid refluxes only • Multiple intraluminal impedance (MII) ▫ Higher sensitivity compared to pH probe ▫ Detect both acidic and non-acidic fluid, solids, and air • Combination of latter two ▫ Best diagnostic choice, detects acid, weakly acid, and nonacid reflux episodes ▫ Recognized by both NASPGHAN & ESPGHAN NASPGHAN: North American Society for Pediatric Gastroenterology, Hepatology, and Nutrition ESPGHAN: European Society for Pediatric Gastroenterology, Hepatology, and Nutrition Martin R. et al. Gastroesophageal reflux in premature infants. Uptodate. Accessed on: May 13, 2015

14. Management Step-wise Approach: 1st line: Non-pharmacological 2nd line: Pharmacological

15. Guidelines 2009 2013

16. Goals of Therapy • Short term: ▫ Minimize signs and symptoms ▫ Prevent adverse drug reactions ▫ Improve health related outcomes (e.g. weight gain) • Long term: ▫ Prevention of development of GERD

17. Non-pharmacological Therapy • First-line treatment in symptomatic babies who are experiencing frequent vomiting and effortless regurgitations without significant clinical complications • Available options: Corvaglia L et al. Gastroenterology Research and Practice 2013 Body positioning Feeding strategies Feed thickening Hydrolyzed formulas

18. Body Posture • Widely used: prone or left-side positions • Ewer et al. [1999] studied prospectively using 24h lower esophageal pH monitoring in 18 preterm (<37 weeks of gestation) who received full feeds (150 ml/kg/day) ▫ Infants were nursed for 8 hours in three positions (prone, left, right lateral) ▫ Results: Ewer AK. et al. Arch Dis Child Fetal Neonatal Ed 1999;81:F201–F205

19. Body Posture Cont. • Omari TI et al. [2004] combined esophageal manometry and MII to investigate the efficacy of left vs. right lateral position on GER in 10 healthy preterm (35-37 wks) ▫ Compared to right lateral position, left lateral position had significantly less  GER (P < .01)  Higher proportion of liquid GER (P < .05)  Faster GE (P < .005) Omari TI. et al. J Pediatr 2004;145:194-200

20. Feeding Strategies • Feeding frequency: ▫ Omari et al. [2002] observed a positive correlation between the frequency of feedings (every 2,3,or 4 hrs) and the occurrence of nonacid GER episodes with concomitant decrease in acidic GER episodes in mildly symptomatic infants ▫ Study recommendation: frequent, small volume feeds may improve GER • Bolus vs. continuous tube feedings ▫ Assessed by Jadcherla et al. [2012]: found a significant negative correlation (P < .03) between feeding duration and total GER events, number of nonacidic GERs ▫ Useful strategy: reduction in feeding flow rate (mL/min) Corvaglia L et al. Gastroenterology Research and Practice 2013

21. Available Pharmacological Options 1. Alginate-based formulations 2. Histamine-2 receptor blockers 3. Proton pump inhibitors 4. Prokinetic agents

22. Alginate-Based Formulations • Reported to be the most commonly prescribed anti- reflux medication in preterm infants with symptomatic for GER • Mechanism of action: ▫ Forms low density but viscous foamy gel in the presence of gastric acid ▫ Floats on the surface of gastric content during GER episodes • Available forms: ▫ Sodium alginate + sodium bicarbonate (Gaviscon®) • Adverse drug reactions: ▫ “Aluminum toxicity”, abdominal distension, hypernatremia, constipation (products contain aluminum), thickening of the stool and anal fissure Corvaglia L et al. Gastroenterology Research and Practice 2013

23. Clinical Evidence • Limited data • Covaglia et al. [2011] evaluated the efficacy sodium alginate (Gaviscon®) using a 24 h pH-MII in 22 symptomatic preterm newborn ▫ Sodium alginate was given 4X at alternate meals [drug-given (DG) vs. drug-free (DF) meals] and was found to have significant effect in decreasing the number of GER detected either by:  pH monitoring (DG vs. DF: median 17.00 vs. 29.00, P = 0.002)  MII (DG vs. DF: 4.0 vs. 6.00, P = 0.050)  Acid esophageal exposure (DG vs. DF: 4.0% vs. 7.6%, P = 0.030) Corvaglia L et al. Gastroenterology Research and Practice 2013

24. H2RA • FDA approved in ages ≥ 1 month • Mechanism of action: ▫ Decrease acid secretion by inhibiting the histamine-2 receptor on the gastric parietal cells • Available forms: ▫ Ranitidine, famotidine, cimetidine, nizatidine • Adverse drug reactions: ▫ New evidence:  Linked to infection (in VLBW) and development of necrotizing enterocolitis (NEC) ▫ Increased risk of liver disease and gynecomastia (cimetidine) Corvaglia L et al. Gastroenterology Research and Practice 2013

25. Clinical Evidence • Efficacy of use in preterm, “an issue of debate” • Kuusela AL et al. [1998] studied the optimal doses of ranitidine for both preterm and term infants ▫ 16 preterm (gestational age under 37 weeks) and term infants treated with three different bolus doses of ranitidine (0.5 mg, 1.0 mg, and 1.5 mg per kg) ▫ Results: Corvaglia L et al. Gastroenterology Research and Practice 2013 Premature & term neonates <2 weeks: Oral: 2 mg/kg/day divided every 12 hours IV: 1.5 mg/kg/day loading followed by maintenance dose every 12 hours

26. H2RA & NEC • Guillet et al. [2006] performed a retrospective case- control study on VLBW infants to investigate the association between the incidence of NEC and the use of H2-blockers, as ranitidine, famotidine, and cimetidine ▫ Found overall incidence of NEC of 7.1%, especially with longer duration (18.9 ± 15.5 days) • Recent study [2012] confirmed by Terrin et al. ▫ NEC was more frequent in infants treated with ranitidine (rate 9.8%) compared to those who did not (rate 1.6%) • Latest evidence [2013] by Bilali et al. ▫ NEC in preterm infants treated with ranitidine when compared to the control group (17.2% vs. 4.3%) Corvaglia L et al. Gastroenterology Research and Practice 2013

27. PPI • Not approved for children <1 year and clinically ineffective to relieve GER symptoms • Mechanism of action: ▫ Blocks gastric proton pump that catalyzes the final phase of the acid secretory process of parietal cells • Available forms: ▫ Omeprazole, esomeprazole, rabeprazole, lansoprazole, pantoprazole • Adverse drug reactions: ▫ Headache, diarrhea, constipation, and nausea (2% to 7%) ▫ Growing evidence of NEC & hypochlorhydria Corvaglia L et al. Gastroenterology Research and Practice 2013

28. Clinical Evidence • Data on the safety and efficacy of PPIs in the preterm population are few and somewhat controversial • Omari et al. [2007] conducted 2-week randomized, double blinded, placebo-controlled trial for effectiveness of omeprazole [dose: 0.7 mg/kg/day] on preterm infants (n= 10) with GERD ▫ Omeprazole therapy significantly reduced gastric acidity (%time pH <4, 54% vs 14%, P < 0.0005) ▫ Esophageal acid exposure (%time pH <4, 19% vs 5%, P < 0.01) ▫ Number of acid GER episodes (119 vs 60 episodes, P < 0.05) ▫ Limited by lack of sample size Corvaglia L et al. Gastroenterology Research and Practice 2013

29. Clinical Evidence • Moore DJ et al. [2003] conducted a double-blinded, randomized, placebo-controlled trial to assess the efficacy of omeprazole with GER and/or esophagitis in 30 irritable infants (3-12 months) ▫ Using visual analogue scale, irritability were measure at baseline and the end of each 2-week treatment period ▫ Results:  Reflux index fell significantly during omeprazole treatment vs. placebo (- 8.9% ± 5.6%, -1.9% ± 2.0%, P < .001)  VA score (assessed by parents) for the level of irritability while taking omeprazole or placebo did not differ significantly (n = 30, 5.0 ± 3.1 versus 5.9 ± 2.1, P = .214) • No difference in GER reduction between lansoprazole (54%) vs. placebo (54%) (Orenstein SR et al. [2009]) ▫ Rate of respiratory infection was higher in lansoprazole group (10 vs 2; P= .032) Corvaglia L et al. Gastroenterology Research and Practice 2013

30. Prokinetic Agents • Improve gastric emptying, to reduce emesis, and to enhance LES tone • Agents ▫ Cisapride ▫ Domperidone ▫ Erythromycin ▫ Metoclopramide Corvaglia L et al. Gastroenterology Research and Practice 2013

31. Cisapride (Propulsid®) • Largely investigated • Mechanism of action: ▫ Enhance the release of acetylcholine from the mesenteric plexus decreasing GER ▫ Antagonist of the rapid component of the delayed rectifier current of potassium in cardiac cells (antiarrhythmic effect) • Ariagno et al. [2001] demonstrated ▫ A significant reduction in reflux indexes and in the number of GER episodes lasting ≥5 minutes ▫ Ineffective on the total number of refluxes/24 hours and on the duration of the longest episode • Dose dependent QTc prolongation and cardiac arrhythmias—no longer used for GER Corvaglia L et al. Gastroenterology Research and Practice 2013

32. Domperidone (Motilium®) • Mechanism of action: ▫ Blocks dopamine receptors in chemoreceptor trigger zone of the CNS  Enhance the response to acetylcholine of tissue in upper GI tract causing enhanced motility and accelerated gastric emptying without stimulating gastric, biliary, or pancreatic secretions • Few evidence in infants and children but none for preterm infants • Safety alerts: ▫ Increased risk of serious adverse cardiac effects including dose dependent QTc prolongation, arrhythmias and sudden cardiac death Corvaglia L et al. Gastroenterology Research and Practice 2013

33. Erythromycin • Mechanism of actions: ▫ Strong non-peptide motilin receptor agonist that contributes to enhance gastric emptying and intra-digestive migratory motor complex • Although use of erythromycin large randomized controlled trial demonstrated significant improvement on parenteral-nutrition associated cholestasis in preterm infants, however, no significant improvement were found in resolution of GER • Adverse drug reactions: ▫ Reported cases of increased risk of infantile hypertrophic pyloric stenosis (especially use during the first 2 weeks of life) ▫ Reported cases of cardiac arrhythmias Corvaglia L et al. Gastroenterology Research and Practice 2013

34. Metoclopramide (Reglan®) • Mechanism of action: ▫ Similar to domperidone • A Cochrane review published in 2004 affirmed the effectiveness of metoclopramide in reducing both clinical symptoms and reflux indexes in infants with GERD, but limited by ▫ Conflicting results of the studies ▫ Lack of a valid demonstration of the metoclopramide‘s efficacy or toxicity • Adverse drug reactions: ▫ Irritability (most frequent), followed by dystonic reactions, drowsiness, oculogyric crisis, emesis, and, eventually, apnea Corvaglia L et al. Gastroenterology Research and Practice 2013

35. By now, you are probably here??

36. Take Home Message • Although GER is very common condition among preterm infants with unclear treatment management, ▫ Therapy should be tailored based on clinical presentation and complications ▫ Nonpharmacological management should be considered as first line  “happy spitters” ▫ To avoid any harmful overtreatment, pharmacological therapy should strictly be limited to selected infants suffering from GER complications or failure of conservative measures ▫ When choosing pharmacological options:  Consider risk vs. benefit ratio based on current evidence

37. Pharmacist Role • Provide evidence based guidance for selection of appropriate pharmacotherapeutic agents • Identify inappropriate doses, drug-drug interactions, or dose adjustments (if necessary) • Monitor adverse drug reactions • Provide bedside teaching to other health care providers (when necessary) • Provide discharge counselling to the parents and/or caregivers

38. Patient Case • SS, B.Boy twin II, preterm (32 weeks) delivered on 18th of April from an unbooked mother as a case of emergency C/S • Mother: 19 yo Saudi, female married to her 1st cousin, no known chronic illness, G1P2 + 0 • At birth: ▫ Apgar score: 6 in 1 min, 8 in 5 min ▫ Vital: Temp: Afebrile | HR 120 bpm | BP: 45/25 mmHg | RR: 40 brths/min | O2 Sat: 92% RA ▫ Physical exam: unremarkable, head circ: 29 cm, abd girth: 20.5 cm (non distended) ▫ Case of very low birth weight (VLBW): 1.13 kg • NKA • After birth, developed mild respiratory distress • Shifted to NICU with high flow nasal cannula (7 L/min)

39. NICU, Day 0 • Reason for admission: prematurity, R/O of sepsis, mild RDS, VLBW • Physical Exams: • Skin: normal • CNS: active baby • Chest: clear, on 1 L/min NC, FiO2: 21% • CVS: S1 + S2+ 0; not on any inotropes • Vitals: Temp: 36.5 | HR 125 bpm | BP: 52/25 mmHg | RR: 65 brths/min on | O2 Sat: 92% RA • GI: soft + lax; NPO, TPN (10% dextrose) + Lipids (2.5 gm/kg) • TFI: 70 mL/kg/day • Medications: • Ampicillin 55 mg IV q12h; Gentamicin 5 mg IV q36h, Caffeine Citrate 22 mg IV load followed by 6 mg IV daily, Hepatitis B immunoglobulin 100 IU IV once • Assessment: Stable patient with no active issues • Plan: Start feeding after placing OGT; US (head) next week

40. NICU, Day 1 • CNS: active, moving all four limbs • CVS: HD stable; BP: 60/29 mmHg; HR: 130’s • Resp: On 0.5 L/min NC; on/off tachypnea; O2 sat: 98% • GI: started feeding according to the protocol; UOP: 3.9 ml/kg/hr • Lab: • Medication: same • Assessment: stable • Plan: ▫ Keep O2 sat >92% with supplemental oxygen ▫ CXR, CBC daily, CRP, blood culture, blood glucose q8h ▫ Continue same management & increase TFI to 110 mL/kg/day Na: 145 K: 4.8 Cl: 110 CO2: 19.2 BUN: 3.2 Cr: 82 WBC: 5 Hgb: 16.7 Hct: 46.7 Plt: 179 Glu: 3.1 Ca: 2.33 PO41.62 Alb: 31 ALP: 198 AST: 5 Tot. Bill: 84.3

41. NICU, Day 2 • CNS: very active; Temp: afebrile • CVS: HD stable; BP: 55/32 mmHg; HR: 130’s • Resp: still on NC; RR: 65-32; O2 sat: 95% • GI: feeding per protocol; UOP: 3.8 ml/kg/hr; Abd girth: ↑ 1.5 cm and no passage of stool • Lab: unremarkable; ROP: negative; Blood culture: no growth • Medication: same • Assessment: stable, mild RDS • Plan: ▫ D/C antibiotic; oxygen ▫ Glycerin suppository once as needed ▫ Preparation for transfer to HDU

42. NICU, Day 3-5 • CNS: no complaints; head circ: same • CVS: stable; BP: 60’s/30’s mmHg; HR: 130’s • Resp: At RA with occasional tachypnea; RR: 32-60 brth/min; O2 sat: >95% • GI: ▫ On full feed (5-10 mL q2-3h); TPN + lipid (same), Wt: 1.02 kg (↓ by 10 gm) ▫ Abd girth: ↑ 1.0 cm; not passing stool ▫ Vomited once (small amount) • UOP: ~3 mL/kg/hr • Medication: Caffeine Citrate 6 mg PO once daily • Plan: ▫ TFI ↑sed to 140 mL/kg/day; kept on prone position; d/c TPN

43. NICU, Week 2 (24/04—29/04) • CNS: unremarkable CVS: stable; BP: 60’s-70’s/20’s-30’s mmHg; HR: 130-190 bpm • Resp: on RA; RR: 32-45 brth/min; O2 sat: 100% • GI: ▫ Abd: soft + lax; passed stool; girth: same ▫ Feed ↑ to 13 mL q2-3h ▫ Patient kept on elevated, right lateral prone position (26/04) ▫ Frequent regurgitation and vomiting (milk); multiple times a day; feed refusal ▫ Started feed thickening on 26/04 • Lab: Wt gain: static (1.116 kg) • Medication: Caffeine Citrate 6 mg PO once daily; Ranitidine 0.56 mg IV q12h (27/04) • Plan: ▫ Continue same management; head US to R/O IVH; shift to HDU Na: 139 K: 5.8 Cl: 97 CO2: 19.9 BUN: 2.2 Cr: 58 Vomiting Frequency 26/4 27/4 28/4 29/4 2X 3X 2X --

44. Continuation of Care • HDU: Stable over the weekend; active; not crying • CNS + CVS: unremarkable; BP: 50-60’s/20-30’s; HR: 130-140 bpm • Resp: on RA; RR: 35-40; O2 sat: >98% • GI: Wt: 1.190 kg (↑ 70 gm) ▫ Abd: soft + lax; passing stool ▫ No reports of regurgitation or vomiting • TFI: 150 mL/kg/day • UOP: 6.4 mL/kg/hr • Lab: unremarkable; US: negative for IVH • Medication: Caffeine Citrate 6 mg PO once daily; Ranitidine 0.8 mg PO q12h • Plan: ▫ Start Ranitidine 2 mg PO q8h X 2-3 days if no vomiting, weight gain, improvement of feeding

Gastroesophageal Reflux in Preterm Neonate

Gastroesophageal Reflux in Preterm Neonate

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