This document summarizes the case of a 1 month 18 day old male infant presenting with projectile vomiting for 7 days and abdominal distension for 3 days. On examination, the infant has a visible lump in the epigastrium. Based on examination findings and ultrasound results showing an elongated hypertrophic pylorus, the infant is diagnosed with infantile hypertrophic pyloric stenosis. He undergoes pyloromyotomy surgery and makes a good postoperative recovery.
3. Pt name: Promod, age : 1month 18 days
s/o nagraj
kumbarpet
DOB:17/12/2014
DOA :05/02/2015.
Single/live/term /AGA term male baby born via naturalis at WCH
hospital, davangere on 17/12/2014 at 08.45 AM.
Baby cried immediately after birth.
Birth wt – 2.3 kg
4. C/C : Vomiting after each feed since 7days projectile,
non- bilious in nature.
Distension of abdomen since 3 days .
Obstetric history: Regular ANCs taken, three scan
done USGs normal,. taken iron and folicacid
supplements, taken 2 dose of TT. Pregnancy
uneventful..
Family history: ML: 5 years, 3rd NCM
G2P2L1, No h/o of similar complains in parents
5. GPE: 48 day old male baby with vomiting & excessive
crying with visible lump in epigastrium well hydrated
and alert.
Vitals: HR-128 bpm
RR- 38 cpm
CFT < 3secs
Head to toe examination:
AF- at level
Visible lump over epigastrium
Visible gastric peristalsis from lt to rt hypochondrium
7. S/E:
o CVS: S1 & S2 heard, no murmur
o R/S: B/L air entry equal, no added sounds.
o CNS: Normal
o P/A: Inspection- visible lump over epigastrium,
visible gastric peristalsis from lt to rt hypochondrium
Palpation – palpable mobile mass, firm in cosistency
in epigastrium measuring about 3 cm below liver edge
Auscultation- bowel sounds present
10. Discussion
48 days old male baby presenting with projectile non
bilious vomiting immediately after feed with visible lump
over epigastrium, visible gastric peristalsis from lt to rt
hypochondrium with ABG showing metabolic
alkalosis,hypokalemia & USG abdomen showing
hypertrophic elongated pylorus with dilated stomach
favours the diagnosis of IHPS
11. Treatment
IV antibiotics and IV fluids Isolyte-P maintainence for
20hrs.
Surgery – laparoscopic pyloromyotomy done on
06/02/2015.
Post operative 5ml feeds BM started after 5 hrs of surgery,
increasing slowly every 6 hrs.
12. Introduction
Infantile hypertrophic pyloric stenosis (IHPS) is the most
common cause of gastric outlet obstruction in children &
is one of the most frequent conditions requiring surgery in
infants.
IHPS is an acquired condition in which the
circumferential muscle layer of the pyloric sphinter
becomes thickened, resulting in narrowing & elongation
of the pyloric channel.
This produces a high-grade gastric outlet obstruction with
compensatory dilation, hypertrophy & hyperperistalsis of
stomach
13. Epidemology
The incidence of IHPS is approximately 2 to 5 per 1,000
births per year in most white populations.
Less common in India, and among black and Asian
populations, with a frequency that is one third to one-fifth
that in the white population.
The male-to-female ratio is approximately 4:1.
There is a familial link, but a hereditary propensity to the
development of IHPS is likely polygenic with no single
locus accounting for the fivefold increase in the risk of
first-degree relatives.
14. Male and female children of affected fathers carry a risk
of 5% and 2.5% respectively, of developing IHPS
Male and female children of affected mothers carry a risk
of 19% and 7%, respectively of developing IHPS
Concordance in monozygotic twins is 0.25-0.44 and that
in dizygotic twins is 0.05-0.10
16. In IHPS the pyloric ring is no longer a clearly defined
separation between the pyloric canal and duodenum
Instead the muscle of the pyloric antrum is hypertrophic (3
or more mm), which separates the normal antrum (1mm
thickness) from the duodenum
The lumen is filled with compressed and redundant
mucosa, which obstructs the passage of gastric contents
18. Etiology
It has been found that, when compared to controls, in
IHPS specimens, the muscle layer is deficient in:
– the quantity of nerve terminals
–markers for nerve-supporting cells (Neurotrophins-
peptides that govern survival of ENS neurons)
– nitric oxide synthase activity
–mRNA production for nitric oxide synthase.
Axonal degeneration in both myentric plexus &
intramuscular nerves
19. One more hypothesis is that there is dyscoordination b/w
gastric peristalsis & pyloric relaxation resulting in,
simultaneous gastric & pyloric contraction, & work
hypertrophy of the pyloric muscle.
More recently an association b/w maternal & infant
exposure to erythromycin that stimulates phase 3 MMC
(migrating myoelectric complex) activity exposing
immature pylorus to high gastric pressures was found
leading to development of IHPS .
Gastric outlet obstruction due to pylorospasm has been
reported in neonates receiving PGE infusions
20. Clinical presentation
The typical clinical presentation in a term male infant
between 3-6 wks of age having progressive, nonbilious,
projectile vomiting and demands to be re-fed soon
afterwards ("hungry vomiter")
Vomiting consistently follows every feeding & is forceful
leading to significant dehydration.
Starvation can exacerbate diminished hepatic glucoronyl
transferase activity, and indirect hyperbilirubinemia may
be seen in 1-2% of affected infants.
21. Prolonged vomiting leads to the loss of large quantities of
gastric secretions rich in H+ and Cl- .
As a result of dehydration, the kidney attempts to
conserve Na+ to maintain volume, by exchanging them
for K+ and H+ (paradoxical aciduria).
The net result is a loss of H+ and K+, which results in
hypokalemic, hypochloremic metabolic alkalosis.
Significant hypoglycemia can occur which may
precipitate seizures
22. Diagnosis
Initially suggested by the typical clinical presentation.
The hallmark of diagnosis is the finding of a small, mobile,
ovoid mass referred to as an olive in the epigastrium in a calm
infant with relaxed abdominal muscles best palpated from the
left, located in the midepigastrium beneath the liver edge..
The olive can be felt to roll under the fingertips during
sweeping motion- no other structure gives this sensation.
If the olive is not palpable in an infant who has a clinical picture
suggestive of IHPS, further studies are warranted.
23. Ultrasonography is used to measure the thickness of the
pyloric wall and the length of the pyloric canal
– normal wall thickness <2mm, IHPS >4 mm
– normal length of the pyloric canal <10 mm,
IHPS >17 mm
- diameter in IHPS > 17mm.
If USG is not diagnostic and IHPS remains a concern, the
next test of choice is an upper GI contrast studies.
The canal is outlined by a string of contrast material
coursing through spaces between redundant mucosa
(“string sign”)
26. Treatment
The preoperative treatment is directed towards correcting the
fluid, acid-base, and electrolyte losses.
Intravenous fluid therapy is begun with 0.45–0.9% saline, in 5–
10% dextrose, with the addition of KCl in concentrations of
30–50mEq/L.
the infant is rehydrated till normal urine output and the serum
bicarbonate concentration is less than 30mEq/dL, which
implies that the alkalosis has been corrected.
Correction of the alkalosis is essential to prevent postoperative
apnea, which may be associated with anaesthesia
27. Infant can undergo the Fredet-Ramstedt pylormyotomy,
which is the procedure of choice.
If the mucosa is entered (usually on the duodenal side), it
can be primarily repaired and reinforced with an omental
patch.
Large perforations are managed by closing the
pyloromyotomy, rotating the pylorus 90°, and repeating
the myotomy.
Mortality and morbidity of less that 0.5%
29. Highly effective simple, elegant, and inexpensive
operation.
Described as 'one of the most easy and gratifying
procedures performed by pediatric surgeons’, the most
consistently successful operation ever described.
Post-operative complications:
–Wound infection
– Incomplete myotomy, treated by repeat myotomy or
endoscopic balloon dilation
30. Laparoscopic pyloromyotomy is
performed for improved cosmesis
and shorter operative time.
Endoscopic balloon dilation has
been used to treat IHPS, most
patients failed balloon dilation
and were treated with
pyloromyotomy
31. Feeding can be resumed within 6 to 12 hours
postoperatively with small volume of sugar water
advancing volume & osmolarity every 2-3 hrs until infant
is taking breast milk
Post-operative vomiting may occur in up to 50% of infants,
thought to be secondary to edema of the pylorus at the
incision site
Most infants will tolerate full feeds within 24 to 48 hrs
32. Non-surgical treatment
Injection of botulinum toxin, Antispasmodics to relieve
pylorospasm
Transpyloric nasoduodenal feeding
Atropine: Oral or IV atropine has been used in a dose of
0.06 mg/kg/day in eight divided doses, increased by 0.15
mg/kg/day till vomiting ceased and remained so for a
period of 24 hours at a stretch, then substituted by oral
atropine at double the effective IV dose for 3 weeks
33. Atropine temporarily suppresses spastic contractions of
pyloric muscle in pyloric stenosis, and it resulted in
cessation of vomiting and eventual regression of pyloric
hypertrophy.
Medical management may be successful in less severe
cases, but treatment takes longer and the complication rate
from medical management was higher.
Surgical therapy is considered superior to conservative
management, since complications are seldom, long-term
results are equal, and patients get better sooner.
34. Prognosis
Most children treated for HPS have excellent short &
long-term outcomes
Postoperative USG studies have documented a return to
normal muscle thickness within 4 wks a/w healing of
pyloric muscle & return of function
35. References
Christine A Gleason, Sherin U Devaskar. Avery’s diseases
of newborn: 9th edition. 2012; 984-85
Richard J Martin, Avroy A Fanaroff, Michel C Walsh.
Fanaroff & Martin’s Neonatal and Perinatal medicine: 9th
edition 2011; 1415-18
Ashcraft, Keith W; Murphy.J Patrick. Pediatric Surgery:
6th edition.2000; 391-94
Keith T.Oldham, Paul M.Colombani, Robert P.Foglia,
Michael A.Skinner. Principles & Practice of Pediatric
Surgery: 2005; 1168-72
Google images
36. References
Christine A Gleason, Sherin U Devaskar. Avery’s
diseases of newborn: 9th edition. 2012; 984-85
Richard J Martin, Avroy A Fanaroff, Michel C Walsh.
Fanaroff & Martin’s Neonatal and Perinatal medicine:
9th edition 2011; 1415-18
Ashcraft, Keith W; Murphy.J Patrick. Pediatric Surgery:
6th edition.2000; 391-94
Keith T.Oldham, Paul M.Colombani, Robert P.Foglia,
Michael A.Skinner. Principles & Practice of Pediatric
Surgery: 2005; 1168-72
Google images