Wilson–Mikity syndrome

Wilson–Mikity syndrome
Wilson–Mikity syndrome
Other names	Pulmonary dysmaturity syndrome
Specialty	Pediatrics

Wilson–Mikity syndrome, a form of chronic lung disease (CLD) that exists only in premature infants, leads to progressive or immediate development of respiratory distress.^[2]^[3] This rare condition affects low birth babies and is characterized by rapid development of lung emphysema after birth, requiring prolonged ventilation and oxygen supplementation.^[4] It is closely related to bronchopulmonary dysplasia (BPD), differing mainly in the lack of prior ventilatory support. All the initial patients described with Wilson–Mikity syndrome were very low birth weight infants that had no history of mechanical ventilation, yet developed a syndrome that clinically resembled BPD. Upon the death of some of these infants, autopsies showed histologic changes similar to those seen in BPD.^[5]

It was characterized by Miriam G. Wilson and Victor G. Mikity in 1960.^[6]

Symptoms and signs

The onset of respiratory difficulty occurs at the first day of life and continues up to three weeks into the infant's life, at which point treatment is needed for infant survival.^[4]

Complications

Mothers who have developed chorioamnionitis during pregnancy put their infant at higher risk for development of Wilson–Mikity syndrome.^[3] It is a rare complication that requires prolonged treatment. Infection, however, is not shown to be an etiological factor, but a correlation to chorioamnionitis is identified as a risk.^[3]^[7]

Cause

The cause of Wilson–Mikity syndrome is unknown.^[2]

Diagnosis

The diagnosis of Wilson–Mikity syndrome can be made through two distinct symptoms: analogous characteristics of respiratory distress syndrome and presence of diffuse and streaky infiltrates with small cystic changes, seen through a chest X-ray.^[2]^[7] Early screening allows for the identification of a collapsed lung, cystic changes within the lung, and possible start of right-sided heart failure.^[2] Upon autopsy, alveolar collapse and alveoli rupture can be seen. This can reduce the number of capillaries within the system and lead to cyanosis.^[2]^[4] Cyanosis occurs from chronic or intermittent respiratory distress and episodes of dyspnea (or apnea). Symptoms can develop within hours post-birth or be gradual; infants will experience transient respiratory distress,^[2]^[3] causing a lapse in diagnosis by around 30 to 40 days. Dangerous recurrent apnea (or dyspnea) can occur in the first two to six weeks postpartum. This cessation of breathing can progress to cyanosis and lung collapse.

Infants display deteriorating respiratory symptoms along with early chronic lung changes which can be seen on chest radiography.^[7] These changes are diagnosed either directly upon birth or within the first month, as the premature infant requires mechanical ventilation for survival.^{[citation needed]}

Treatment

When caught early enough, continuous, mechanical oxygen therapy can be used to reverse the infant's poor circulation and decreased blood oxygen, a symptom known as cyanosis.^[4] Improvement is gradual; however, cases show that after the first year of treatment using oxygen therapy and mechanical ventilators, infants show normal respiratory activity and are free from chest infiltrates with small cystic changes. Absence of fever (febrile), and normal white blood cell count correspond to successful reversion and allow for a positive prognosis.^[2]^[7]

When not treated properly, methods of reversion using oxygen supplementation and ventilation have the possibility to put the infant at risk for rare complications.

retrolental fibroplasia and/or oxygen toxicity within the lungs.^[2]^[7] Continued dyspnea is a sign that Wilson–Mikity syndrome is still affecting the infant. Increased ventilation to allow proper respiration is then required. Patients in recovery are slowly taken off oxygen support and eventually are able to ventilate with minimal to no respiratory distress.^[2]

There is a lack of research on the long-term effects of Wilson-Mikity into adulthood. ^[citation needed]

Epidemiology

Around 75% of affected infants survive and are able to receive oxygen therapies and treatments to overcome this disease. In fatal cases, infants do not have noticeable or substantial respiratory recovery and can develop right-sided heart failure, ultimately leading to death.^[6]^[7] Patients that are not recovering will also continue to show signs of dyspnea, respiratory distress, and continued low body weight, heightening the risk of death. Infants that survive six months or longer have substantially better prognosis.^{[citation needed]}

References

PMID 5789544
.

^
PMID 5388332
.

^
ISSN 1028-4559
.

^
PMID 5828438
.

PMID 14654617
.

^
PMID 13845104
.

^
PMID 12556928
.

Further reading

Hoepker, A; Seear, M; Petrocheilou, A; Hayes D Jr; Nair, A; Deodhar, J; Kadam, S; O'Toole, J (Oct 2008). "Wilson-Mikity syndrome: updated diagnostic criteria based on nine cases and a review of the literature". Pediatric Pulmonology. 43 (10): 1004–12.
S2CID 25580427
.

Lehman, DH (October 1969). "The Wilson-Mikity syndrome. Case report and review of literature". California Medicine. 111 (4): 298–304.
PMID 5388332
.

External links

Classification
ICD-9-CM: 770.7

fetal disease
Maternal factors
complicating pregnancy,
labour or delivery
placenta

Placenta praevia

Placental insufficiency

Twin-to-twin transfusion syndrome

chorion/amnion

Chorioamnionitis

umbilical cord

Umbilical cord prolapse

Nuchal cord

Single umbilical artery

presentation

Breech birth

Asynclitism

Shoulder presentation

Growth

Small for gestational age / Large for gestational age

Preterm birth / Postterm pregnancy

Intrauterine growth restriction

Birth trauma

scalp
Cephalohematoma

Chignon

Caput succedaneum

Subgaleal hemorrhage

Brachial plexus injury
Erb's palsy

Klumpke paralysis

Affected systems
Respiratory

Intrauterine hypoxia

Infant respiratory distress syndrome

Transient tachypnea of the newborn

Meconium aspiration syndrome

Pleural disease
Pneumothorax

Pneumomediastinum

Wilson–Mikity syndrome

Bronchopulmonary dysplasia

Cardiovascular

Pneumopericardium

Persistent fetal circulation

Bleeding and
hematologic disease

Vitamin K deficiency bleeding

HDN
ABO

Anti-Kell

Rh c

Rh D

Rh E

Hydrops fetalis

Hyperbilirubinemia

Kernicterus

Neonatal jaundice

Velamentous cord insertion

Intraventricular hemorrhage
Germinal matrix hemorrhage

Anemia of prematurity

Gastrointestinal

Ileus

Necrotizing enterocolitis

Meconium peritonitis

Integument and
thermoregulation

Erythema toxicum

Sclerema neonatorum

Nervous system

Perinatal asphyxia

Periventricular leukomalacia

Musculoskeletal

Gray baby syndrome

muscle tone
Congenital hypertonia

Congenital hypotonia

Infections

Vertically transmitted infection

Neonatal infection
rubella

herpes simplex

mycoplasma hominis

ureaplasma urealyticum

Omphalitis

Neonatal sepsis
Group B streptococcal infection

Neonatal conjunctivitis

Other

Miscarriage

Perinatal mortality
Stillbirth

Infant mortality

Neonatal withdrawal

Fetal Alcohol Spectrum Disorder

Retrieved from "https://en.wikipedia.org/w/index.php?title=Wilson–Mikity_syndrome&oldid=1195930091"

[pmid5789544-1] PMID 5789544
.

[pmid5388332-2] 
PMID 5388332
.

[:0-3] 
ISSN 1028-4559
.

[:2-4] 
PMID 5828438
.

[pmid14654617-5] PMID 14654617
.

[pmid13845104-6] 
PMID 13845104
.

[:1-7] 
PMID 12556928
.

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