Images 12.3A–12.3D: Diffusion-weighted images and apparent diffusion coefficient (ADC) map demonstrate restricted diffusion of the thalami (red arrows).

Introduction

  Hypoxic-ischemic encephalopathy (HIE) occurs in a newborn when there is global hypoxic-ischemic brain injury.

Clinical Presentation

  Severely affected newborns have low Apgar scores at birth. Within 24 hours, they develop seizures and apnea. Patients with mild injury may make a full recovery, but survivors suffer from a spectrum of cerebral palsy and seizures. It accounts for approximately 25% of neonatal deaths. The prognosis for preterm infants is worse. Mildly affected infants may have no immediate symptoms, but are at risk of spastic weakness, cognitive delay, and vision and hearing impairments.

Radiographic Appearance and Diagnosis

  MRI is the modality of choice to image neonates with suspected HIE. There is a variable appearance depending on whether the ischemia is total or partial, whether the infant is preterm or term, and the timing of the imaging after the injury. Though there is some overlap, several main patterns are recognized in HIE. In order of descending frequency, they are:

       1.  Watershed Injury. The white matter and cortex of the vascular watershed areas are vulnerable to injury. The changes can be unilateral or bilateral and are first visible on diffusion-weighted images.

  Necrosis of the periventricular white matter is seen and is referred to as periventricular leukomalacia. This is followed by cyst formation and eventually parenchymal loss and hydrocephalus ex vacuo.

Images 12.3E–12.3J: Diffusion-weighted images and ADC map demonstrate acute infarctions of the bilateral frontal and occipital lobes and deep gray matter in a newborn with HIE.

Images 12.3K–12.3M: Axial T2-weighted images demonstrate extensive periventricular white matter hyperintensities due to periventricular leukomalacia.

Images 12.3N and 12.3O: Axial T1-weighted images demonstrate hyperintensity of the basal ganglia, thalamus, and brainstem in an infant with HIE.

  In normal, full-term newborns, the posterior limb of the internal capsule is hyperintense on T1WI and hypointense on T2WI. In infants with severe, acute HIE, absence of normal hyperintensity on T1WI is characteristic, and is known as the “absent posterior limb sign.”

       3.  Multicystic Encephalopathy. Multicystic encephalopathy occurs after infants experience mild signs of hypoxia ischemia, followed by an unexpectedly severe encephalopathy, most commonly after term birth. The presumed mechanism is a protracted, difficult delivery. It presents radiographically with multiple cysts of the white matter and cerebral cortex. The cystic cavities are traversed by a web of delicate glial strands and contain fluid, debris, and macrophages. Ulegyria refers to shrunken deep cortical gyri, usually in the parasagittal region. It is one of the leading causes of epilepsy arising from the posterior cortex.

Images 12.3P and 12.3Q: Axial T2-weighted and T1-weighted images demonstrate hyperintensity of the brainstem, basal ganglia, and thalami. There is hypointensity of the posterior limb of the internal capsule (red arrows). Images 12.3R and 12.3S: Axial T2-weighted and T1-weighted images demonstrate normal hypointensity and hyperintensity of the posterior limb of the internal capsule (yellow arrows).

  Over time, severe cases of multicystic encephalopathy may cause necrosis such that the brain essentially vanishes, leaving only the meninges remaining.

Treatment

  A number of randomized controlled trials have shown that therapeutic hypothermia is beneficial in term and late preterm newborns with HIE in both reducing mortality and improving neurodevelopment outcomes in both term and preterm infants if started before 6 hours of age.

Images 12.3T–12.3W: Axial T2-weighted and T1-weighted images demonstrate diffuse cortical signal abnormality in a patient and cystic changes in the white matter in a patient with multicystic encephalopathy.

Images 12.3X and 12.3Y: Axial and sagittal T2-weighted images demonstrate complete loss of the brain in a child with severe HIE.

References

1.  Heinz ER, Provenzale JM. Imaging findings in neonatal hypoxia: a practical review. AJR Am J Roentgenol. January 2009;192(1):41–47.

2.  Cabaj A, Bekiesińska-Figatowska M, Mądzik J. MRI patterns of hypoxic-ischemic brain injury in preterm and full term infants—classical and less common MR findings. Pol J Radiol. July–September 2012;77(3):71–76.

3.  Jacobs SE, Berg M, Hunt R, Tarnow-Mordi WO, Inder TE, Davis PG. Cooling for newborns with hypoxic ischaemic encephalopathy. Cochrane Database Syst Rev. January 2013:1.

4.  de Vries LS, Groenendaal F. Patterns of neonatal hypoxic–ischaemic brain injury. Neuroradiology. June 2010;52(6):555–566.

5.  Douglas-Escobar M, Weiss MD. Hypoxic-ischemic encephalopathy: a review for the clinician. JAMA Pediatr. April 2015;169(4):397–403.