Hubbry Logo
search
logo
Brain herniation avatar
Brain herniation
Brain herniation
current hub
1922735

Brain herniation

logo
Community Hub0 Subscribers
Read side by side
Brain herniation
View on Wikipedia
from Wikipedia

Cerebral herniation
MRI showing injury due to brain herniation
SpecialtyNeurology, neurosurgery Edit this on Wikidata

Brain herniation is a potentially deadly side effect of very high pressure within the skull that occurs when a part of the brain is squeezed across structures within the skull. The brain can shift across such structures as the falx cerebri, the tentorium cerebelli, and even through the foramen magnum (the hole in the base of the skull through which the spinal cord connects with the brain). Herniation can be caused by a number of factors that cause a mass effect and increase intracranial pressure (ICP): these include traumatic brain injury, intracranial hemorrhage, or brain tumor.[1]

Herniation can also occur in the absence of high ICP when mass lesions such as hematomas occur at the borders of brain compartments. In such cases local pressure is increased at the place where the herniation occurs, but this pressure is not transmitted to the rest of the brain, and therefore does not register as an increase in ICP.[2]

Because herniation puts extreme pressure on parts of the brain and thereby cuts off the blood supply to various parts of the brain, it is often fatal. Therefore, extreme measures are taken in hospital settings to prevent the condition by reducing intracranial pressure, or decompressing (draining) a hematoma which is putting local pressure on a part of the brain.

Signs and symptoms

[edit]
Decorticate posturing, with elbows, wrists and fingers flexed, and legs extended and rotated inward

Brain herniation frequently presents with abnormal posturing,[2] a characteristic positioning of the limbs indicative of severe brain damage. These patients have a lowered level of consciousness, with Glasgow Coma Scores of three to five. Coma and persistent vegetative state also occurs.[2] One or both pupils may be dilated and fail to constrict in response to light.[2] Vomiting can also occur due to compression of the vomiting center in the medulla oblongata. Severe headaches and seizures as a result of increased intracranial pressure are not uncommon. Cardiovascular and pulmonary symptoms may also be present as the brain loses function, but might also be associated with bleeding. These symptoms are known as Cushing's Triad: hypertension (with widening pulse pressure), irregular respirations (commonly Cheyne-Stokes), bradycardia and in severe cases cardiac arrest.[3][4]

Causes

[edit]

Causes of brain herniation include:[5]

Classification

[edit]
Types of brain herniation.[6]

The tentorium is an extension of the dura mater that separates the cerebellum from the cerebrum. There are two major classes of herniation: supratentorial and infratentorial. Supratentorial refers to herniation of structures normally found above the tentorial notch, and infratentorial refers to structures normally found below it.[7]

  • Supratentorial herniation

1) Uncal (transtentorial)

2) Central

3) Cingulate (subfalcine or transfalcine)

4) Transcalvarial

5) Tectal (posterior)

  • Infratentorial herniation

6) Upward (upward cerebellar or upward transtentorial)

7) Tonsillar (downward cerebellar)

Uncal herniation

[edit]

In uncal herniation, a common subtype of transtentorial herniation, the innermost part of the temporal lobe, the uncus, can be squeezed so much that it moves towards the tentorium and puts pressure on the brainstem, most notably the midbrain.[8] The tentorium is a structure within the skull formed by the dura mater of the meninges. Tissue may be stripped from the cerebral cortex in a process called decortication.[9]

The uncus can squeeze the oculomotor nerve (a.k.a. CN III), which may affect the parasympathetic input to the eye on the side of the affected nerve, causing the pupil of the affected eye to dilate and fail to constrict in response to light as it should. Pupillary dilation often precedes the somatic motor effects of CN III compression called oculomotor nerve palsy or third nerve palsy. This palsy presents as deviation of the eye to a "down and out" position due to loss of innervation to all ocular motility muscles except for the lateral rectus (innervated by abducens nerve (a.k.a. CN VI) and the superior oblique (innervated by trochlear nerve a.k.a. CN IV). The symptoms occur in this order because the parasympathetic fibers surround the motor fibers of CN III and are hence compressed first.[citation needed]

Compression of the ipsilateral posterior cerebral artery will result in ischemia of the ipsilateral primary visual cortex and contralateral visual field deficits in both eyes (contralateral homonymous hemianopsia).

Another important finding is a false localizing sign, the so-called Kernohan's notch, which results from compression of the contralateral[10] cerebral crus containing descending corticospinal and some corticobulbar tract fibers. This leads to Ipsilateral hemiparesis in reference to the herniation and contralateral hemiparesis with reference to the cerebral crus.[citation needed]

With increasing pressure and progression of the hernia there will be distortion of the brainstem leading to Duret hemorrhages (tearing of small vessels in the parenchyma) in the median and paramedian zones of the mesencephalon and pons. The rupture of these vessels leads to linear or flamed shaped hemorrhages. The disrupted brainstem can lead to decorticate posture, respiratory center depression and death. Other possibilities resulting from brain stem distortion include lethargy, slow heart rate, and pupil dilation.[9]

Uncal herniation may advance to central herniation.[7] The sliding uncus syndrome represents uncal herniation without alteration in the level of consciousness and other sequelae mentioned above.

Central herniation

[edit]

In central herniation, the diencephalon and parts of the temporal lobes of both of the cerebral hemispheres are squeezed through a notch in the tentorium cerebelli.[8][11] Transtentorial herniation can occur when the brain moves either up or down across the tentorium, called ascending and descending transtentorial herniation respectively; however descending herniation is much more common.[1] Downward herniation can stretch branches of the basilar artery (pontine arteries), causing them to tear and bleed, known as a Duret hemorrhage. The result is usually fatal.[11] Other symptoms of this type of herniation include small, fixed pupils with[12] paralysis of upward eye movement giving the characteristic appearance of "sunset eyes". Also found in these patients, often as a terminal complication is the development of diabetes insipidus due to the compression of the pituitary stalk. Radiographically, downward herniation is characterized by obliteration of the suprasellar cistern from temporal lobe herniation into the tentorial hiatus with associated compression on the cerebral peduncles. Upwards herniation, on the other hand, can be radiographically characterized by obliteration of the quadrigeminal cistern. Intracranial hypotension syndrome has been known to mimic downwards transtentorial herniation.

Cingulate herniation

[edit]
Subfalcine herniation on CT

In cingulate or subfalcine herniation, the most common type, the innermost part of the frontal lobe is scraped under part of the falx cerebri, the dura mater at the top of the head between the two hemispheres of the brain.[8][13] Cingulate herniation can be caused when one hemisphere swells and pushes the cingulate gyrus by the falx cerebri.[7] This does not put as much pressure on the brainstem as the other types of herniation, but it may interfere with blood vessels in the frontal lobes that are close to the site of injury (anterior cerebral artery), or it may progress to central herniation.[8] Interference with the blood supply can cause dangerous increases in ICP that can lead to more dangerous forms of herniation.[14] Symptoms for cingulate herniation are not well defined.[14] Usually occurring in addition to uncal herniation, cingulate herniation may present with abnormal posturing and coma.[7] Cingulate herniation is frequently believed to be a precursor to other types of herniation.[14]

Transcalvarial herniation

[edit]

In transcalvarial herniation, the brain squeezes through a fracture or a surgical site in the skull.[7] Also called "external herniation", this type of herniation may occur during craniectomy, surgery in which a flap of skull is removed, the protruding brain region preventing the piece of skull from being replaced during the operation.[1]

Upward herniation

[edit]

Increased pressure in the posterior fossa can cause the cerebellum to move up through the tentorial opening in upward, or cerebellar herniation.[8] The midbrain is pushed through the tentorial notch upward. This is also known as ascending transtentorial herniation since it occurs across the tentorium cerebelli.

Tonsillar herniation

[edit]

In tonsillar herniation, also called downward cerebellar herniation,[7] transforaminal herniation, or "coning", the cerebellar tonsils move downward through the foramen magnum possibly causing compression of the lower brainstem and upper cervical spinal cord as they pass through the foramen magnum.[8] Increased pressure on the brainstem can result in dysfunction of the centers in the brain responsible for controlling respiratory and cardiac function. The most common signs are intractable headache, head tilt, and neck stiffness due to tonsillar impaction. The level of consciousness may decrease and also give rise to flaccid paralysis. Blood pressure instability is also evident in these patients.[12]

Congenital tonsillar herniation of the cerebellum is also known as a Chiari malformation (CM), or previously an Arnold-Chiari malformation (ACM). There are four types of Chiari malformation, and they represent very different disease processes with different symptoms and prognosis. These conditions can be found in asymptomatic patients as an incidental finding, or can be so severe as to be life-threatening. This condition is now being diagnosed more frequently by radiologists, as more patients undergo MRI scans of their heads, especially upright MRI, which is more than twice as sensitive for detecting this condition.[15] Cerebellar tonsillar ectopia (CTE) is a term used by radiologists to describe cerebellar tonsils that are "low lying" but that do not meet the radiographic criteria for definition as a Chiari malformation. The currently accepted radiographic definition for a Chiari malformation is that cerebellar tonsils lie at least 5mm below the level of the foramen magnum. Some clinicians have reported that some patients appear to experience symptoms consistent with a Chiari malformation without radiographic evidence of tonsillar herniation. Sometimes these patients are described as having a 'Chiari [type] 0'.

There are many suspected causes of tonsillar herniation including: decreased or malformed posterior fossa (the lower, back part of the skull) not providing enough room for the cerebellum; hydrocephalus or abnormal CSF volume pushing the tonsils out; or dural tension pulling the brain caudally. Connective tissue disorders, such as Ehlers Danlos syndrome, can be associated.

For further evaluation of tonsillar herniation, CINE flow studies are used. This type of MRI examines flow of CSF at the cranio-cervical joint. For persons experiencing symptoms but without clear MRI evidence, especially if the symptoms are better in the supine position and worse upon standing/upright, an upright MRI may be useful.[2]

Treatment

[edit]
MRI showing damage due to herniation. This patient was left with residual disabilities including those involving movement and speech.[16]

Treatment involves removal of the etiologic mass and decompressive craniectomy. Brain herniation can cause severe disability or death. In fact, when herniation is visible on a CT scan, the prognosis for a meaningful recovery of neurological function is poor.[2] The patient may become paralyzed on the same side as the lesion causing the pressure, or damage to parts of the brain caused by herniation may cause paralysis on the side opposite the lesion.[11] Damage to the midbrain, which contains the reticular activating network which regulates consciousness, will result in coma.[11] Damage to the cardio-respiratory centers in the medulla oblongata will cause respiratory arrest and (secondarily) cardiac arrest.[11] Investigation is underway regarding the use of neuroprotective agents during the prolonged post-traumatic period of brain hypersensitivity associated with the syndrome.[17]

See also

[edit]

References

[edit]
[edit]
Revisions and contributorsEdit on WikipediaRead on Wikipedia

Brain herniation

View on Grokipedia
from Grokipedia
Brain herniation refers to the abnormal displacement of brain tissue from one intracranial compartment to another, typically through dural folds or foramina, due to increased intracranial pressure that overwhelms compensatory mechanisms such as CSF displacement or brain atrophy.[1][2] This life-threatening condition arises when supratentorial or infratentorial masses cause a shift in brain structures, potentially compressing vital areas like the brainstem and leading to rapid neurological deterioration or death without immediate intervention.[1] The primary causes of brain herniation include space-occupying lesions such as epidural or subdural hematomas, intracerebral hemorrhages, malignant cerebral infarctions, primary or metastatic tumors, cerebral abscesses, and hydrocephalus, which elevate intracranial pressure through mass effect, edema, or obstruction of cerebrospinal fluid pathways.[1][2] Other contributing factors encompass diffuse subarachnoid hemorrhage, pneumocephalus, excessive cerebrospinal fluid drainage, hypoxic-ischemic events, and metabolic derangements like hepatic encephalopathy, often precipitated by trauma, stroke, infection, or radiation therapy.[1][2] Brain herniation is classified into several types based on the direction and structures involved: subfalcine (cingulate) herniation, where the cingulate gyrus shifts under the free edge of the falx cerebri, potentially compressing the anterior cerebral artery; uncal (lateral transtentorial) herniation, involving the uncus of the temporal lobe displacing medially through the tentorial notch; central herniation, a downward shift of the diencephalon and brainstem through the tentorial incisura; tonsillar herniation, where the cerebellar tonsils protrude through the foramen magnum, risking medullary compression; upward (ascending transtentorial) herniation, caused by infratentorial masses pushing the superior cerebellum through the tentorial notch; and transcalvarial herniation, where brain tissue protrudes through a calvarial defect such as after craniectomy.[1] These patterns can occur in isolation or combination, with imaging such as CT or MRI essential for identification.[1] Clinically, brain herniation manifests with progressive symptoms including severe headache, altered mental status, pupillary abnormalities (e.g., anisocoria in uncal herniation), motor deficits such as hemiparesis or decorticate/decerebrate posturing, and the Cushing triad of hypertension, bradycardia, and irregular respirations, culminating in coma, respiratory arrest, or cardiac failure if untreated.[1][2] Prognosis is poor, with high mortality rates due to irreversible brainstem ischemia or herniation-related vascular compromise, though early recognition and interventions like mass evacuation, osmotherapy, or decompressive craniectomy can improve outcomes in select cases.[1][2]

Pathophysiology

Definition and Mechanisms

Brain herniation is defined as the abnormal displacement of brain tissue from its normal anatomical position into adjacent compartments or through fixed openings in the skull or dural partitions, such as the tentorial incisura or foramen magnum, primarily due to elevated intracranial pressure (ICP). This shift compresses critical structures, including the brainstem, cranial nerves, and cerebral vasculature, potentially leading to irreversible neurological damage or death.[1][3][4] The primary mechanisms underlying brain herniation stem from mass effects created by space-occupying lesions, such as hematomas, tumors, or cerebral edema, which generate localized or global pressure gradients between supratentorial and infratentorial compartments. These gradients force brain structures to shift across rigid barriers, like the falx cerebri or tentorium cerebelli. Central to this process is the Monro-Kellie doctrine, which posits that the skull encloses a fixed volume of intracranial contents—brain parenchyma (approximately 80%), blood (10%), and cerebrospinal fluid (CSF; 10%)—such that an increase in any one component must be offset by a decrease in the others to maintain normal ICP. Recent evolutions, such as Monro-Kellie 4.0 (as of 2025), expand this framework to incorporate dynamic elements like cerebrovascular autoregulation failure, glymphatic system dysfunction, and intracranial compartment syndrome, providing a more comprehensive understanding of ICP elevation and herniation risk.[1][3][4][5] When compensatory mechanisms, such as CSF displacement into the spinal subarachnoid space or reduction in cerebral blood volume via autoregulation, are overwhelmed, ICP rises exponentially, precipitating herniation.[1][3][4] In the detailed pathophysiological process, an initial increase in intracranial volume—often from edema, hemorrhage, or mass expansion—triggers a cascade: early compensation maintains ICP below 15–20 mmHg, but as volume exceeds this threshold (typically >10–15% of total intracranial volume), decompensation occurs, with ICP surging to 40–50 mmHg or higher. This elevated pressure distorts brain tissue, causing it to herniate through the path of least resistance, such as transtentorial or tonsillar shifts, which in turn compress the brainstem's reticular activating system and vital centers, leading to distinct herniation syndromes characterized by ischemia, infarction, and secondary injury from vascular occlusion.[1][4][3] Historical descriptions of brain herniation emerged in the late 19th and early 20th centuries, with Harvey Cushing's 1901 experimental work on increased ICP providing early insights into the physiological responses, such as the Cushing reflex, that often precede herniation. Further foundational observations included William Macewen's 1880s descriptions of uncal herniation in postmortem examinations of temporal lobe abscess cases, and James Collier's 1904 account of cerebellar tonsillar herniation. Classifications evolved throughout the 20th century, notably with Plum and Posner's 1966 delineation of the cephalic-to-caudal progression of herniation syndromes.[6][7][8][1]

Intracranial Compartments and Pressure Dynamics

The intracranial space is divided into distinct compartments by dural reflections, which play a critical role in the pathophysiology of brain herniation. The supratentorial compartment, housing the cerebral hemispheres, lies above the tentorium cerebelli, a crescent-shaped dural fold that extends from the falx cerebri posteriorly. The falx cerebri, a sickle-shaped midline septum, further subdivides the supratentorial space into left and right cerebral hemispheres. Below the tentorium lies the infratentorial compartment, containing the cerebellum and brainstem, creating a relatively rigid barrier that limits compensatory shifts in brain tissue during pressure imbalances.[9][7] Normal intracranial pressure (ICP) in adults ranges from 7 to 15 mmHg in the supine position, reflecting a balance among brain parenchyma, cerebrospinal fluid, and blood volume within the fixed cranial vault. This equilibrium is governed by the Monro-Kellie doctrine, which posits that any increase in one component's volume must be offset by a decrease in another to maintain stable ICP. As intracranial volume expands—due to edema, mass lesions, or hemorrhage—the relationship between volume and pressure follows an exponential compliance curve, initially allowing small volume changes with minimal pressure rise due to compensatory mechanisms like cerebrospinal fluid displacement. However, beyond a critical point, compliance decreases sharply, leading to exponential ICP elevation and loss of cerebral autoregulation, where blood flow becomes pressure-passive and vulnerable to ischemia.[10][11][12] Sustained ICP exceeding 20-25 mmHg compromises cerebral perfusion pressure (CPP), calculated as CPP = MAP - ICP (where MAP is mean arterial pressure), typically targeted above 60 mmHg to ensure adequate cerebral blood flow and prevent ischemia. When ICP surpasses these thresholds, herniation becomes imminent as tissue displaces across dural boundaries, exacerbating pressure gradients. A late physiological response to severe ICP elevation is Cushing's triad, characterized by systemic hypertension, bradycardia, and irregular respirations, signaling brainstem compression and decompensated intracranial dynamics.[11][13][14]

Causes and Risk Factors

Traumatic Causes

Traumatic brain herniation arises from mechanical forces that produce space-occupying lesions or diffuse swelling, resulting in elevated intracranial pressure (ICP) and displacement of brain tissue across rigid dural compartments. Primary etiologies include epidural hematomas, which form from arterial bleeding between the dura and skull, often following skull fractures; subdural hematomas, arising from venous tears and accumulating blood over the brain surface; cerebral contusions, involving bruising and microhemorrhages in cortical regions; and intracerebral hemorrhages, where bleeding occurs within brain parenchyma.[1] These lesions, combined with diffuse axonal injury (DAI)—a shearing of white matter tracts—account for most traumatic cases, as they rapidly increase brain volume and disrupt normal pressure dynamics.[15] The pathogenic sequence in traumatic herniation typically initiates with high-impact events that generate rapid acceleration-deceleration forces, propelling the brain against the skull and causing coup-contrecoup injuries: focal damage at the impact site (coup) and opposing contrecusions on the contralateral side (contrecoup).[15] This primary injury triggers secondary cascades, including vasogenic and cytotoxic edema from blood-brain barrier disruption and excitotoxic neurotransmitter release, which elevate ICP and exceed the skull's compensatory capacity, such as cerebrospinal fluid displacement.[15] As ICP surpasses 20-25 mmHg, brain tissue shifts, compressing vital structures like the brainstem and cerebral vessels, potentially culminating in herniation syndromes.[1] Trauma represents the predominant etiology of brain herniation in adults, particularly from severe traumatic brain injury (TBI), which affects approximately 2.5 million individuals annually in the United States.[15][16] Incidence is notably higher in young males, who experience TBI rates more than twice those of females, peaking in the 15-24 age group owing to involvement in motor vehicle collisions (accounting for 20% of TBI hospitalizations) and other high-risk activities.[15] Globally, approximately 27 million TBI cases occur each year (GBD 2019).[15][17] Specific examples include penetrating injuries from gunshots or blasts, which introduce foreign material or cause focal hematomas that exert localized mass effects, prompting acute uncal or transtentorial herniation without widespread swelling.[15] In non-penetrating scenarios, such as falls in older adults or vehicular assaults in youth, contusions and DAI from rotational forces similarly precipitate herniation through progressive edema and ICP escalation.[15]

Non-Traumatic Causes

Non-traumatic causes of brain herniation arise from spontaneous pathological processes that elevate intracranial pressure (ICP) through mass effect, edema, or vascular compromise, often progressing more gradually than in traumatic scenarios. These etiologies include intracerebral hemorrhage (ICH), typically hypertensive in origin, which creates a focal mass lesion that displaces brain tissue and compresses vital structures. Ischemic stroke with cytotoxic and vasogenic edema, such as in malignant middle cerebral artery infarction, leads to diffuse brain swelling and herniation if untreated. Brain tumors, whether primary like gliomas or metastatic, exert progressive mass effects, potentially causing subfalcine herniation due to midline shift. Cerebral venous thrombosis (CVT) results in venous congestion, hemorrhagic infarcts, and edema, which can precipitate transtentorial herniation in severe cases.[1][18][19] The pathophysiology in these cases involves the Monro-Kellie doctrine, where increased volume from hemorrhage, edema, or tumor growth exceeds compensatory mechanisms, raising ICP and forcing brain tissue across dural partitions. For instance, slow-growing gliomas may induce subfalcine shift over weeks, while acute CVT can cause rapid edema and herniation within days. Hepatic encephalopathy, a metabolic derangement from liver failure, triggers astrocyte swelling and cerebral edema, potentially leading to herniation in fulminant cases. Hyponatremia-induced edema similarly disrupts osmotic balance, causing brain swelling and ICP elevation, particularly if correction is mismanaged. Infectious processes like brain abscesses form encapsulated masses that mimic tumors in their compressive effects, displacing tissue and risking herniation.[1][20][21] Epidemiologically, non-traumatic brain herniation predominantly affects the elderly, with ICH incidence doubling each decade after age 35 and cerebral amyloid angiopathy contributing to up to 50% of spontaneous hemorrhages in those over 65. Hypertension is a major comorbidity, approximately doubling the risk of ICH (adjusted odds ratio 2.45-2.55), which often progresses to herniation in severe cases. Non-traumatic etiologies account for a significant proportion of herniation syndromes in older adults, driven by age-related vascular fragility and comorbidities.[19][22][23]

Clinical Presentation

General Signs and Symptoms

Brain herniation manifests through a series of universal clinical features that reflect the progressive distortion of intracranial structures due to elevated pressure. Early signs often include severe headache and vomiting, which arise from the initial rise in intracranial pressure compressing pain-sensitive structures. Altered mental status is a hallmark early indicator, progressing from mild confusion to drowsiness and obtundation, as assessed by a decline in the Glasgow Coma Scale score, typically from normal (15) to below 13 in affected patients.[11][24] As herniation advances, late universal signs emerge, including the Cushing response—characterized by hypertension, bradycardia, and irregular respirations—which signals brainstem compression and impending decompensation. Papilledema, visible as optic disc swelling on fundoscopy, develops from sustained pressure transmission to the optic nerve sheath. Abnormal motor responses such as decerebrate or decorticate posturing indicate midbrain or pontine involvement, reflecting a rostral-caudal deterioration of neurological function.[1][11][25] Systemic effects further underscore the gravity of herniation, with distinctive respiratory patterns like Cheyne-Stokes breathing evolving into central neurogenic hyperventilation or apnea due to medullary dysfunction. Autonomic instability may present as temperature dysregulation or fluctuations in blood pressure beyond the Cushing triad, contributing to overall hemodynamic chaos. For instance, in uncal herniation, early pupillary asymmetry can serve as a subtle precursor to these broader changes.[1][26] The progression of symptoms typically unfolds rapidly, from acute onset over minutes in traumatic cases to subacute evolution over hours in non-traumatic scenarios, with mortality risk escalating as brainstem reflexes are lost—reaching up to 90% in patients exhibiting decerebrate posturing. This timeline emphasizes the need for immediate intervention to halt deterioration.[1][25][27]

Type-Specific Manifestations

Brain herniation syndromes exhibit distinct neurological patterns depending on the type, reflecting the specific structures compressed during the displacement of brain tissue. These manifestations often correlate with the location of mass effect, such as supratentorial expansions causing lateralized shifts or infratentorial lesions leading to posterior fossa compression. Common patterns include hemiparesis or hemianesthesia in supratentorial herniations due to compression of the cerebral peduncles or corticospinal tracts, while infratentorial types more frequently produce ataxia, nystagmus, or cranial nerve palsies from cerebellar or brainstem involvement.[1][4] In uncal herniation, early compression of the ipsilateral oculomotor nerve results in a fixed, dilated pupil, often the first diagnostic clue, followed by contralateral hemiparesis from midbrain compression; progression may include ptosis, ophthalmoplegia, and altered consciousness, with potential ipsilateral weakness due to Kernohan's notch phenomenon.[28] Central herniation typically presents with a rostral-to-caudal deterioration, starting with small, reactive pupils and progressing to midposition fixed pupils, along with flexor posturing evolving to extensor posturing; bilateral motor deficits and the Cushing triad—hypertension, bradycardia, and irregular respirations—signal brainstem involvement, often culminating in respiratory arrest.[1] Cingulate or subfalcine herniation manifests primarily with contralateral lower extremity weakness or paresis due to anterior cerebral artery territory ischemia from pericallosal artery compression, potentially accompanied by headache or subtle altered mental status; if the dominant hemisphere is affected, aphasia (expressive, receptive, or conduction) may occur, and severe cases can lead to midline shift with anisocoria.[29] Tonsillar herniation causes rapid brainstem compression, producing neck stiffness, respiratory irregularities, and cardiorespiratory instability such as apnea or cardiac arrhythmias; diagnostic clues include pinpoint pupils, flaccid quadriplegia, and loss of oculocephalic reflexes, often progressing to coma and death without intervention.[1][30] Upward herniation, often secondary to posterior fossa masses, features Parinaud syndrome with upward gaze palsy, convergence-retraction nystagmus, and light-near dissociation, alongside possible diabetes insipidus from hypothalamic-pituitary axis disruption; motor signs may include bilateral upper extremity weakness, and vital signs can show the Cushing triad of hypertension, bradycardia, and irregular respirations.[1] Transcalvarial herniation, typically occurring through a calvarial defect post-craniotomy, presents with localized swelling, seizures, or focal neurological deficits such as hemiparesis depending on the herniated region; it may mimic paradoxical herniation with declining consciousness or autonomic instability if intracranial pressure gradients reverse.[31][32] Across types, brainstem compression commonly disrupts vital signs, leading to apnea, bradycardia, or arrhythmias, while asymmetry in pupillary responses or motor function serves as a key diagnostic indicator of lateralized herniation, distinguishing it from generalized intracranial hypertension symptoms like headache.[1][3]

Classification

Uncal Herniation

Uncal herniation, also known as transtentorial herniation, is the most common form of brain herniation and involves the displacement of the uncus—the medial portion of the parahippocampal gyrus in the temporal lobe—through the tentorial notch due to increased intracranial pressure from supratentorial masses.[28] This process typically begins with lateral and downward movement of the uncus, leading to compression of the ipsilateral oculomotor nerve (cranial nerve III) as it passes through the tentorial incisura, followed by impingement of the ipsilateral cerebral peduncle against the opposite tentorial edge.[28] The resulting brainstem distortion disrupts vital neural pathways, progressing rapidly if untreated and often stemming from conditions such as epidural or subdural hematomas, cerebral tumors, or traumatic brain injury.[28] The classic clinical triad of uncal herniation consists of an ipsilateral fixed and dilated pupil due to oculomotor nerve compression, contralateral hemiparesis from corticospinal tract involvement in the cerebral peduncle, and rapidly evolving altered consciousness reflecting brainstem dysfunction.[28] The pupillary dilation is often the earliest sign, appearing as anisocoria with the affected pupil unresponsive to light, while motor deficits may initially be subtle before worsening to decerebrate posturing.[28] This syndrome accounts for brain herniation cases in traumatic brain injury, highlighting its prevalence among supratentorial pathologies that generate focal mass effect.[33] A key complication is Kernohan's notch phenomenon, where the herniating uncus compresses the contralateral cerebral peduncle against the tentorial edge, producing false localizing signs such as ipsilateral hemiparesis that mimic the side of the primary lesion.[28] This ipsilateral motor deficit arises from midbrain deformation, potentially leading to diagnostic confusion, and underscores the need for prompt recognition to avert irreversible brainstem ischemia or respiratory arrest.[28] Early intervention can reverse uncal herniation in 50-75% of cases, emphasizing its potentially salvageable nature compared to other herniation types.[28]

Central Herniation

Central herniation, also known as central transtentorial herniation, involves the downward displacement of the diencephalon and midbrain through the tentorial incisura due to symmetric supratentorial swelling, such as from diffuse cerebral edema or mass effect.[7] This process results from elevated intracranial pressure that compresses the brainstem, leading to ischemia of perforating arteries, venous congestion, and potential Duret hemorrhages—small, slit-like bleeds in the brainstem parenchyma.[1] Unlike asymmetric herniations, central herniation produces a rostrocaudal pattern of deterioration, affecting central brain structures bilaterally without prominent lateralized cranial nerve deficits.[7] The progression occurs in distinct stages reflecting sequential brainstem compression. In the early diencephalic stage, patients exhibit small, reactive pupils (typically 1-2 mm), drowsiness or altered sensorium from reticular activating system involvement, and early Cheyne-Stokes respiration due to diencephalic dysfunction.[7][1] As herniation advances to the pontine stage, pinpoint pupils (nonreactive), deepening coma, decerebrate posturing, and irregular breathing patterns emerge, often accompanied by loss of oculocephalic reflexes.[7] The terminal medullary stage manifests as flaccid coma, fixed midposition pupils, slow gasping respirations progressing to apnea, and eventual cardiovascular collapse from compression of vital medullary centers.[1] Clinical signs are characteristically symmetric and include bilateral motor deficits, such as paratonia evolving to decorticate or decerebrate posturing, alongside respiratory instability from Cheyne-Stokes cycles to central neurogenic hyperventilation and finally apnea.[7] Hyperthermia may occur in the pontine phase due to loss of hypothalamic thermoregulation.[1] Central herniation is frequently associated with diffuse processes like anoxic brain injury or metabolic encephalopathies, where uniform supratentorial expansion precipitates the descent.[34]

Cingulate Herniation

Cingulate herniation, also known as subfalcine herniation, occurs when a hemispheric mass effect displaces the cingulate gyrus medially under the free edge of the falx cerebri, leading to compression of adjacent brain structures.[29] This displacement arises from increased intracranial pressure that overcomes compensatory mechanisms, such as those maintaining normal pressure between 8 and 28 cm H₂O, often due to unilateral supratentorial lesions like hematomas, tumors, or traumatic brain injury.[29] The mechanism involves the cingulate gyrus shifting across the midline, which can compress the pericallosal and callosomarginal branches of the anterior cerebral artery, potentially causing vascular occlusion and ischemia in the frontal lobe.[1] Clinical signs of cingulate herniation are often subtle in early stages, presenting with nonspecific symptoms such as headache, nausea, and vomiting due to elevated intracranial pressure.[29] As the herniation progresses, patients may develop contralateral leg weakness from infarction of the motor homunculus in the anterior cerebral artery territory, along with possible aphasia if dominant hemisphere structures are affected.[1] These manifestations can be overshadowed by the underlying pathology, making early detection challenging without imaging.[29] A primary risk associated with cingulate herniation is anterior cerebral artery infarction, which can result in frontal lobe ischemia, hemiparesis, and further deterioration including seizures or progression to more severe herniation syndromes.[29] Compression may also lead to effacement of the ipsilateral lateral ventricle and midline shift, exacerbating global brain compression.[1] Cingulate herniation is the most common type of supratentorial brain herniation, frequently observed in cases of unilateral lesions such as intracerebral hematomas or traumatic brain injuries, though exact incidence rates are underreported and vary by population.[29] It is particularly prevalent in settings of acute hemispheric mass effect, accounting for a significant proportion of herniation events in neurocritical care.[1]

Transcalvarial Herniation

Transcalvarial herniation involves the protrusion of edematous brain tissue through a defect in the calvarial bone, serving as a path of least resistance amid elevated intracranial pressure.[1] This type of herniation is distinct as an extracranial process, where brain parenchyma expands outward beyond the skull's integrity. It manifests in two primary forms: external herniation through acquired skull defects, such as those created by decompressive craniectomy, and herniation via congenital or developmental openings like patent fontanelles or sutures, which is more common in infants.[35] External cases often arise postoperatively, while in neonates, they may occur secondary to conditions like bacterial meningitis causing acute pressure buildup.[36] The underlying mechanism entails focal intracranial pressure surpassing the calvarial structural limits, prompting cortical extrusion and potential compression of overlying vessels against bony margins.[1] This extrusion can induce axonal stretching, venous infarction, and hemorrhagic contusions at the defect edges, exacerbating local tissue damage. Characteristic signs include visible scalp swelling or a "mushroom cap" appearance of herniated tissue at the site, particularly if the defect is narrow, along with seizures from cortical irritation and focal neurological deficits such as weakness or sensory loss in the corresponding region.[37] This herniation frequently complicates decompressive craniectomy performed for traumatic brain injury or other causes of intracranial hypertension, with reported incidences reaching up to 25% in affected surgical cohorts; it may also arise from traumatic skull fractures.[37] Brain edema typically peaks within the first week post-procedure, heightening the risk of this extrusion.

Upward Herniation

Upward herniation, also known as ascending or upward transtentorial herniation, involves the upward displacement of cerebellar structures, such as the vermis and tonsils, through the tentorial incisura due to mass effects from infratentorial lesions. This process typically arises from expanding lesions in the posterior fossa that increase intracranial pressure below the tentorium cerebelli, forcing the cerebellum and adjacent brainstem upward against the tentorial edge. Common causes include posterior fossa hemorrhages, tumors, or abscesses, which compress the brainstem and distort the normal anatomy of the infratentorial compartment.[7][3][1] The mechanism begins with the infratentorial mass effect kinking the brainstem and causing patchy ischemia, while the upward push leads to compression of the dorsal midbrain and aqueduct of Sylvius. This can result in obstructive hydrocephalus from aqueductal narrowing, further exacerbating the pressure gradient. As the herniation progresses, the cerebellar vermis herniates superiorly, shearing neurovascular structures against the tentorium and clivus, which can lead to rapid neurological deterioration.[7][3][38] Clinically, upward herniation presents with characteristic signs stemming from early compression of the tectal plate and later brainstem involvement. In the early stage, tectal compression manifests as Parinaud's syndrome, featuring vertical gaze palsy (particularly upward), light-near dissociation of the pupils (with midposition, poorly reactive pupils), convergence-retraction nystagmus, and lid retraction. Neck stiffness may occur due to meningeal irritation from the mass lesion, and small reactive pupils can be observed from midbrain dysfunction. As the condition advances to late brainstem involvement, patients develop loss of consciousness from compression of the ascending arousal system, oculocephalic reflex abnormalities, and potential diabetes insipidus from pituitary stalk damage. Respiratory irregularities and complete loss of brainstem reflexes signal irreversible progression.[7][1][3] Upward herniation is less common than downward transtentorial types, often described as rare in clinical series, and carries a high mortality rate due to its rapid progression and potential for nonsurvivable brainstem injury. Prognosis is favorable if recognized early before midbrain herniation fully compromises vital functions, with potential for reversal through decompression; however, once respiratory compromise occurs, good recovery is seen in fewer than 5% of cases.[7][38][3]

Tonsillar Herniation

Tonsillar herniation, also known as downward cerebellar herniation, occurs when the cerebellar tonsils displace inferiorly through the foramen magnum, compressing the medulla oblongata against the clivus or odontoid process.[39] This displacement, often termed "coning," is typically triggered by infratentorial swelling or mass effect within the posterior fossa, which forces the cerebellar structures caudally.[39] The resulting compression disrupts vital brainstem functions, particularly those governing respiration and cardiovascular regulation, potentially leading to rapid respiratory arrest.[39] Clinical signs of tonsillar herniation include nuchal rigidity due to meningeal irritation, apnea from medullary compression, and bradycardia as part of Cushing's triad, which also encompasses hypertension and irregular respirations.[39] The condition progresses swiftly to cardiorespiratory failure if untreated, with patients often exhibiting altered consciousness, flaccid quadriplegia, and loss of brainstem reflexes.[39] Common associations include exacerbations of Chiari malformation type I, where congenital tonsillar ectopia worsens under increased intracranial pressure, and large tumors in the posterior fossa, such as medulloblastomas or ependymomas, that generate significant mass effect.[39] Other precipitating factors encompass infratentorial hemorrhages, abscesses, or hydrocephalus obstructing cerebrospinal fluid flow.[39] Prognosis is generally poor once respiratory centers are compromised, with the process often proving irreversible due to profound brainstem ischemia and edema; mortality rates approach 80% in severe cases, particularly those linked to trauma.[40] Early recognition and intervention are critical to mitigate these outcomes, though survival frequently involves significant neurological deficits.[39]

Diagnosis

Clinical Evaluation

The clinical evaluation of suspected brain herniation begins with immediate triage using the ABCs protocol—airway, breathing, and circulation—to ensure patient stability in emergency settings, as compromised oxygenation or perfusion can exacerbate intracranial pressure and worsen outcomes.[41] This involves securing a patent airway, particularly in comatose patients at risk of aspiration, assessing respiratory rate and pattern for irregularities, and establishing circulatory access to monitor and support blood pressure, with hyperventilation avoided unless herniation signs are imminent.[1] A detailed history taking follows stabilization, focusing on the rapidity of symptom onset to differentiate acute from subacute processes and inquiring about trauma history versus underlying medical conditions such as tumors, strokes, or infections that may precipitate herniation.[1] For instance, sudden onset after head injury raises suspicion for traumatic causes like epidural hematoma, while gradual progression might suggest mass lesions.[1] Collateral information from witnesses or records is crucial when the patient is unresponsive. Neurological assessment employs standardized tools like the Glasgow Coma Scale (GCS), which scores eye opening, verbal response, and motor response on a scale of 3-15; a score below 8 indicates severe impairment and coma, signaling potential herniation requiring urgent intervention.[24] Pupillary light reflex testing is essential, evaluating pupil size, symmetry, and reactivity to light; fixed, dilated pupils often denote third cranial nerve compression from uncal herniation.[42] Vital signs monitoring identifies Cushing's triad—hypertension, bradycardia, and irregular respirations—as a late indicator of brainstem compression.[14] Motor response evaluation distinguishes decorticate posturing (upper extremity flexion with lower extremity extension, reflecting corticospinal tract disruption above the midbrain) from decerebrate posturing (rigid extension of all extremities, indicating deeper brainstem involvement), both elicited by noxious stimuli and prognostic of herniation severity.[25] These bedside techniques collectively guide suspicion of herniation, prompting rapid escalation to confirmatory measures while avoiding delays in stabilization.[1]

Imaging and Laboratory Findings

Non-contrast computed tomography (CT) serves as the primary imaging modality for the acute detection of brain herniation due to its rapid acquisition and widespread availability in emergency settings. Characteristic findings include a midline shift exceeding 5 mm, which signifies substantial mass effect and herniation risk, often prompting urgent intervention. Effacement of the basal cisterns and sulcal obliteration further indicate elevated intracranial pressure compressing brain structures. In central herniation specifically, caudal displacement of the pineal gland and brainstem may be evident on CT, reflecting downward progression through the tentorial notch. Magnetic resonance imaging (MRI) offers superior soft tissue contrast for detailed evaluation of herniation extent and underlying etiologies, such as tumors or infarcts, though it is typically reserved for non-acute scenarios or when CT is inconclusive. Advanced CT perfusion techniques can identify ischemia resulting from vascular compression during herniation, aiding in prognosis and management decisions. Intracranial pressure (ICP) monitoring via an intraventricular catheter remains the gold standard for direct measurement, with therapeutic goals to maintain ICP below 20 mm Hg to prevent further herniation. Laboratory assessments complement imaging by identifying reversible contributors to herniation. Coagulation studies, including prothrombin time and platelet count, are routinely obtained to evaluate bleeding risks, particularly in trauma-related cases requiring potential neurosurgery. Electrolyte panels screen for hyponatremia, a common precipitant of cerebral edema that exacerbates herniation and necessitates prompt correction to avoid osmotic shifts. Arterial blood gas analysis assesses respiratory compromise and acid-base status, which can deteriorate rapidly in herniation syndromes affecting brainstem function.

Management and Treatment

Initial Stabilization

Initial stabilization in brain herniation prioritizes securing the airway, optimizing cerebral perfusion, and rapidly reducing intracranial pressure (ICP) to prevent further neurological deterioration. Airway management is critical, with endotracheal intubation recommended for patients with a Glasgow Coma Scale (GCS) score of 8 or less to protect against aspiration and facilitate controlled ventilation.[43] During intubation, neuroprotective techniques such as pretreatment with fentanyl and use of agents like etomidate or ketamine minimize ICP spikes.[44] Brief hyperventilation to a partial pressure of arterial carbon dioxide (PaCO2) of 30–35 mmHg serves as a temporizing measure to induce vasoconstriction and lower ICP, but should be limited to less than 2 hours to avoid cerebral ischemia.[43] Patient positioning plays a key role in enhancing venous drainage from the intracranial compartment. Elevating the head of the bed to 30 degrees, while maintaining a neutral neck position to avoid jugular vein compression, promotes cerebral venous outflow and helps reduce ICP without compromising mean arterial pressure.[43] This maneuver is implemented immediately upon recognition of herniation signs, such as Cushing's triad or pupillary changes, and is combined with strict avoidance of hypotension or hypoxia.[44] Osmotherapy is a cornerstone for acutely drawing fluid from edematous brain tissue across the blood-brain barrier. Intravenous mannitol, administered as a 0.5–1 g/kg bolus, is effective for rapid ICP reduction in herniation syndromes, with repeat doses permissible if serum osmolality remains below 320 mOsm/kg.[43] Alternatively, hypertonic saline (e.g., 3% or higher concentrations via central line) targets serum sodium levels up to 155–160 mEq/L, offering similar osmotic effects and potentially fewer renal complications; monitoring of serum sodium every 4–6 hours is essential to prevent overcorrection.[44] Continuous monitoring of ICP and cerebral perfusion pressure (CPP) guides resuscitation efforts, with invasive ICP monitoring (e.g., via intraventricular catheter) recommended when herniation is suspected to maintain CPP above 60 mmHg. Recent guidelines emphasize advanced neuromonitoring, including cerebral oxygenation, as part of tiered ICP management.[43][45] Seizure prophylaxis is routinely initiated with phenytoin (loading dose 15–20 mg/kg IV) in patients at high risk, such as those with traumatic brain injury leading to herniation, to prevent early post-traumatic seizures that could exacerbate ICP. These interventions form the bridge to definitive management, emphasizing a multidisciplinary approach in a neurocritical care setting.[43]

Surgical and Medical Interventions

Surgical interventions for brain herniation focus on rapidly evacuating mass lesions and alleviating intracranial pressure (ICP) to reverse the herniation process. Craniotomy is a standard procedure for removing space-occupying hematomas, such as epidural or subdural collections, that precipitate herniation by causing midline shift and compression; this approach allows direct access to the lesion while preserving bone integrity for later replacement.[46] In cases of refractory ICP where medical management fails, decompressive craniectomy is performed by excising a large bone flap (typically 12-15 cm in diameter) and opening the dura to permit brain expansion, thereby reducing the risk of further herniation and brainstem compression.[47] Type-specific surgical strategies are tailored to the herniation subtype to address localized compression. For tonsillar herniation, often resulting from posterior fossa masses or swelling, suboccipital decompressive craniectomy relieves cerebellar tonsil impaction at the foramen magnum by expanding the posterior fossa space and preventing respiratory arrest.[48] In uncal herniation due to temporal lobe swelling, aggressive temporal lobectomy—resecting the anterior and inferior temporal lobe—can rapidly decompress the uncus and midbrain, improving outcomes in traumatic cases with significant contusion.[49] Medical therapies complement surgery by targeting ICP reduction through metabolic suppression. High-dose barbiturates, such as pentobarbital, are administered to induce coma, decreasing cerebral metabolic rate and blood flow to control refractory ICP in herniating patients; loading doses of 10-20 mg/kg followed by maintenance infusions aim for serum levels of 30-40 mcg/mL.[50] Corticosteroids, however, are contraindicated in traumatic brain injury-associated herniation, as the CRASH trial demonstrated an 18% relative increase in mortality risk with their use due to complications like hyperglycemia and infection.[51] Multimodal protocols integrate therapies like therapeutic hypothermia for select patients with ongoing herniation despite initial stabilization measures, such as intubation and hyperventilation. Cooling to 32-34°C reduces ICP by lowering cerebral metabolism and edema formation, though the Eurotherm3235 trial showed it effectively controls hypertension but yields unfavorable neurologic outcomes in some traumatic brain injury cases.[52] The DECRA trial (2011) on early decompressive craniectomy in diffuse traumatic brain injury, incorporating hypothermia as a second-tier option, reported lower ICP but higher rates of poor functional outcomes compared to medical management alone, highlighting mixed efficacy in multimodal approaches.[53]

Prognosis and Complications

Short-Term Outcomes

Brain herniation carries a high short-term mortality rate, ranging from 50% to 80% in cases associated with massive hemispheric ischemic infarctions, primarily due to brainstem compression and respiratory failure.[54] For uncal herniation, particularly in traumatic brain injury, reversal is possible in 50% to 75% of cases if rapid intervention occurs before progression to coma.[28] Tonsillar herniation is often terminal, with mortality approaching 100% when brainstem involvement leads to irreversible respiratory arrest, though early surgical decompression can occasionally prevent death.[39] Several factors influence short-term survival, including the time to intervention and initial clinical presentation. A low Glasgow Coma Scale (GCS) score at presentation, specifically 3 to 5, strongly predicts poor outcomes, with survival rates as low as 20% and fewer than half of survivors achieving meaningful recovery.[55] In surviving patients, recovery involves intensive care unit (ICU) monitoring for 48 to 72 hours to assess intracranial pressure stability and neurological status, followed by gradual weaning from mechanical ventilation once brainstem function improves and oxygenation is adequate.[56] This phase focuses on preventing secondary insults like hypoxia, with successful extubation typically attempted after confirming airway protection and adequate respiratory drive. Early complications include a risk of re-herniation due to persistent mass effect or edema, necessitating vigilant monitoring, and nosocomial infections such as ventilator-associated pneumonia, which affect up to 50% of severe brain injury patients in the ICU.[57] These infections contribute to prolonged ventilation and increased short-term mortality if not managed aggressively with antibiotics and infection control measures.

Long-Term Sequelae

Survivors of brain herniation often experience persistent neurological deficits that vary based on the herniation type and affected brain regions. Common impairments include hemiplegia, which affects approximately 30% of survivors due to ischemic damage or compression in motor pathways during the acute phase.[58] Aphasia may occur in cases involving temporal or frontal lobe involvement, leading to language processing difficulties, while ataxia is frequent in cerebellar or brainstem herniations, resulting in coordination and balance issues.[59] These motor and sensory-motor deficits can significantly limit mobility and daily functioning. Cognitive effects are equally prevalent among survivors, encompassing memory impairment and executive dysfunction that persist beyond the initial recovery period. Memory deficits, particularly in working and episodic recall, arise from hippocampal and prefrontal damage associated with herniation syndromes.[60] Executive dysfunction manifests as difficulties in planning, decision-making, and impulse control, affecting up to 50-70% of severe TBI survivors.[61] Additionally, post-traumatic stress disorder (PTSD) develops in 20-40% of cases, exacerbated by the trauma of the event and ongoing neurological challenges, with prevalence rates ranging from 15-36% in low-bias studies of TBI cohorts.[62] Rehabilitation for brain herniation survivors typically involves multidisciplinary approaches, including physical, occupational, and speech therapy tailored to individual deficits. These interventions aim to maximize functional recovery by leveraging neuroplasticity, the brain's capacity to reorganize neural pathways.[63] In pediatric patients, early initiation of rehabilitation capitalizes on heightened neuroplasticity during development, leading to improved outcomes compared to adults; for instance, children with transient transtentorial herniation achieve favorable recovery in 75% of cases through aggressive neurointensive care and therapy.[64] Comprehensive programs often integrate cognitive remediation and adaptive strategies, enhancing quality of life despite residual impairments.[65] In a cohort of supratentorial mass lesion patients with reversed transtentorial herniation, 64% of survivors were independent at follow-up, but broader severe TBI studies show lower long-term independence around 45-59% due to compounded complications.[64][66] Outcomes in brain herniation are generally poorer than in general severe TBI due to the severity of the condition. Ongoing research from the TRACK-TBI study, as of 2025, highlights that while many moderate-to-severe TBI survivors with herniation face lifelong challenges, a subset demonstrates progressive gains in independence over 1-7 years, underscoring the need for extended monitoring.[67]

References

  1. Brain Herniation - StatPearls - NCBI Bookshelf
  2. Brain herniation: MedlinePlus Medical Encyclopedia
  3. Brain Herniation - Neurologic Disorders - Merck Manual Professional Edition
  4. https://pubs.rsna.org/doi/full/10.1148/rg.2019190018
  5. History of the cushing reflex - PubMed
  6. Transtentorial Herniation - StatPearls - NCBI Bookshelf - NIH
  7. James Collier (1870–1935) and uncal herniation - PMC - NIH
  8. Neuroanatomy, Tentorium Cerebelli - StatPearls - NCBI Bookshelf
  9. Intracranial Pressure Monitoring - StatPearls - NCBI Bookshelf - NIH
  10. Increased Intracranial Pressure - StatPearls - NCBI Bookshelf - NIH
  11. Intracranial Compliance Concepts and Assessment: A Scoping ...
  12. Cerebral Perfusion Pressure - StatPearls - NCBI Bookshelf
  13. Cushing Reflex - StatPearls - NCBI Bookshelf - NIH
  14. Traumatic Brain Injury - StatPearls - NCBI Bookshelf
  15. High Intracranial Pressure, Brain Herniation and Death in Cerebral ...
  16. Nontraumatic Intracranial Hemorrhage - NCBI - NIH
  17. Uncommon Causes of Nontraumatic Intracerebral Hemorrhage
  18. Hepatic Encephalopathy - StatPearls - NCBI Bookshelf - NIH
  19. Three important subgroups of hypertensive persons at greater risk of ...
  20. Risk Factors for Cerebral Hemorrhage in the Era of Well-Controlled ...
  21. Glasgow Coma Scale - StatPearls - NCBI Bookshelf
  22. Decerebrate and Decorticate Posturing - StatPearls - NCBI Bookshelf
  23. Emergency Neurological Life Support: Intracranial Hypertension and ...
  24. Relationship between cerebral blood flow and the development of ...
  25. Uncal Herniation - StatPearls - NCBI Bookshelf
  26. Subfalcine Herniation - StatPearls - NCBI Bookshelf - NIH
  27. Brain Herniation - Brain, Spinal Cord, and Nerve Disorders
  28. Incipient Transcalvarial Cerebral Herniation - PubMed
  29. Paradoxical brain herniation following decompressive craniectomy
  30. [PDF] Vol. 1 No. 1 (2022) : LHSJ Oktober 2022 (26-41) SYSTEMATIC ...
  31. https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4791176/
  32. Anterior Fontanelle Herniation | American Academy of Pediatrics
  33. Anterior fontanel herniation in group B streptococcus meningitis in ...
  34. Complications of Decompressive Craniectomy - Frontiers
  35. Upward transtentorial herniation - PMC - NIH
  36. Tonsillar Herniation - StatPearls - NCBI Bookshelf - NIH
  37. Head trauma in China - PubMed
  38. [PDF] Intracranial Hypertension and Herniation Protocol Version 4.0
  39. Pupillary Light Reflex - StatPearls - NCBI Bookshelf - NIH
  40. https://doi.org/10.1007/s12028-012-9754-5
  41. https://doi.org/10.1177/08850666231156589
  42. Craniotomy or Decompressive Craniectomy for Acute Subdural ...
  43. Decompressive Craniectomy in Severe Traumatic Brain Injury - NIH
  44. Outcomes following Suboccipital Decompressive Craniectomy for ...
  45. Aggressive Temporal Lobectomy for Uncal Herniation in Traumatic ...
  46. Barbiturates for the treatment of intracranial hypertension after ...
  47. Hypothermia for Intracranial Hypertension after Traumatic Brain Injury
  48. Decompressive Craniectomy in Diffuse Traumatic Brain Injury
  49. Predictors of Fatal Brain Edema in Massive Hemispheric Ischemic ...
  50. https://www.tandfonline.com/doi/full/10.1080/01616412.2025.2515523
  51. Prognostication in Severe Traumatic Brain Injury in Adults
  52. Management and weaning from mechanical ventilation in ...
  53. Nosocomial infections and immunity: lesson from brain-injured ...
  54. Transcranial direct current stimulation for the treatment of motor ...
  55. Ataxia Caused by Traumatic Brain Injury (TBI)
  56. Reorganization of Sensory and Motor Systems in Hemiplegic Stroke ...
  57. Cognitive Impairment Following Traumatic Brain Injury - PubMed
  58. Cognitive Sequelae of Traumatic Brain Injury - PMC - NIH
  59. Post-Traumatic Stress Disorder after Civilian Traumatic Brain Injury
  60. Adaptive Neuroplasticity in Brain Injury Recovery - PubMed Central
  61. Long-time outcome after transient transtentorial herniation ... - PubMed
  62. Review Article Rehabilitation for Children After Acquired Brain Injury
  63. Long-term outcome after medical reversal of transtentorial herniation ...
  64. Functional Outcomes Over the First Year After Moderate to Severe ...
User Avatar
No comments yet.