Traumatic Brain Injury

Traumatic Brain Injury (TBI)

Definition

Traumatic Brain Injury (TBI) is an alteration in brain function or evidence of brain pathology caused by an external mechanical force, leading to temporary or permanent neurological impairment.

Alteration in brain function includes: loss of consciousness, amnesia, confusion, focal neurological deficit, or change in mental state.

Epidemiology & Importance

Major cause of death and disability worldwide
Common in young adults (road traffic accidents) and elderly (falls)
Significant ICU burden → prolonged ventilation, raised ICP, secondary brain injury

Pathophysiology of TBI

A. Primary Brain Injury (At the moment of impact)

Occurs immediately and is non-reversible

Mechanisms

Direct impact (coup–contrecoup)
Acceleration–deceleration
Rotational forces

Types

Cerebral contusion
Laceration
Diffuse axonal injury (DAI)
Skull fractures
Intracranial hematomas

B. Secondary Brain Injury (Minutes → days)

Potentially preventable & treatable

Mechanisms

Hypoxia
Hypotension
Hypercapnia / hypocapnia
Raised ICP → ↓ CPP
Excitotoxicity (↑ glutamate)
Mitochondrial dysfunction
Neuroinflammation
Cerebral edema
Seizures(increased metabolism)
Hyperglycemia / hypoglycemia
Pyrexia

# Key principle in ICU: Prevent secondary brain injury

Classification of TBI

A. By Severity (Glasgow Coma Scale)

Severity	GCS Score
Mild	13–15
Moderate	9–12
Severe	≤8

B. By Morphology (Imaging Based)

Extra-axial Lesions

Epidural hematoma (EDH)
Subdural hematoma (SDH)
Subarachnoid hemorrhage (tSAH)

Intra-axial Lesions

Cerebral contusion
Intracerebral hemorrhage
Diffuse axonal injury

Initial Assessment — ATLS Approach

1.Primary Survey (ABCDE)

2. Neuroimaging in TBI

Non-contrast CT Head

First-line investigation
Rapid, available
Detects fractures, bleeds, mass effect

MRI Brain

DAI
Brainstem injury
Prognostication (later)

Raised Intracranial Pressure (ICP)

Normal ICP

Adults: 7–15 mmHg in horizontal position
An ICP value >20 mmHg is considered abnormal, while levels exceeding 25 mmHg warrant urgent and aggressive intervention, as they are associated with a high risk of secondary brain injury.
The gold standard technique for ICP monitoring is the use of an external ventricular drain (EVD)-diagnostic and therapeutic . This device is inserted into the ventricular system, typically at the level of the foramen of Monro.

Raised ICP Pathophysiology

Brain edema
Hematoma
Impaired CSF drainage
Acute hypoxemia (for example, due to a respiratory infection) leads to cerebral vasodilation, which increases cerebral blood flow (CBF).
Impaired venous drainage can also occur due to intracranial causes, such as injury to the venous sinuses
External compression of the neck (e.g., tight cervical collars) can obstruct jugular venous outflow
Positive pressure ventilation raises intrathoracic pressure, reducing cerebral venous return
Elevated intra-abdominal pressure (seen in conditions like constipation or even during patient transport when heavy objects rest on the abdomen) can indirectly increase venous pressure and ICP

Monroe–Kellie Doctrine

Total intracranial volume =Brain + Blood + CSF (constant)

Cerebral Perfusion Pressure (CPP)

CPP = MAP − ICP

Parameter	Target
ICP	< 22 mmHg
CPP	50–70 mmHg

#Hypotension (SBP < 100–110 mmHg) is strongest predictor of mortality

In patients with traumatic brain injury (TBI), positioning and pressure referencing are crucial for accurate hemodynamic assessment.

Most TBI patients are nursed with the head elevated to 30°, Because of the vertical height difference between the heart and the head in a 30° head-up position, there can be a pressure gradient of ~10–11 mmHg. As a result, referencing MAP at the right atrium will overestimate cerebral perfusion pressure (CPP).

Therefore, both:

ICP transducer, and
Arterial pressure transducer (MAP)

must be zeroed at the level of the external auditory meatus (tragus)—which approximates the level of the brain.

ICU Management of Severe TBI

A. Airway & Ventilation

Indications for intubation

GCS ≤ 8
Airway compromise

Target:(From Taable of Text Book Of Critical care)

Parameter	Target Value
Pulse oximetry (SpO₂)	≥ 95%
PaO₂	≥ 100 mmHg
PaCO₂	35–45 mmHg
pH	7.35–7.45
SBP	≥ 100 mmHg
ICP	20–25 mmHg (upper limit)
CPP	≥ 60 mmHg
PbtO₂	≥ 15 mmHg
Temperature	36–38°C
Serum Sodium	135–145 mEq/L
INR	≤ 1.4
Platelets	≥ 75,000/mm³
Hemoglobin	≥ 7 g/dL
Glucose	80–180 mg/dL

Blood Pressure (SBP targets – age specific)

Age	SBP Target (BTF)
18–49 yrs	≥ 110 mmHg
50–69 yrs	≥ 100 mmHg
≥ 70 yrs	≥ 110 mmHg

👉 Prevent even a single episode of hypotension

B. Hemodynamic Management

Avoid hypotension
Maintain MAP to achieve CPP ≥ 60
Balanced crystalloids preferred

C. ICP Control — Tier Wise(Different in different guidelines)

First-tier

Head elevation 30°
Neutral neck-Loosen collar – improve venous drainage
Analgesia + sedation
Normoxia, normocapnia
Normoglycemia
Treat fever
CSF drainage (EVD)

Traditionally, the use of lumbar CSF drainage in patients with raised intracranial pressure was avoided due to concern for brain herniation (“coning”). The rationale was that removing cerebrospinal fluid from the spinal compartment could create a pressure gradient between the cranial and spinal compartments, potentially precipitating downward displacement of brain structures.

However, more recent experience suggests that this risk may have been overestimated, particularly in carefully selected patients. As a result, lumbar drains are increasingly being utilized in some centers as an adjunct for managing refractory intracranial hypertension, especially when conventional therapies have failed.

Second-tier

Osmotherapy

Mannitol (0.25–2 g/kg)-mannitol can precipitate out in the cold,higher incidence of renalcomplications
Hypertonic saline(3% 3–5 mL/kg)

Hyperventilation

Hyperventilation belongs to the SECOND-TIER therapy for raised intracranial pressure (ICP) in severe traumatic brain injury.

Why SECOND-TIER?

Hyperventilation causes ↓ PaCO₂
Leads to cerebral vasoconstriction
Results in ↓ cerebral blood volume → ↓ ICP

# Effect is rapid but temporary
# Causes reduced cerebral blood flow → risk of ischemia

Hence, it is NOT first-line.

Current Guideline Position

Avoid prophylactic hyperventilation
Target PaCO₂: 35–40 mmHg (normal ventilation)
Short-term hyperventilation (PaCO₂ 30–35 mmHg):

Only for acute neurological deterioration(e.g. a blown pupil) to buy a few extra minutes
As a bridge to definitive therapy (surgery / osmotherapy)

—> Never maintain PaCO₂ < 30 mmHg

Third-tier

Barbiturate coma
Decompressive craniectomy
Targeted hypothermia (NO BENEFIT -Eurotherm study)

Decompressive Craniectomy in TBI (Refractory Intracranial Hypertension)

1. DECRA trial

Population: Diffuse TBI
Intervention trigger: ICP >20 mmHg for >15 minutes despite initial therapy
Comparison: Standard care (including barbiturates) vs early DC

Findings:

DC effectively reduced ICP
However, it resulted in worse functional neurological outcomes

Critical interpretation:

The ICP threshold (20 mmHg) and short duration (15 min) were likely too low, leading to premature surgery

2. RESCUEicp trial

Population: Severe TBI with refractory ICP
Intervention trigger: ICP >25 mmHg for 1–12 hours
Comparison: Medical therapy vs DC

Findings:

Mortality reduction: ~22 additional survivors per 100 patients in the surgical group
BUT → Many survivors had severe disability / poor quality of life

Key dilemma:

Survival vs neurological outcome
Raises ethical concerns regarding acceptable outcomes and patient selection

Coagolopathy

Traumatic brain injury (TBI) can also trigger trauma-induced coagulopathy (TIC). As a result, patients may develop a spectrum ranging from hypercoagulability (early) to hypocoagulability and bleeding tendency (later)

Use Point-of-care viscoelastic tests which helps Early detection of coagulopathy → prevents hematoma expansion.

Tranexamic acid (TXA)—-CRASH-3 trial,

1. Mortality Benefit (Time-Dependent)

Reduced head injury–related death, especially in:

Mild to moderate TBI (GCS 9–15)

No significant benefit in:

Very severe TBI (GCS 3–8)

Earlier administration = better outcomes

2. Timing is Critical

Benefit seen only if TXA given within 3 hours
No benefit (may be harmful) if given late (>3 hours)

Dose

Loading dose: 1 g IV over 10 minutes
Maintenance: 1 g IV infusion over 8 hours

Antiplatelet

patients who are already on antiplatelet therapy (e.g., aspirin, clopidogrel), routine platelet transfusion is not recommended For procedures such as craniotomy or decompressive surgery A target platelet count >100 × 10⁹/L .

Patients on Direct Oral Anticoagulants (DOACs) in TBI

Dabigatran
→ Reversed by Idarucizumab
Rivaroxaban (also apixaban, edoxaban)
→ Reversed by Andexanet alfa

Because of limited access to specific reversal agents, many centers rely on:

Prothrombin Complex Concentrate (PCC)
Fresh Frozen Plasma (FFP)
→ Less effective than PCC but still used where PCC is unavailable

Deep Vein Thrombosis Prophylaxis

Initial Strategy: Mechanical Prophylaxis First

Start mechanical prophylaxis early in all patients unless contraindicated:

Intermittent pneumatic compression (IPC) devices
Compression stockings

These reduce venous stasis without increasing bleeding risk

Pharmacological Prophylaxis (Anticoagulation)

Major concern: hematoma expansion in brain
Therefore, anticoagulation is delayed and individualized

Current Practical Approach (Guideline-Oriented Insight)

Can be considered if repeat neuroimaging shows stable hemorrhage
By 48–72 hours:initiate low molecular weight heparin (LMWH)

Role of IVC Filter

Consider in:

Very high VTE risk
Contraindication to anticoagulation
Prolonged immobilization

Inferior vena cava filter prevents pulmonary embolism by trapping emboli from lower limbs

Albumin vs Saline

Use of albumin for resuscitation in TBI has been shown to be harmful
It is associated with increased mortality compared to normal saline

This finding is largely derived from the SAFE trial (TBI subgroup analysis)

Mechanism

Albumin is relatively hypotonic
Can increase cerebral edema
Leads to worsening ICP and poorer outcomes

Normal Saline vs Balanced Crystalloids

Normal saline (0.9% NaCl) remains the standard fluid in TBI
Despite theoretical benefits of balanced crystalloids (e.g., less hyperchloremia):

No strong evidence shows superiority of balanced solutions over saline in TBI

sedatives (midazolam/propofol)

First-line: Propofol infusion (if MAP stable)
Avoid hypotension at all costs → may switch to midazolam
Combine with analgesia (opioids like fentanyl)
Aim for targeted sedation (not over-sedation)
Consider escalation (e.g., barbiturates) in refractory ICP

Early vs Late Tracheostomy

Early Tracheostomy (≈ ≤7 days)

Potential Benefits:

May reduce duration of mechanical ventilation
Associated with shorter ICU length of stay
Improved patient comfort and reduced sedation needs

Potential Downsides:

Risk of performing the procedure in patients who may have recovered quickly
Some evidence suggests delay in transfer to rehabilitation, possibly due to ongoing ICU-level care decisions

Decision = case-by-case, multidisciplinary

Seizure Prophylaxis

Early post-traumatic seizures (≤7 days)
Levetiracetam or Phenytoin
Prophylaxis for 7 days only

Feature	Levetiracetam (Levipil)	Phenytoin
Mechanism	Binds SV2A (synaptic vesicle protein) → ↓ neurotransmitter release	Blocks voltage-gated Na⁺ channels → stabilizes neuronal membrane
Role in TBI	Increasingly preferred (guidelines allow either)	Traditional standard drug for early PTS prophylaxis
Efficacy (Early PTS)	Similar to phenytoin (no superiority)	Proven benefit for early seizures (<7 days)
Late PTS prevention	Not effective	Not effective
Dosing (Loading)	1–3 g IV (commonly 1–2 g)	15–20 mg/kg IV-Slow infusion (≤50 mg/min)
Maintenance dose	500–1500 mg BD	4–6 mg/kg/day (divided)
Therapeutic drug monitoring	Not required	Required (target 10–20 µg/mL)
Drug interactions	Minimal	Extensive (CYP450 inducer)
Hepatic metabolism	Minimal	Extensive hepatic metabolism
Renal adjustment	Required	Usually not needed
Adverse effects (common)	Sedation, dizziness	Nystagmus, ataxia, diplopia
Serious adverse effects	Behavioral changes (agitation)	SJS/TEN, DRESS, hepatotoxicity
IV-related complications	Rare	Hypotension, arrhythmias (esp. rapid infusion)
Pregnancy	Relatively safer	Teratogenic (fetal hydantoin syndrome)
Guideline preference	Increasingly favored in ICU practice	Still acceptable first-line

# Temperature & Glycemic Control

Avoid fever (↑ CMRO₂)
Target glucose: 140–180 mg/dL
Tight control → hypoglycemia risk

# Nutrition

Early enteral feeding (within 24–48 h)
High-protein, hypercaloric
Prevent catabolism

# Complications of TBI

Raised ICP
Herniation syndromes
Neurogenic pulmonary edema
SIADH / Cerebral salt wasting
ARDS
Sepsis
Long-term cognitive & behavioral deficits

Prognostication in Traumatic Brain Injury (TBI)

— CLINICAL PROGNOSTIC FACTORS (MOST IMPORTANT)

A. Glasgow Coma Scale (GCS)

Strongest early predictor

GCS	Prognosis
13–15	Mild, good outcome
9–12	Moderate
≤8	Severe, high mortality

Limitations:

Sedation, paralysis, intoxication confound

B. Pupillary Reactivity

Pupils	Prognosis
Both reactive	Better outcome
One fixed	Intermediate
Bilateral fixed dilated	Very poor prognosis

Bilateral non-reactive pupils → suggests:

Brainstem dysfunction
Raised ICP / herniation

C. Age

Age	Outcome
<40 yrs	Better
>60 yrs	Worse

Mechanism:

Reduced neuroplasticity
More comorbidities

D. Hypotension & Hypoxia (SECONDARY INSULTS)

SBP <90 mmHg → doubles mortality
Hypoxia (PaO₂ <60 mmHg) → major predictor of poor outcome

Preventing secondary injury = strongest modifiable prognostic factor

E. Motor Response (GCS Motor Score)

Best component of GCS
Extensor/no response → poor outcome

— CT-BASED PROGNOSTICATION

Marshall CT Classification

Category	Features	Prognosis
Diffuse I	Normal CT	Good
Diffuse II	Cisterns present	Moderate
Diffuse III	Cisterns compressed	Poor
Diffuse IV	Midline shift >5 mm	Worse
Evacuated mass	Variable
Non-evacuated mass	Very poor

Rotterdam CT Score (More Accurate)

Components:

Basal cisterns
Midline shift
Epidural lesion
IVH/SAH

Score	Mortality
1	~0%
6	~60–80%

Higher score = worse prognosis

4. INTRACRANIAL PRESSURE (ICP) & PHYSIOLOGY

Sustained ICP >22 mmHg → poor outcome
CPP <60 mmHg → cerebral ischemia → poor outcome

Pressure Reactivity Index (PRx)

Reflects autoregulation

PRx	Interpretation
Negative	Intact autoregulation
Positive (>0.25)	Impaired → poor prognosis

Brain Tissue Oxygen (PbtO₂) <20 mmHg → worse outcomes

5. MRI FINDINGS

Key Predictors:

Diffuse Axonal Injury (DAI):

Grade III (brainstem) → very poor prognosis

Brainstem lesions → worst outcomes
Corpus callosum involvement → severe injury

6. BIOMARKERS

Biomarker	Source	Significance
S100B	Astrocytes	Injury severity
NSE	Neurons	Poor outcome
GFAP	Glial cells	Highly specific
UCH-L1	Neurons	FDA-approved (mild TBI)

Not standalone tools yet (guidelines: adjunct only)

7. ELECTROPHYSIOLOGY

EEG

Non-reactive EEG → poor prognosis
Status epilepticus → worse outcomes

Somatosensory Evoked Potentials (SSEP)

Bilateral absent N20 → poor prognosis

8. PROGNOSTIC MODELS

IMPACT Model

(International Mission for Prognosis and Analysis of Clinical Trials)

Variables:

Age
GCS motor
Pupils
CT findings
Hypoxia, hypotension

CRASH Model

(Corticosteroid Randomisation After Significant Head Injury)

Predicts:

14-day mortality
6-month outcome

Widely used in research & clinical estimation

9. OUTCOME SCALES

Glasgow Outcome Scale (GOS)

Score	Outcome
1	Death
2	Vegetative
3	Severe disability
4	Moderate disability
5	Good recovery

Extended GOS (GOSE)

More granular (8 categories)

10. TIMING OF PROGNOSTICATION

Time	Reliability
<24 hrs	Poor
24–72 hrs	Moderate
>72 hrs	More reliable

Always:

Correct confounders (sedation, hypothermia)
Avoid early withdrawal decisions

REFFERENCE-OHS MANUAL, text book of critical care