Pituitary apoplexy differential diagnosis: Difference between revisions

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Revision as of 16:29, 1 August 2017

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Akshun Kalia M.B.B.S.[2]

Overview

Pituitary apoplexy must be differentiated from other diseases that cause severe headache such as subarachnoid hemorrhage, meningitis, intracranial mass, cerebral hemorrhage, cerebral infarction, intracranial venous thrombosis, migraine, head injury, lymphocytic hypophysitis and radiation injury.

Differentiating Pituitary apoplexy From Other Diseases

Pituitary apoplexy should be differentiated from other diseases causing severe headache for example: ^[1]^[2]^[3]^[4]^[5]^[6]^[7]^[8]^[9]^[10]

	Symptoms			Gold Standard	CT/MRI	Other Investigation Findings
Disease	Symptoms			Diagnosis
	Headache		Other features
	Onset	Characterstics	Other features
Subarachnoid hemorrhage	Sudden	Severe headache Thunderclap Described as the worst headache of life	Double vision Nausea and vomiting Symptoms of meningeal irritation Sudden decreased level of consciousness	Digital subtraction angiography	The modality of choice for diagnosis of subarachnoid hemorrhage is noncontrast head computed tomography (CT), with or without lumbar puncture.^[1] CT shows hyperattenuating material filling the subarachnoid space.	Lumbar puncture (LP) is necessary when there is a strong suspicion of subarachnoid hemorrhage. LP will show: Elevated opening pressure Elevated red blood cell (RBC) Xanthochromia
Meningitis	Sudden	Headache is associated with: fever neck stiffness	Photophobia Phonophobia Irritability altered mental status	Lumbar puncture for CSF	CT scan of the head may be performed before LP to determine the risk of herniation.	Diagnosis is based on clinical presentation in combination with CSF analysis. CSF analysis is the investigation of choice. For more information on CSF analysis in meningitis please click here.
Intracranial mass	Gradual	Headache usually comes in the morning	Nausea Vomiting Change in mental status Seizures focal neurological deficits	MRI	CT or MRI is the initial test to detect intracranial lesions. These imaging tests determine the location of intracranial mass lesion(s) and help in guiding therapy.	Biopsy of the lesion is needed to identify the nature of the lesion such as: Tumor Abscess X- ray of the skull is a non specific test, but useful if any of the lesions are calcified.
Cerebral hemorrhage	Sudden	Rapidly progressing headache	Symptoms of increased intracranial pressure (ICP) Focal neurological deficits	CT without contrast (differentiate ischemic stroke from hemorrhagic stroke.)	CT is very sensitive for identifying acute hemorrhage which appears as hyperattenuating clot. Gradient echo and T2 susceptibility-weighted MRI are as sensitive as CT for detection of acute hemorrhage and are more sensitive for identification of prior hemorrhage.	PT/ INR and aPTT should be checked to rule out coagulopathy.
Intracranial venous thrombosis	Gradual	Diffuse headache Headache can be the only symptom of cerebral venous thrombosis	Focal neurological dfeficits Seizures Depressed level of consciousness	Digital subtraction angiography	The classic finding of sinus thrombosis on unenhanced CT images is a hyperattenuating thrombus in the occluded sinus. CT and MRI may identify Cerebral edema and venous infarction may be apparent.	CT venography detects the thrombus, computed tomography with radiocontrast in the venous phase (CT venography or CTV) has a detection rate that in some regards exceeds that of MRI. Cerebral angiography may demonstrate smaller clots, and obstructed veins may give the "corkscrew appearance".
Migraine	Sudden	Severe to moderate headache One-sided Pulsating Lasts between several hours to three days.	nausea and vomiting Preceding aura photophobia phonophobia	---	CT and MRI may be needed to rule out other suspected possible causes of headache.	Migraine is a clinical diagnosis that does not require any laboratory tests. Laboratory tests can be ordered to rule out any suspected coexistent metabolic problems or to determine the baseline status of the patient before initiation of migraine therapy.
Head injury	Sudden	Headache: Dull Throbbing can be on one side or all around the forehead	Confusion Drowsiness Personality change Seizures Nausea and vomiting Loss of consciousness lucid interval	CT scan without contrast	CT scan is the first test performed and identifies cerebral hemorrhage (appears as hyperattenuating clot) following head injury. CT scan is also less time consuming. MRI is more sensitive, takes more time and is done in patients with symptoms unexplained by CT scan.	The Glasgow Coma Scale is a tool for measuring degree of unconsciousness and is thus a useful tool for determining severity of injury. The Pediatric Glasgow Coma Scale is used in young children.
Lymphocytic hypophysitis		Headache: Generalized Retro-orbital or Bitemporal	Lymphocytic hypophysitis is most often seen in late pregnancy or the postpartum period with the following symptoms: Mass lesion effect such as headache or visual field defects Hypopituitarism	Pituitary biopsy	CT & MRI typically reveal features of a pituitary mass.	The most accurate test is pituitary biopsy which will show lymphocytic infiltration.
Radiation injury		Headache develops gradually	Impairment of mental function is the most prominent feature such as personality change, impairment of memory, confusion, learning difficulties Focal neurological abnormalities and evidence of raised intracranial pressure	Surgical exploration including biopsy (histological confirmation)	CT & MRI will show: Focal radiation necrosis Diffuse white matter injury Contrast-enhancing mass surrounded by edema and mass effect	PET scan Radiation necrosis is hypo metabolic and will have decreased uptake of fluorodeoxyglucose.

References

↑ Endrit Ziu & Fassil Mesfin (2017). "Subarachnoid Hemorrhage". PMID 28722987.
↑ Benedikt Schwermer, Daniel Eschle & Constantine Bloch-Infanger (2017). "[Fever and Headache after a Vacation in Thailand]". Deutsche medizinische Wochenschrift (1946). 142 (14): 1063–1066. doi:10.1055/s-0043-106282. PMID 28728201.
↑ Otto Rapalino & Mark E. Mullins (2017). "Intracranial Infectious and Inflammatory Diseases Presenting as Neurosurgical Pathologies". Neurosurgery. doi:10.1093/neuros/nyx201. PMID 28575459.
↑ I. B. Komarova, V. P. Zykov, L. V. Ushakova, E. K. Nazarova, E. B. Novikova, O. V. Shuleshko & M. G. Samigulina (2017). "[Clinical and neuroimaging signs of cardioembolic stroke laboratory in children]". Zhurnal nevrologii i psikhiatrii imeni S.S. Korsakova. 117 (3. Vyp. 2): 11–19. doi:10.17116/jnevro20171173211-19. PMID 28665364.
↑ Sanjay Konakondla, Clemens M. Schirmer, Fengwu Li, Xiaogun Geng & Yuchuan Ding (2017). "New Developments in the Pathophysiology, Workup, and Diagnosis of Dural Venous Sinus Thrombosis (DVST) and a Systematic Review of Endovascular Treatments". Aging and disease. 8 (2): 136–148. doi:10.14336/AD.2016.0915. PMID 28400981.
↑ Priyanka Yadav, Alec L. Bradley & Jonathan H. Smith (2017). "Recognition of Chronic Migraine by Medicine Trainees: A Cross-Sectional Survey". Headache. doi:10.1111/head.13133. PMID 28653369.
↑ S. Wulffeld, L. S. Rasmussen, B. Hojlund Bech & J. Steinmetz (2017). "The effect of CT scanners in the trauma room - an observational study". Acta anaesthesiologica Scandinavica. 61 (7): 832–840. doi:10.1111/aas.12927. PMID 28635146.
↑ Johnston PC, Chew LS, Hamrahian AH, Kennedy L (2015). "Lymphocytic infundibulo-neurohypophysitis: a clinical overview". Endocrine. 50 (3): 531–6. doi:10.1007/s12020-015-0707-6. PMID 26219407.
↑ Makale MT, McDonald CR, Hattangadi-Gluth JA, Kesari S (2017). "Mechanisms of radiotherapy-associated cognitive disability in patients with brain tumours". Nat Rev Neurol. 13 (1): 52–64. doi:10.1038/nrneurol.2016.185. PMID 27982041.
↑ Sato N, Sze G, Endo K (1998). "Hypophysitis: endocrinologic and dynamic MR findings". AJNR Am J Neuroradiol. 19 (3): 439–44. PMID 9541295.

Template:WH Template:WS

[1] Endrit Ziu & Fassil Mesfin (2017). "Subarachnoid Hemorrhage". PMID 28722987.

[2] Benedikt Schwermer, Daniel Eschle & Constantine Bloch-Infanger (2017). "[Fever and Headache after a Vacation in Thailand]". Deutsche medizinische Wochenschrift (1946). 142 (14): 1063–1066. doi:10.1055/s-0043-106282. PMID 28728201.

[3] Otto Rapalino & Mark E. Mullins (2017). "Intracranial Infectious and Inflammatory Diseases Presenting as Neurosurgical Pathologies". Neurosurgery. doi:10.1093/neuros/nyx201. PMID 28575459.

[4] I. B. Komarova, V. P. Zykov, L. V. Ushakova, E. K. Nazarova, E. B. Novikova, O. V. Shuleshko & M. G. Samigulina (2017). "[Clinical and neuroimaging signs of cardioembolic stroke laboratory in children]". Zhurnal nevrologii i psikhiatrii imeni S.S. Korsakova. 117 (3. Vyp. 2): 11–19. doi:10.17116/jnevro20171173211-19. PMID 28665364.

[5] Sanjay Konakondla, Clemens M. Schirmer, Fengwu Li, Xiaogun Geng & Yuchuan Ding (2017). "New Developments in the Pathophysiology, Workup, and Diagnosis of Dural Venous Sinus Thrombosis (DVST) and a Systematic Review of Endovascular Treatments". Aging and disease. 8 (2): 136–148. doi:10.14336/AD.2016.0915. PMID 28400981.

[6] Priyanka Yadav, Alec L. Bradley & Jonathan H. Smith (2017). "Recognition of Chronic Migraine by Medicine Trainees: A Cross-Sectional Survey". Headache. doi:10.1111/head.13133. PMID 28653369.

[7] S. Wulffeld, L. S. Rasmussen, B. Hojlund Bech & J. Steinmetz (2017). "The effect of CT scanners in the trauma room - an observational study". Acta anaesthesiologica Scandinavica. 61 (7): 832–840. doi:10.1111/aas.12927. PMID 28635146.

[8] Johnston PC, Chew LS, Hamrahian AH, Kennedy L (2015). "Lymphocytic infundibulo-neurohypophysitis: a clinical overview". Endocrine. 50 (3): 531–6. doi:10.1007/s12020-015-0707-6. PMID 26219407.

[9] Makale MT, McDonald CR, Hattangadi-Gluth JA, Kesari S (2017). "Mechanisms of radiotherapy-associated cognitive disability in patients with brain tumours". Nat Rev Neurol. 13 (1): 52–64. doi:10.1038/nrneurol.2016.185. PMID 27982041.

[pmid9541295-10] Sato N, Sze G, Endo K (1998). "Hypophysitis: endocrinologic and dynamic MR findings". AJNR Am J Neuroradiol. 19 (3): 439–44. PMID 9541295.

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@@ Line 68: / Line 68: @@
 {| class="wikitable"
-! rowspan="3" |Disease
+! rowspan="4" |Disease
-! colspan="2" rowspan="2" |Symptoms
+| colspan="3" rowspan="2" |'''Symptoms'''
 ! colspan="3" |Diagnosis
 |-
-! rowspan="2" |Gold Standard
+! rowspan="3" |Gold Standard
-! rowspan="2" |CT/MRI
+! rowspan="3" |CT/MRI
-! rowspan="2" |Other Investigation Findings
+! rowspan="3" |Other Investigation Findings
 |-
-!Headache
+| colspan="2" |'''Headache'''
-!Other features
+! rowspan="2" |Other features
+|-
+!Onset
+!Characterstics
 |-
 |[[Subarachnoid hemorrhage]]
+|Sudden
 |
-* [[Headache|Severe headache]]<nowiki/>as the worst headache of life
+* [[Headache|Severe headache]]
-* Headache starts suddenly and after a popping or snapping feeling in the head
+* <nowiki/>[[Thunderclap headache|Thunderclap]]
+* Described as the worst headache of life
 |
 * [[Double vision]]
@@ Line 88: / Line 93: @@
 * Symptoms of [[meningeal irritation]]
 * Sudden [[Loss of consciousness|decreased level of consciousness]]
-* Rapid progression of symptoms
 |[[Digital subtraction angiography]]
 |
@@ Line 100: / Line 104: @@
 |-
 |[[Meningitis]]
-|[[Headache]] with [[fever]] and [[neck stiffness]]
+|Sudden
+|[[Headache]] is associated with:
+* [[fever]]
+* [[neck stiffness]]
 |
-* [[Photophobia]] (inability to tolerate bright light)
+* [[Photophobia]]
-* [[Phonophobia]] (inability to tolerate loud noises)
+* [[Phonophobia]]
-* [[Irritability]], [[altered mental status]] (in small children)
+* [[Irritability]]
+* [[altered mental status]]
 |[[Lumbar puncture]] for [[CSF]]
 |
@@ Line 114: / Line 123: @@
 |-
 |[[Intracranial mass]]
-|[[Headache]] with focal neurological deficits
+|Gradual
+|[[Headache]] usually comes in the morning
 |
 * [[Nausea]]
@@ Line 120: / Line 130: @@
 * [[Change in mental status]]
 * [[Seizures]]
-* Can be associated comorbid conditions like [[tuberculosis]], etc
+* focal neurological deficits
 |[[MRI]]
 |
@@ Line 133: / Line 143: @@
 |-
 |[[Cerebral hemorrhage]]
-|Rapidly worsening headache with focal neurological deficits
+|Sudden
+|Rapidly progressing headache
 |
-* [[Headache]], vomiting, and depressed level of [[consciousness]] from [[increased intracranial pressure]] (ICP)
+* Symptoms of [[increased intracranial pressure]] (ICP)
-* Progression of focal neurological deficits over periods of hours
+* Focal neurological deficits
-|[[CT]] scan without contrast
+|[[CT]] without [[Contrast medium|contrast]]
+(differentiate [[ischemic stroke]] from [[hemorrhagic stroke|hemorrhagic stroke.]])
 |
-* [[CT scan]] without contrast is the initial test performed to differentiate [[ischemic stroke]] and rule out [[hemorrhagic stroke|hemorrhagic stroke.]]
 * [[CT]] is very sensitive for identifying acute [[hemorrhage]] which appears as hyperattenuating clot.
 * Gradient echo and T2 susceptibility-weighted [[MRI]] are as sensitive as [[CT]] for detection of acute hemorrhage and are more sensitive for identification of prior hemorrhage.
 |
 * [[PT]]/ [[INR]] and [[aPTT]] should be checked to rule out [[coagulopathy]].
-|-
-|[[Cerebral]] [[Infarction]]
-|Headache with tightness around the forehead and focal neurological deficits
-|The [[symptoms]] of an [[ischemic stroke]] vary widely depending on the site and blood supply of the area involved. For more information on [[symptoms]] of [[ischemic stroke]] based on area involved please [[Ischemic stroke#Diagnosis#History and symptoms|click here]].
-|[[Cerebral angiography]]
-|
-* [[CT scan]] without contrast is the initial test performed to diagnose [[ischemic stroke]] and rule out [[hemorrhagic stroke|hemorrhagic stroke.]] CT may show hypo-attenuation and swelling of involved area.
-* [[MRI|MR]] diffusion weighted imaging is the most sensitive and specific test for diagnosing [[ischemic stroke]] and may help detect presence of [[infarction]] in few minutes of onset of [[symptoms]].
-|
-* [[Carotid]] [[doppler]] may be done to check for patency of [[carotid arteries]] and blood supply to the [[brain]].
-* [[Cerebral angiography]] is an [[Invasive (medical)|invasive]] test and detect [[abnormalities]] of the [[blood vessels]], including narrowing, blockage, or [[malformations]] (such as [[Aneurysm|aneurysms]] or [[arterio-venous malformations]]).
 |-
 |[[Intracranial venous thrombosis]]
+|Gradual
 |
-* Diffuse [[headache]] that progresses over several days to weeks
+* Diffuse [[headache]]
 * [[Headache]] can be the only symptom of [[Cerebral venous sinus thrombosis|cerebral venous thrombosis]]
 |
-* Inability to move one or more limbs.
+* Focal neurological dfeficits
-* Weakness on one side of the face.
+* [[Seizure|Seizures]]
-* [[Seizure|Seizures]]: 40% of all patients have seizure.
+* [[Coma|Depressed level of consciousness]]
-* [[Coma|Depressed level of consciousness]] and otherwise unexplained changes in [[mental status]] are common symptoms in the elderly.<sup>[[Cerebral venous sinus thrombosis history and symptoms#cite note-4|[4]]]</sup>
 |[[Digital subtraction angiography]]
 |
@@ Line 181: / Line 179: @@
 |-
 |[[Migraine]]
-|Severe or moderate [[headache]] (which is often one-sided and pulsating) lasts between several hours to three days.
+|Sudden
 |
-* Gastrointestinal upset such as [[nausea and vomiting]]
+* Severe to moderate [[headache]]
-* Preceding [[Aura (symptom)|aura]] (in 35% pts)
+* One-sided
-* Heightened sensitivity to:
+* Pulsating
-** Bright lights ([[photophobia]])
+* Lasts between several hours to three days.
-** Noise ([[phonophobia]]).
+|
+* [[nausea and vomiting]]
+* Preceding [[Aura (symptom)|aura]]
+* [[photophobia]]
+* [[phonophobia]]
 |'''---'''
 |
@@ Line 195: / Line 197: @@
 |-
 |[[Head injury]]
+|Sudden
 |Headache:
 Dull
@@ Line 219: / Line 222: @@
 |-
 |[[Lymphocytic hypophysitis]]
+|
 |Headache:
 * Generalized
@@ Line 233: / Line 237: @@
 |-
 |[[Radiation injury]]
+|
 |Headache develops gradually
 |

Pituitary apoplexy differential diagnosis: Difference between revisions

Revision as of 16:29, 1 August 2017

Overview

Differentiating Pituitary apoplexy From Other Diseases

References

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