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DVM 3 - 2 > Dogs and Cats 23 > Flashcards

Dogs and Cats 23 Flashcards

1
Q

A-V blocks what are the 3 degrees and what occurs

A

○ First degree - prolonged PR interval
○ Second - intermittent AV conduction
○ Third degree - complete AV block with escape rhythm and no relationship between P and QRS - AV dissociation

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2
Q

Approach to A-V blocks what need to rule out and what is priamry cardiac

A

i. Rule out drug administration, electrolyte disturbance - especially for first degree blocks
ii. If primary cardiac, often not structural - CANNOT FIX
□ Long-term anti-cholinergic may help if positive response to test
□ Pacemakers
® Good long-term response
® Better if no CHF
® Some mild complications
® Expensive

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3
Q

A-V block when to determine whether vagal stimulated, what treat with and causes

A 
□ To determine whether vagal -> Administer atropine (0.04 mg/kg IV) and repeat ECG 10-15minutes later 
® If HR increase by 100% or > 140 bpm = vagal 
® If P rate increase but QRS doesn't = not vagal 
® If in between repeat test
® If no change P than atrial standstill
® SSS variable response  
□ Causes of excess vagal tone 
® Chronic respiratory disease
® GI disease
® Hypothyroidism 
® Ocular or retrobulbar disease
® CNS (increase intra-cranial pressure)
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4
Q

what are some important points to remember about A-V blocks

A

§ In AV blocks if the conduction system is OK high up in the ventricular conduction system the more normal the QRS looks
§ AV blocks can be due to structural disease - BUT OF THE CONDUCTION SYSTEM NOT USUALLY THE MYOCARDIUM
§ Generally if treating a tachyarrhythmia we don’t want to also decrease heart contractility

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5
Q

congenital cardiac disease classification, what do they cause and main types in dogs and cats

A

Classification
- Arteriovenous shunts
- Failure of normal valve development
- Incomplete separation or mal-positioning of great vessels
- NEARLY ALWAYS cause murmur BUT DON’T ALWAYS cause congestive heart disease
○ Intensity of murmur not related to how bad it is
Types
- Dogs: patent ductus arteriosus (PDA) -> pulmonic stenosis (PS)/ Aortic stenosis (AS)
- Cats: AV dysplasia/VSD

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6
Q

Extra-cardiac shunt = PDA signalment and pathophysiology

A
  • Common in dogs
  • Females > males
  • Genetic predisposition some breeds
  • What occurs
    ○ PDA diverts foetal blood from PA into aorta
    § Aorta pressure > PA pressure in diastole and systole so LEFT TO RIGHT SHUNT at all stages of cardiac cycle when born
    □ Unless there is pulmonary hypertension (reverse PDA)
    ○ Increased venous return from lungs
    § Volume overload on LA and LV - dilation and hypertrophy
    ○ Increased after-load on RV
    § Concentric hypertrophy (not as significant as left-side)
    ○ Aneurysm (bulge) in descending aorta
    ○ If pulmonary hypertension
    § PA pressure > aorta pressure so R to L
    □ Usually very large shunt so resistance to flow
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7
Q

PDA clinical signs when not and when often clinical and then what occurs

A

○ Often not clinical, but may show fatigue or poor growth
§ CHF develops within 6 - 12 months if it is going to at all
○ With right-left shunts - reversal
§ Due to pulmonary hypertension
□ Consequence of PDA
□ Occurrence congenital or acquired pulmonary disease
§ Chronic hypoxia leads to polycythaemia (massively increased PCV and hyperviscosity) -> seizures
§ Murmur may get softer
§ May not heart murmur
○ Differential cyanosis - may occur
§ Caudal part of the body blood supply occurs as shunting occurs so deoxygenated blood at this point
§ Cranial part of body supplied by brachycephalic trunk branches off aorta BEFORE PDA -> oxygenated blood

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8
Q

What are the 2 main clinical findings with a PDA

A

1) Continuous (machinery) murmur detected at vaccination
§ Aortic pressure is always greater than PA pressure systole and diastole
§ Precordial thrill at left heart base - may be able to feel
2) Widened pulse pressure
Low aortic diastolic pressure

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9
Q

What are the 3 main ways to diagnose a PDA

A

○ Clinical findings - continuous murmur over left side in puppy - not much else can do this
○ Radiography
§ Lateral - cardiac enlargement, especially LA, pulmonary over-circulation, CHF if severe
§ DV - triple bulge: PA, aorta, L auricle
○ Echocardiography - can see the shunt and enlarged left atrium

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10
Q

What are the first 3 types of PDA, what occurs, diagnose and treatment

A

○ Type 1 - small PDA
§ Generally asymptomatic L -> R shunt
§ X-ray normal at 1-2 years
§ Surgery not urgent but recommended for normal life span
○ Type II - medium PDA
§ Asymptomatic L -> R shunt with continuous murmur and thrill L heart base and also audible at L apex (mitral regurgitation due to LV dilation) and normal-bounding pulse
§ Mid-moderate heart enlargement < 1 year old
§ Surgery recommended, but can wait a few weeks
○ Type III a - large PDA prior to CHF
§ Usually decreased exercise tolerance with continuous murmur and thrill present over most of the left thorax and often MR murmur at L apex with bounding pulse
§ Marked heart enlargement < 6 months old with significant increase in pulmonary vascular marking
§ Surgery recommended without delay

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11
Q

What are the last 2 types of PDA what occurs, clinical signs and treatment

A

○ Type III b - large PDA plus CHF
§ All of IIIa feature PLUS dyspnoea due to pulmonary oedema
§ Often in poor body condition and may have atrial fibrillation
§ Treat medical conditions prior to surgery as soon as stable
○ Type IV - large PDA plus pulmonary hypertension
§ R -> L or balanced shunt
§ May show weakness or collapse with exercise (can present from 2 weeks to 12 years)
§ NO SURGERY (contraindicated due to pulmonary hypertension), treatment is medical (phlebotomy, hydroxyurea) to decrease PCV

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12
Q

Treatment for PDA and prognosis

A
  • Surgery
    ○ Methods of ligation
    § Surgical ligation - requires thoracotomy so some risk and post-op chest drain
    □ Haemorrhage possible but recovery good
    § Coil embolization - transvenous using fluoroscopy - better probably
    ○ Restrict exercise one month post-op
  • Prognosis
    ○ Much better if corrected
    ○ Concurrent MR worsens prognosis
    ○ Age at which closed or presence of CHF does NOT worsen prognosis
    ○ Individual variation
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13
Q

Pulmonic stenosis types, how common in dogs and what occurs

A
  • Valvular, sub-valvular or supra-valvular
  • Relatively common in dogs
    ○ English bulldogs (male)
    ○ Boxers
    ○ Beagles (inherited)
    ○ Small breeds
  • What occurs
    ○ Reduced diameter of RVOT (right ventricular outflow tract)
    § Increased after-load
    § Concentric hypertrophy
    ○ Post-stenotic dilation as blood increases in velocity - why hear murmur
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14
Q

Pulmonic stenosis clinical signs

A

○ Incidental murmurs
§ Ejection murmur LEFT HEART BASE
§ Normal femoral pulses
§ 10% have diastolic murmur as well
○ Exercise fatigue, weakness and syncope if severe
○ Rarely get RSCHF unless concurrent tricuspid dysplasia

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15
Q

Pulmonic stenosis diagnosis

A

○ Clinical findings
○ ECG
○ Radiographs
§ DV gets reverse D with pulmonary trunk bulge due to dilation
§ RV enlargement
§ Contrast angiography
○ Echocardiogram
§ Needed for severity assessment and diagnosis
§ RV hypertrophy and RA dilation
§ Narrowing at pulmonic valve
§ Measure velocity and convert to pressure gradient for treatment recommendations

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16
Q

Pulmonic stenosis when to treat

A

○ Pressure gradient > 80mmHg
§ Increased risk of syncope/sudden death
§ Treatment currently recommended
○ Pressure gradient 50-80 mmHg
§ Asymptomatic but long-term prognosis poor
○ Pressure gradient < 50mmHg
§ Mild stenosis so don’t really require treatment
○ May live a normal life span if no clinical signs - NO BREEDING
○ IF there is RSCHF due to concurrent tricuspid dysplasia then treatment may be beneficial regardless of severity

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17
Q

Pulmonic stenosis treatment options

A

○ Closed patch graft
○ Closed valvulotomy
○ Balloon dilation (valvulopasty) - most recommended
§ Down the jugular and then dilate
§ Best response if CHF at time of diagnosis
§ Some associated mortality
§ Still have increased pressure gradient

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18
Q

Aortic stenosis which most common, breeds and pathophysiology

A
  • SAS most common
    ○ Fibrous ring of tissue immediately below aortic valve
  • Newfoundlands, boxers and goldern retrievers
  • Pathophysiology:
    ○ Increased after-load on LV
    § Concentric LV hypertrophy
    ○ Flow becomes turbulent distal to the stenosis
    § Post stenotic dilation
    ○ Coronary arteriosclerosis and myocardial necrosis/fibrosis develops
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19
Q

Aortic stenosis clinical signs

A

○ Exertional syncope and sudden death
§ Bradycardia secondary to increased LV systolic pressure and vasodilation
§ Arrhythmias usually secondary to haemodynamic changes
○ Not many get LSCHF
○ Murmur may be incidental
§ L base but pulses will be weaker
§ To and fro if also insufficiency
§ Takes time to develop as hypertrophy progresses
§ Not clear about severity until > 12 months

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20
Q

Aortic stenosis diagnosis

A 
○ Physical examination 
○ Radiography 
§ LV enlargement and post-stenotic dilation 
○ Echocardiography - gold standard 
§ LA enlargement and dilation of ascending aorta
§ LV hypertrophy
§ Turbulence
Measure velocity across aortic valve
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21
Q

Aortic stenosis treatment

A

○ Not indicated for mild disease
○ Prophylactic antibiotics
○ Exercise restriction
○ Beta-blockers
○ Balloon dilation
§ Very technically demanding - cannot go through jugular
§ No evidence actually prolongs survival
§ May be helpful if CHF due to concurrent MVD

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22
Q

AV valve malformations what are the 2 main ones, what common in and what result in

A
  • Same as acquired valvular disease - same treatment
    1) Tricuspid
    ○ Part of multiple defects in cats
    ○ Large-breed dogs
    ○ Labradors
    ○ Usually insufficiency due to fusion of chordae or thickening of leaflets
    2) Mitral
    ○ Very common sole or as part of ecd in cats
    ○ Large-breed dogs
    ○ English bull terrier
    ○ Usually insufficiency not stenosis
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23
Q

Tetralogy of fallot how common and consists of

A
  • Uncommon ( cat < dog)
  • Consists of:
    ○ High VSD
    ○ Pulmonic stenosis
    ○ Overriding aorta
    § Dextroposition
    ○ RV hypertrophy
    § Compensatory
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24
Q

Pulmonary hypertension diagnosis and treatment

A

Diagnosis
- Often one of suspicion NOT conformation
- Echo can show signs of increased RV outflow obstruction (increased PA velocity; tricuspid regurgitation)
- Echo can be normal
Treatment
- Treat underling cause if possible
○ Heart worm or pulmonary oedema
- Phosphodiesterase inhibitors at the moment main stay of treatment - if above not effective
○ Pimobendan
○ Sildenafil - vigra - vasodilator - only if pimobendan doesn’t work by itself
○ Theophylline

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25
Q

Systemic hypertension what is it and causes with most common and not common

A
  • Persistently high arterial blood pressure (BP)
  • BP = CO x TPR
  • BP = (HR x SV) x TPR
  • Very important disease of cats
    Causes
  • Primary
  • Secondary
    ○ Renal disease - MOST COMMON
    ○ Cardiac disease
    ○ Hyperadrenocorticism
    ○ Hypokalaemia
    ○ Diabetes mellitus (dogs not cats)
    ○ Acromegaly
    ○ Polycthaemia
    ○ Pheochromocytoma
    ○ Hyperthyroidism - NOT COMMON - If have hypertension with hyperthyroidism then probably have concurrent renal disease
    OR stress-induced false reading - VERY COMMON
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26
Q

Why is hypertension important

A
  • Risk or organs with small capillary beds
  • Eye -> haemorrhage, chorioretinopathy, detachment
  • Heart -> hypertrophy, murmur, arrhythmia, gallop
  • Brain -> HT-encephalopathy
  • Kidneys -> progressive renal disease
  • -> possible catastrophic pathology before diagnosis
    ○ Retinal detachment
    ○ Why recommend older cats get annual blood pressure checks
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27
Q

Measuring blood pressure what is the 2 main ways and the gold standard

A
  • Direct - gold standard
  • Indirect
    ○ Doppler and sphygmamometer
    § Best for cats
    ○ Oscillometry
    Good for High definition oscillmetry for dogs
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28
Q

Doppler measurement of BP what does it measure, cuff width needed and technique

A

measures systolic BP

  • Cuff width = 30-40% of circumference
  • Standardise protocol (white coat effect)
    1. quiet environment
    2. Acclimatisation period
    3. At least 3-5 consistent measurements
    4. Repeat abnormal findings (ensure persistent)
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29
Q

Approach to diagnose before there is an issue with hypertension

A
  • Establish if possible that there is a true reading
  • Full CBC, biochemistry, electrolytes
  • Total T4
  • Urine (cystocentesis)
  • Consider abdominal ultrasound if hypokalaemia
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30
Q

Treatment of hypertension in cats what are the 6 main component

A
  1. Identify and treat underlying cause if possible
  2. Weight reduction
  3. Decrease dietary NaCl
  4. Supplement potassium if low
  5. Consider aldosterone antagonism if hypokalaemia (spirolactone)
  6. Specific hypotensive drugs
    ○ Amlodipine +/- ACE inhibitor
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31
Q

Amlodipine what is it, what does it do, onset, duration, efficacy and dosing

A

treatment of hypertension in cats and dogs

  • Block Ca2+ influx into vascular smooth muscle -> VASODILATION
  • Slow onset of action
  • Long duration of action
  • Good efficacy
  • ONCE daily dosing
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32
Q

ACE inhibitors what used for, types, mechanism of action, efficacy

A

treatmetn of hypertension in cats and dogs

  • Benazepril, enalapril, ramipril
  • RAAS inhibition and weak vasodilation
  • Poor efficiacy - 50% cats
  • Target organ protective? Not if azotaemia
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33
Q

Treatment of hypertension in dogs

A
  • Prazosin if renal failure
  • Amlodipine
  • ACE inhibitors minimal effect
  • Beta-blockers may be considered
  • Treat underlying disease
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34
Q

Radiographs and the brain how sensitive and pros and cons

A

Radiographs are insensitive for most brain diseases
PROS
- Readily available to most veterinarians
- Good screening tool for some diseases
CONS
- Limited to detecting bone changes
- Complex anatomy makes interpretation difficult

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35
Q

Ultrasound and imaging the brain how can work

A

Ultrasound doesn’t work properly -> encased in the brain which doesn’t work with ultrasound

  • Thin spot (open fontanelle) in the skull -> can use to ultrasound the brain - very cranial part of the brain
  • Sometimes gain access through foramen magnum
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36
Q

CT vs MRI what good for

A

CT - allows brain case to be easily seen -> skull fracture

MRI - provides the best evaluation of neural tissue - BEST FOR BRAIN - great contrast - lesions look white

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37
Q

CT or MRI for the following situations 1. head trauma, 2. seizures, 3 hilt tilt 4. altered mentation 5. pituitary disease 6. trigeminal or facial neuopathy

A
  1. CT - bone lesion and hameeorhage most common
  2. MRI - lesion looking for within brain
  3. CT - if peripheral (history of otitis), MRI if central
  4. MRI - subtle disease
  5. CT - most seen n CT only MRI if subtle
  6. MRI
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38
Q

Contrast studies with the brain how used, how works and examples of contrast agents

A

Lesions are often better seen with intravenous contrast
- Where possible always give intravenous contrast
- Contrast enhancement occurs due to increased vascularity OR breakdown of the blood brain barrier - EXAM - leak of contrast
1) Iodinated contrast agents for computed tomography
- Eg Iohexol
○ High atomic number absorbs more x-rays appears white
2) Paramagnetic contrast agents for magnetic resonance imaging
- Eg gadolinium
○ Alters the local magnetic field shortens TI relaxation time appears white on TI weighted sequence
§ HAS TO BE TI WEIGHTED

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39
Q

What are some important interpretation that need to occurs when imaging the brain

A 
- Location:
○ cranial vs caudal fossa
○ lobes? brain stem?
○ intra-axial or extra-axial
- Mass effect:
○ midline shift &amp; herniation
- Cerebral oedema:
○ vasogenic, cytotoxic, periventricular
- Haemorrhage: how old is the lesion?
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40
Q

Brain anatomy for imaging what are important aspects

A
  • cribriform plate - nasal issues may infiltrate brain through this - see if intact
  • cranial fossa - everything cranial to fossis tentorium
  • Brain anatomy why important?
  • To correlate lesion location with clinical signs
    § DO THEY MATCH?
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41
Q

Brain lesions what are the 2 classification why classified and define each one with examples

A
  • Helps prioritise differential diagnoses
    1) Intra-axial brain lesions arise from brain parenchyma
    ○ surrounded by brain parenchyma
    ○ Narrow area of contact with skull
    ○ Examples: glioma, lymphoma, neurocytoma, neuroepithelial tumour, abscess, granuloma, necrosis, haematoma.
    2) Extra-axial lesions arise from outside brain parenchyma
    ○ ‘broad’ base toward the periphery of the brain
    ○ +/- dural tail (meninges thickened above and beyond the largest part of the mass)
    ○ Examples: meningioma, pituitary tumour, choroid plexus tumour, ependymoma, bone tumour, abscess, subdural haematoma
42
Q

The mass effect what is it and the 3 types

A
  • The addition of material (cells, oedema fluid, blood etc.) to a fixed volume cavity
  • Causes displacement, compression and distortion of normal anatomy
    Recognising the ‘mass effect’ can help identify the type of lesion - particularly important in CT study as cannot see specific changes as well
    3 TYPES
    1. midline shift - faulx cerebri moving out of midline
    2. ventricular obstruction
    3. herniation
43
Q

Cerebral oedema how seen in MRI and CT and the classification

A

MRI - hyper-intese (bright)
CT - hypo-attenuating (dark)
- The MRI appearance of cerebral oedema is classified according to LOCATION, which is dictated by pathophysiology.
○ Vasogenic / Cytotoxic / Periventricular Oedema
- Understanding this helps prioritise differential diagnoses.

44
Q

What are the 3 types of cerebral oedema in MRI, what look like, where trach and when occurs

A
  1. Vasogenic oedema is the most common type of cerebral oedema
    - increased permeability of vascular endothelium
    - tracks along white matter
    - often associated with tumours, necrosis, other mass lesions
    - occurs with diffuse vascular injury
  2. Cytotoxic oedema is confined to grey matter
    - Tacks along the grey matter (white within the grey matter on imaging)
    - ischemia -> failure of ATP sodium pumps -> sodium accumulation within cells -> cells swell with water (ECF)
    - less mass effect than vasogenic oedema
    - may be caused by hypoxic injury, hepatic encephalopathy
  3. Periventricular oedema occurs with acute increase in intra-ventricular pressure
    - increased ventricular pressure - > CSF seeps through ependyma and into adjacent brain parenchyma - CONCERNED ABOUT ACUTE INCREASE IN VENTRICULAR PRESSURE
    - around ventricles and occurs with obstructive hydrocephalus
45
Q

Hemorrhage when imaging the brain how good are CT and MRI, why and which sequence is best

A

CT is sensitive for haemorrhage
- hyper-attenuating (bright)
- rapid acquisition : preferred for acute head trauma
MRI can detect small haemorrhages & indicate age of haemorrhage
- complex changes to signal on T1W and T2W sequence depending on age of haemorrhage
○ Iron within blood cells, iron will dissociate from haemoglobin, eventually blood cells lyse and iron and haemoglobin within the haemorrhage
○ Acute haemorrhage bright on T2 dull on T1
- T2* GRE sequence is VERY sensitive for haemorrhage: appears black

46
Q

Skull trauma which imaging modalities are good, why and what looking for

A
  • Ultrasound - don’t bother
  • MRI - maybe depending on status of patient
  • CT is often preferred
    ○ rapid acquisition
    ○ sensitive for haemorrhage
    ○ excellent evaluation of bone
    ○ ability to perform 3D reformats
  • Look for: displacement of bone, lucent lines through bone, displacement of fragments toward brain, subdural haemorrhage
    ○ GOOD FOR: differentiating whether fracture is there and if it has gone into the cranium and effecting the brain
    § Prognosis VERY DIFFERENT depending on this so good
  • DON’T FORGET - teeth, TMJs, orbits, cervical spine are often also affected
47
Q

Neoplasia of the nasal cavity what are the 2 main modalities used, what see and which more sensitive

A
  1. Radiograph
    - Nasal neoplasia
    ○ increased opacity of nasal passages
    ○ lysis of turbinates and flat bones
    ○ look for lysis of the cribiform plate
  2. CT is more sensitive than radiographs for evaluation of nasal disease and cribriform plate destruction
48
Q

Neoplasia of the skull common types, what occurs and main modalities used for what

A
  • eg. OSA, FSA, ChSA, MLO (multi-lobular osteosarcoma)
  • Lysis & new bone production
  • Radiographs can underestimate extent of the neoplasm but can be useful for skull neoplasia diagnosis
  • CT or MRI preferred to assess brain involvement, but may not be necessary for diagnosis!
49
Q

Brain neoplasia what require for diagnosis which more sensitive and what principles need to consider

A 
usually requires CT or MRI for diagnosis
- MRI more sensitive
- Consider principles of interpretation discussed earlier
○ intra-axial vs extra-axial
○ mass effect
○ oedema
○ +/- haemorrhage
50
Q

Hydrocephalus what is it, radiographic features and other ways identified

A
  • dilation of the ventricles
  • congenital or acquired (eg. obstruction to CSF drainage, CSF overproduction)
    Radiographic features of hydrocephalus
  • doming of calvarium
  • cortical thinning
  • persistent fontanelle
  • ‘copper beaten’ skull
    Hydrocephalus may be identified on ultrasound
  • dilated lateral ventricles = large spaces of anechoic fluid
  • Hydrocephalus with advanced imaging
    -> CT (dark), MRI (bright)
51
Q

Ischemic infarcts in the brain what also called, which modality best and other can be used

A

MRI is very sensitive for ischemic infarcts or ‘stroke’

  • Seen as restricted diffusion of water on DWI & ADC sequences
  • ischemic area in geometric pattern
  • Haemorrhagic infarcts are also easily detected on MRI but appear similar to haemorrhagic tumours
52
Q

Intumescenes what are the and meninges

A

○ Variation in diameter - Intumescences (thicker areas)
§ Thicker C6-T2 and L4-S3 -> because more grey matter -> corresponds with brachial and lumbosacral plexuses
□ Exerts control of the limbs
□ If have disc intrusions in these areas -> less space in the area -> NOT GOOD
○ Meninges
§ Bedding around the spinal cord, protections against mechanical
§ Also blood brain barrier for chemical

53
Q

Asynchronous growth of the spinal cord and vertebral canal where does this occur, what occurs

A

§ Cauda equina
□ Vertebral column keeps growing once spinal cord stops -> L4-L5 spinal cord stops - ONLY NERVE ROOTS past this point and vertebral column
® Lots of nerve roots at cauda equina area
® L7 nerve roots exit from spinal cord level of L7 and S1

54
Q

Internal anatomy of teh spinal cord what are the 2 main tracts what do they do and where located

A 
○ Mainly fibers (tracts)
§ Brain → organs = descending
§ Organs → brain = ascending
○ Ascending tracts
§ Proprioception - located mostly on outside layers of the white matter
§ Other sensation
□ Tactile, cold/heat, pain…
○ Descending tracts
§ Motor functions - located deeper in white matter near the grey matter 
§ Voluntary control of urination
55
Q

In generaly what is involved in the neurological examination

A 
- Observation (hands off)
○ Mental status
○ Behaviour
○ Gait
- Palpation
- Postural reactions
- Spinal reflexes and tone
- Cranial nerves
- Sensory systems = assessment of pain
56
Q

What are the main clinical signs for pathology in the following areas 1. meninges, 2. proprioceptive 3. other sensations 4. voluntary movement 5. grey matter in middle (intumescences)

A
  1. PAIN - back and neck pain
  2. ataxia, postural reactions absent
  3. loss of pain reception or hyperaesthesia
  4. paraesis
  5. hyper-reflexes and muscle atrophy
57
Q

neck/back pain general clinical signs and how to help test

A
  • Crouched stance and gait
  • Kyphosis = “arched back”
  • Diverse postures…
  • Neck pain -> if move food around normal will move the neck, neck pain will move shoulders
    ○ Could just be a twitch in the neck
58
Q

When you have lesions affecting ascending tracts what are the 2 main clinical presentations and things within

A

1) Proprioceptive (spinal, but not proper word) ataxia
§ Other ataxia -> Vestibular ataxia or cerebellar ataxia ALSO - so DON’T JUST SAY ATAXIA
○ Forebrain, spine or brain stem can be the issue
○ Does the animal know where its limbs are relative to his body?
○ Knuckling over = dragging digits
§ Working on the dorsal aspect
○ Crossing limbs
2) Abnormal postural reactions
○ Poor placing responses -> flip toes and wait for them to replace their feet
○ Hopping and hemi-walking - poor response

59
Q

Descending tracts lesions what are the 2 main clinical presentations and things within

A 
motor tracts - voluntary motor control compromised 
- Paresis
○ (Mono-) - only one limb affected 
○ Para- Pelvic limbs
○ Hemi- Right or left limbs (thoracic and pelvic)
○ Tetra- All four
- Plegia
○ No voluntary movement
○ Same descriptions as above
60
Q

Spinal cord reflexes and tone what help determine, when normal or decreased and what are the 2 main examples

A 
to determine whether UMN or LMN 
- Normal or increased - upper motor neurons lesions
○ C1 to C5 and T3 to L3
- Decreased or absent - lower motor neurons lesions 
○ C6 to T2 and L4 to S3
Examples 
1) crossed extension reflex 
2) cutaneous trunci reflex
61
Q

Crossed extension reflex what is it, what need to do and what occurs with spinal cord lesion

A

spinal cord reflex
§ Apply mechanical stimulus of right hindlimb -> ganglion -> corresponding spinal cord segment -> interneuron and then stimulation of flexor muscle in SAME LEG (withdraw reflex)
§ ADDITIONALLY -> another interneuron goes to opposite side and stimulate extensor muscles in the other leg
□ NORMALLY inhibited by brain
□ SPINAL CORD LESION (deep within white matter) prevents inhibition - RESULTS IN CROSSED EXTENSION (pathological finding

62
Q

Cutaneous trunci reflex what is it, how performed, what abnormal and how accurate

A

spinal cord reflex
§ stimulate the skin - segmental innervation of the skin -> into spinal affected -> coordination at level of C7-T1 spinal cord segment -> stimulation of lateral cutaneous nerve -> stimulates cutaneous truni -> shaking of BOTH SIDES of the trunk
§ LESIONS PRESENT ->
□ T13-L1 - caudally stimulation -> NO RESPONSE
® Eventually when move cranially to the lesion WILL STIMULATE -> possibly used for localisation?
§ NOT very accurate though

63
Q

Localisation of spinal cord lesions what are the 2 things to as and therefore how to localise

A

NEED TO BE ABLE TO NAME THE SPINAL CORD SEGMENTS
- Locate to these segments
Question 1 to ask
- is it all four legs - C1-C5 OR C6-T2
- Is it in pelvic limbs - T3-L3 OR L4-SI
Question 2 to ask
- Are the reflexes normal or increased - C1-C5 OR T3-L3
- Are the reflexes decreased - C6-T2 OR L4 - S3

64
Q

Urinary continence how affected with UMN and LMN

A

○ Voluntary control -> S1-S3 - Pudendal nerve -> voluntary control - straited nerve for the sphincter
○ UMN bladder - lesion anywhere BUT S1-S3
§ Lack of inhibition -> TOO MUCH STIMULATION of sphincter
§ Very hard bladder that is difficult to
○ LMN bladder - lesion in S1-S3
§ Soft bladder that is easy to express

65
Q

Testing sensation why is it important

A
  • Is dog able to feel pain -> reflex will be present but is it aware of what is happening??
  • Assessment ≠ withdrawal reflex
  • Superficial vs deep pain?
  • indicates WORSE COMPRESSIVE LESIONS
66
Q

Schiff-sherrington syndrome what is it, where lesions and clinical signs that results

A
  • Border cells - deep within spinal cord
    ○ Represent ascending tract within white matter -> back legs have inhibitory control of forelimbs
  • Severe thoraco-lumbar lesion
    ○ Lack of inhibition - too much stimulation of front legs -> over extension of the front legs (normal proprioception)
67
Q

Severity of compression lesion in terms of loss of function as get more serious and what if non-compressive?

A
  • Sequential loss of functions as get more severe (deeper compression within white matter)
    ○ Proprioception
    ○ Voluntary motor function
    ○ Urinary (faecal) continence
    ○ Loss of (Pain) sensation -> worse compression lesions
    And what if non compressive?
  • E.g. Urinary incontinence + normal motor function
68
Q

Intervertebral disk anatomy where present, mechanical properties and the two parts and what made of and function

A 
- From C2 to S1
		○ None at C1-C2!
	- Mechanical properties
		○ Joint between vertebrae (two vertebrae can fuse together if lose one disc - not the end of the world) 
○ Shock absorption 
○ Allow wide range of movements
§ Bending
§ Twisting
1) Annulus = outside
○ Collagen
○ Innervated
§ Pain-
2) Nucleus pulposus = inside
○ Watery content
○ Shock absorption - gives it the mechanical property
69
Q

Intervertebral disk changes what are the 2 types, what occurs, signalment and final process

A
  1. Chondroid metaplasia - TYPE 1 DISC (Hansen I)
    ○ Dehydration of nucleus pulposus
    § Jelly-like → “tooth paste” to very hard/calcified
    ○ Chondrodystrophoid breeds – early onset
    § Completed in Dachshunds between 2 and 5 years
    § Most of the discs are dehydrated and sometimes completed calcified
    ○ Final process = tear in dorsal annulus (dehydrated nucleus moves up into the vertebral canal) → disk extrusion
    § Trauma usually minimal = playing, jump onto/from the couch, not witnessed at all…
  2. Fibroid metaplasia - TYPE 2 DISC (Hansen II)
    ○ Nucleus pulposus changed into fibro-cartilage
    ○ Older large breed dogs – later onset
    ○ Final process = progressive thickening of nucleus (more able to adapt, less pressure) + annulus → disk protrusion
70
Q

What are the 4 main disk disease and the 2 associated processes

A
  • Disk extrusion, Hansen I
  • Disk protrusion, Hansen II
  • Acute Non-compressive Nucleus Pulposus, Extrusion (“Hansen III”)
  • Nucleus pulposus extrusion of non-degenerate nucleus
  • Disk associated processes
    ○ Caudal Cervical Malformation Syndrome (CCMS)
    ○ Degenerative Lumbo-Sacral Stenosis (DLSS)
71
Q

Disk extrusion (type I) how common, signlament

A 
- The most common type
○ Overall 2% of dogs
- Mainly small breed dogs
○ Chondrodystrophic
§ 20% of Dachshunds have IVDD
§ Pekingese, French Bulldog, Jack Russell Terrier, Lhasa apso, Shih tzu
○ Non-chondrodystrophic
§ Cocker spaniels, Beagle, bichons, miniature Poodle
○ 90% of IVDD in large breed dogs are extrusions! (the rest have disc protrusion but A LOT LESS COMMON) 
- Age
○ 2 to 7 years in chondrodystrophic
○ 6 to 8 years in non-chondrodystrophic
72
Q

Disk extrusion (I) lesiosn location and signs (where worse)

A
  • Lesion location
    ○ T11 to S1
    § Intercapital ligament - PREVENT THE DISC EXTRUSION
    ○ 75% between T12 and L2 - area of great movement in the spinal cord
    ○ C2 to T1 (neck) - Beagle!
  • Symptoms and signs
    ○ Acute or subacute (≤ 2w)
    ○ From back / neck pain to paralysis with loss of pain sensation (progress the longer you leave without treatment)
    ○ Thoracolumbar more severe than cervical -> spinal cord to vertebral canal ratio is higher so more room to move In the neck
  • Therefore beagles generally just have neck pain, Bichons generally get paralysis straight away
73
Q

What is the grading system for compressive lesions in terms of clinical signs - EXM

A

○ Grade 1 - Back pain
○ Grade 2 - Ambulatory ataxia and/or paresis
○ Grade 3 - Non ambulatory ataxia and/or paresis (still able to move the legs a little bit)
○ Grade 4 - Paralysis = loss of voluntary motor function
○ Grade 5 - Loss of pain sensation

74
Q

Diagnostic modalities for compressive lesions in spinal cord what are the 4 main ones

A

1) radiograph
2) myelography
3) CT-scan
4) MRI

75
Q

In terms of radiographs and myelopgraphy for diagnosing disk extrusions what good and bad for with limitations

A

1) Radiographs
§ Disk calcification
§ Narrowed IV disk space
§ Narrowed intervertebral foramen
§ Lack of sensitivity - don’t grade based on X-ray
2) Myelography
§ Improve Sensitivity of radiograph
§ Accessibility better than CT or MRI but accuracy a lot lower
§ Extradural lesion
§ Oblic views
§ Limitations
□ Technical issues
□ Spinal cord swelling (doesn’t move within)
□ Myelomalacia (spinal cord totally destroyed)
□ Toxicity/Safety

76
Q

In terms of CT and MRI for diagnosing disk extrusion what good for and limitations

A 
1) CT-scan
§ Excellent bone resolution
§ Very quick - 10 mins 
§ IV contrast injection
§ Subarachnoid contrast injection: CT-myelogram - to increase visualisation of soft tissues 
2) MRI
§ Best resolution for soft tissues
§ Safe
§ Long acquisition time - 60 mins under GA
§ Expensive and accessibility is low
77
Q

in terms of disk extrusion when is surgery recommended - EXAM

A

○ Grade 5 within 48h (otherwise irreversible damage)
§ In practice ASAP!
○ Grade 3 and higher
§ Non-ambulatory
§ Sooner is better - better and more likely to recover
§ Meta-analysis in humans in favour of prompt decompression

78
Q

In terms of disk extrusion what medical management or post-opertaive treatment is needed

A

1) Strict rest - MOST IMPORTANT - if don’t may lead to paralysis
§ At least 4 weeks -> allow the immune system to come in and remove the disc material from the spinal cord
□ No walking up-stairs, no toys, no other dogs, stay on the bed and outside only for faeces
§ 4 weeks of progressive reintroduction of exercise
2) Pain management
§ Opioids
□ Injections, CRIs, patches
§ Ketamine, lignocaine
§ Gabapentin 10 to 30mg/kg TID - HOME (oral)
§ Tramadol 2 to 10 mg/kg TID - HOME (oral)
§ NSAIDs - HOME (oral)
§ Corticosteroids - CONTRAINDICATED - no benefits

79
Q

What are the 3 main complications of disc extrusions surgery or medical treatment

A

1) Deterioration
§ Loss of motor function - respiratory
§ Urinary/fecal incontinence, urinary tract infections
§ Loss of sensation, digital wounds, infection
2) Ascending-descending myelomalacia
§ Grade 5 risk after surgery, cannot know it will occur before surgery
§ Result in loss of respiratory muscles -> euthanasia
3) Post-surgical
§ Destabilisation -

80
Q

Disk protrusion how common, what bred and symptoms and signs

A
  • RARE
  • Mainly large breed dogs
    ○ German shepherd dogs, Retrievers…
    ○ do not forget that 90% of disc diseases in large breed dogs are extrusions!!!…
  • Symptoms and signs
    ○ Chronic
    § Except “extrusion on protrusion”
    ○ Less severe
81
Q

Disk protrusion diagnostic modalities used

A

○ Radiographs
§ Clue = Arthritic changes
○ Myelography? no! -> chronic changes (dying axons, toxins can kill other axons - potential to result in paralysis when wake up)
○ MRI > CT-scan
§ Better assessment of the disk
○ Genetic test for Degenerative Myelopathy

82
Q

Disk protusion treatment options

A

1) Medical
§ Pain relief + physiotherapy (hydrotherapy is good)
2) Surgical - hemilaminectomy (thoraco-lumbar disks) +/- fenestrations
§ Not so easy
§ Adherent disk
§ Multiple disks
§ Post-operative deterioration and long recoveries

83
Q

Acute non-compressive nucleus pulposus extrusion what is it, Diagnose, differential and outcome

A
  • Extrusion of non-degenerate disk material -> move around the vertebral
    ○ NO compression - NON SURGICAL CONDITION
  • MRI diagnosis - ONLY ONE TO DIAGNOSIS
    ○ Disk changes
    ○ No compression
  • Differential with
    ○ Fibro Cartilagineous Embolism
  • Fair to good outcome - just rest is needed
84
Q

Caudal cervical malformation syndrome what also called and pathophysiology 2 main types in different signalments

A
  • Wobbler syndrome
  • Pathophysiology
    1. In younger giant breed dogs
    § Great Dane, Basset Hound, Mastiffs…
    § Dorsal/dorso-lateral bone proliferation
    § Nutritional? - unsure of the exact cause
    2. In older large breed dogs
    § Dobermann Pinscher, Dalmatian…
    § Malformation (vertebral columns)/instability (in caudal vertebral column) -> ventral compression
    □ Vertebral bodies - schistocytes sticking into veretbral columns
    □ Ligaments - dorsal ventral ligament
    □ Disk - fibrotic (Hansen II disc)
85
Q

Caudal cervical malformation syndrome clinical signs

A

○ Chronic
○ Cervical spinal cord lesion
§ Thoracic limbs = UMN or LMN
§ Supra scapular muscle atrophy
§ Two engine gait -> LMN in front (paresis - short chopping gait) ataxia in both, UMN in hindlegs
□ Can also get internal rotation of front legs
§ Thoracic limbs spared at the beginning

86
Q

Caudal cervical malformation syndrome diagnosis and treatment with outcome

A 
- Diagnosis
○ Myelo-, CT or MRI (best) 
§ Flexion/extension views? No!
§ Traction-responsive lesions 
□ When add traction to the dogs neck compression changes -> more and less compression 
- Treatment 
1. Medical
§ Poor long term outcome - surgery is better
2. Surgical
§ Traction responsive
□ Distraction-fusion
§ Non traction responsive
□ Ventral slot
§ Good short term outcome, but…
□ mean survival time 18 months (poor quality of life at the end) 
□ Domino effect -> even if fix the one side the other side is likely to cause an issue later
87
Q

Degenerative lumbo-sacral stenosis pathophysiology and breed

A
  • Pathophysiology
    ○ Malformation-instability of L-S (lumbosacral) junction
    § Ventral discal compression - type II disc
    § Lateral (radicular) discal compression
    § Dorsal bony compression - osteophytes
  • Older large breed dogs
88
Q

Degenerative lumbo-sacral stenosis signs and symptoms and diagnosis

A 
- Symptoms and signs
○ ALWAYS AMBULATORY - no spinal cord at this point just nerve roots 
○ Lameness
○ Back pain
○ Muscular atrophy
○ Hyporeflexia (flexion)
○ Incontinence - rare 
- Diagnosis
○ Radiographs
○ CT and MRI - Limitation!!
○ Electrophysiology
89
Q

Degenerative lumbo-sacral stenosis treatment and outcomes

A 
1. Medical
§ Strict rest
§ Guarded long term prognosis
2. Surgical  - best option 
§ Dorsal laminectomy, foraminotomy (create a greater intervertebral foramen to free the nerve roots), facetectomy
□ Highly specialised 
§ ± stabilisation
§ Fair prognosis
90
Q

Other spinal cord diseases

A

1) degenerative myelopathy
2) vertebral malformation
- hemivertebra
- spina bifida
- atlanto-axial instability
- syringomyelia/caudal occipital malformation syndrome (COMS)
3) spinal tumours
4) Discospondylitis
5) Steroid-responsive meningitis-arteritis
6) Fibro-cartilagineous embolism

91
Q

Degenerative myelopathy pathophysiology and signalment

A 
- Pathophysiology?
○ UMN Axonal loss - loss of white matter in the tracts 
○ Unsure on the cause 
§ Vascular supply?
§ Vit B12/E levels?
§ Degeneration of brain neurons?
- Signalment
○ Inheritance suspected
§ German Shepherd, Boxer, Pembroke Welsh Corgi, Rodhesian Ridgeback, Chesapeake Bay Retriever
○ Acquired? -> also see in other breeds 
○ Adults >5y
92
Q

Degenerative myelopathy signs

A 
○ Progressive: 12 to 36m
○ Hind limbs ataxia and paraparesis
§ UMN, then LMN - progressive 
○ then thoracic limbs
○ then cranial nerves
93
Q

Degenerative myelopathy diagnosis and treatment

A
  • Diagnosis
    ○ Rule out other conditions - CANNOT SEE THE CHANGES IN THE SPINAL CORD
    § Type II disk disease
    § Tumours
    ○ Genetic test - Homozygous for SOD-1 mutation
  • No treatment
    ○ Physiotherapy
94
Q

Hemivertebra what does it cause, where located and bred and secondary changes from chronic compression

A 
vertebral malformation 
Screw tail” breeds
§ Bulldogs, Pugs…
§ T8
○ Secondary changes from chronic compression 
§ Progressive spinal cord atrophy - paralysis in hindlimbs 
§ Syringomyelia
§ Sub-arachnoid cysts
95
Q

Spina bifida what is it, associated with and breeds

A 
○ Open dorsal aspect of vertebral canal, often lumbar
○ Association: sacro-caudal dysgenesis
§ Spina bifida
§ A-/dys-genesis of coccygeal vertebras
§ ± meningo-/myelomeningocoele
§ English Bulldog, Manx
96
Q

Atlanto-axial instability what is it, breeds, leads to, clinical signs, diagnosis and treatment

A

vertebral malformation
○ Small breed dogs - acquired (tumour), congenital (abnormal C2)
○ Aplasia, hypoplasia or fracture of the dens (C1-C2)
§ Dens move into spinal cord - compression
○ C1-C5 signs clinical signs - intermittent (not always unstable)
○ MRI, CT > Radiographs, stressed views
○ Neck brace or surgical stabilization (stabilise the joint)

97
Q

Syringomyelia/Caudal occipital malformation syndrome = COMS pathogenesis and breed

A

○ Pathogenesis
i. Overcrowding of the caudal fossa - too much brain tissue in too small skull
ii. Caudal cerebellar herniation (Vermis pushing out) through the occipital foramen
iii. Impairment of CSF flow
iv. Syrinx around C2 and caudal (syringomyelia)
□ Fluid filled pouch within the cervical spinal cord
○ Small breed dogs
§ Cavalier King Charles Spaniel
§ Griffon Bruxellois

98
Q

Syringomyelia/Caudal occipital malformation syndrome = COMS signs and symptoms which most common

A 
§ Scratching (ears, shoulders) (65%)
§ Neck pain (57%) - NECK PAIN IN 
§ Scoliosis (spine twisting) (13%) - due to muscle atrophy - if grey matter is impaired (axons compromised) 
§ Hindlimbs ataxia (22%) - NOT COMMON 
§ Forelimbs ataxia (17%)
99
Q

Syringomyelia/Caudal occipital malformation syndrome = COMS treatment, outcome and prevention

A

○ Treatment
§ Gabapentin, tramadol, corticosteroids
§ Surgical - foramen magnum decompression
○ Outcome
§ Generally can survive a few years
○ Prevention and MRI screening
§ Selection of breeding for larger skulls
§ ALL cavalier kind charles spaniel malformed in their skull - have COMBS may not all develop clinical signs

100
Q

Spinal cord tumours distrubution, age generally occurs, clinical signs, diagnosis and outcome

A 
- Distribution
○ 48% extradural - outside the meninges 
○ 13% intradural/extramedullary
○ 33% intramedullary
- Older patients
○ Exceptions
§ Lymphoma of middle aged cats
§ Nephroblastoma of young dogs
- Clinical signs
○ Slowly progressive
- Diagnosis
○ MRI>CT
○ CSF tap?
○ Biopsy
○ Staging
§ Cat’s lymphoma: abdominal organs and bone marrow
- Outcome  - MOSTLY BAD

DVM 3 - 2 (40 decks)

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