Three main causes of Aortic Stenosis:
1. Congenital bicuspid aortic valve: age 50-60, men>women
2. (Acquired) Calcific aortic stenosis: age 70-80, men=women
3. (Acquired) Rheumatic aortic stenosis: middle-aged women>men, will also have mitral valve disease (note: rheumatic heart disease usually affects mitral, then tricuspid, then aortic in sequence)
Troponins
Troponins are a confirmatory test fo ACS in the setting of a history/clinical picture that suggests ACS. In other settings, it's a marker of myocyte necrosis but completely non-specific. It is only specific for ACS if ordered because the history suggested ACS.
Infective Endocarditis
Strep viridans does not generally cause large vegetations
- Staph and fungal infections cause large vegetations
- ECHO has low sensitivity
Acute versus Chronic Aortic Insufficiency (AI)
1. Chronic AI:
- LV has adapted by eccentric hypertrophy and dilatation to compensate for volume overload
- displaced apex beat
- long, loud, early diastolic decrescendo murmur, best heard at aortic area when the patient is seated and leans forward with breath held in expiration; often goes all the way to S1
- S1 is normal
- Wide pulse pressure, and related signs: waterhammer pulse, Corrigan's pulse, de Musset's sign, Quincke's sign (pulsations in the capillary nail bed), Duroziez's sign (systolic and diastolic murmurs heard over the femoral artery when it is gradually compressed with the stethescope)
2. Acute AI:
- equalization of aortic pressure with LV pressure because LV can't compensate acutely for all the extra volume = diastasis
- Premature S1 that is very soft (the massive reflux of blood from the aorta fills the left ventricle during diastole, increasing LVEDV and filling pressure, and closes the mitral valve prematurely), normal S2
- increased LA pressures leading to pulmonary edema (florid CHF)
- Very quiet and short early diastolic murmur
- Signs of vasoconstricted state, tachycardia, low sBP, dBP and MAP (and low stroke volume)
- pulse pressure not as wide
- Main causes: aortic dissection, aortic valve IE
Wednesday, August 24, 2011
Friday, August 19, 2011
Skin & Soft Tissue Infections
Layers of the Skin & Soft Tissue (out to in) with their corresponding infections:
- Epidermis -> erysipelas
- Dermis -> cellulitis
- Subcutaneous fat -> panniculitis
- Fascia -> fasciitis
- Muscle -> pyomyositis
CLINICAL PEARLS:
1. Differentiating erysipelas versus cellulitis
- Erysipelas has a raised, distinct border
- Cellulitis is less well demarcated
2. Gestalt...
- Red with no pus -> likely Group A Strep
- Red with lots of pus -> likely Staph
3. The number 1 bug for ALL layers is GROUP A STREP.
Number 2 is Staph.
4. Lympangitic streaking can be seen with cellulitis, but not with fasciitis because there is no lymphatic drainage of the fascia.
Recognize sepsis!!
Upon presentation, a patient's chance of dying is 5-10% with an MI, 15% with a stroke, and 50% with sepsis! Yet it remains under-recognized...
Treatment of cellulitis: (to cover both Strep and Staph)
#1 - Cefazolin / Cephalexin (first generation cephalosporins)
- Cloxacillin
- Vanco if suspecting MRSA
- If PCN allergy: Levofloxacin or moxifloxacin
Strep is highly resistant to Septra and Macrolides.
Doxycycline is good for Staph but not so great for GAS.
Click here for the IDSA practice guidelines for the Dx and Rx of SKIN AND SOFT TISSUE INFECTIONS.
- Epidermis -> erysipelas
- Dermis -> cellulitis
- Subcutaneous fat -> panniculitis
- Fascia -> fasciitis
- Muscle -> pyomyositis
CLINICAL PEARLS:
1. Differentiating erysipelas versus cellulitis
- Erysipelas has a raised, distinct border
- Cellulitis is less well demarcated
2. Gestalt...
- Red with no pus -> likely Group A Strep
- Red with lots of pus -> likely Staph
3. The number 1 bug for ALL layers is GROUP A STREP.
Number 2 is Staph.
4. Lympangitic streaking can be seen with cellulitis, but not with fasciitis because there is no lymphatic drainage of the fascia.
Recognize sepsis!!
Upon presentation, a patient's chance of dying is 5-10% with an MI, 15% with a stroke, and 50% with sepsis! Yet it remains under-recognized...
Treatment of cellulitis: (to cover both Strep and Staph)
#1 - Cefazolin / Cephalexin (first generation cephalosporins)
- Cloxacillin
- Vanco if suspecting MRSA
- If PCN allergy: Levofloxacin or moxifloxacin
Strep is highly resistant to Septra and Macrolides.
Doxycycline is good for Staph but not so great for GAS.
Click here for the IDSA practice guidelines for the Dx and Rx of SKIN AND SOFT TISSUE INFECTIONS.
Monday, August 15, 2011
Mumps at Ki Restaurant!!
For all you foodies out there (I am one), note that TPH has reported a mumps outbreak, with 9 cases among employees at a popular Toronto restaurant (a favourite amongst Cardiologists!)..
See link for TPH update:
http://www.toronto.ca/health/cdc/communicable_disease_surveillance/monitoring/pdf/mumps_2011.pdf
MUMPS CLINICAL FEATURES:
Signs and Symptoms:
- viral prodrome (myalgias, anorexia, malaise, headache, and fever)
- unilateral or bilateral parotitis
- respiratory symptoms
Complications:
- meningitis,
- encephalitis,
- orchitis,
- oophoritis,
- pancreatitis
- deafness
Transmission:
- direct contact with respiratory droplets or saliva
- incubation period 12 to 26 days
Diagnostic testing:
- virus isolation/detection from buccal or throat swab + urine collection
- serology (IgM and IgG for mumps)
See link for TPH update:
http://www.toronto.ca/health/cdc/communicable_disease_surveillance/monitoring/pdf/mumps_2011.pdf
MUMPS CLINICAL FEATURES:
Signs and Symptoms:
- viral prodrome (myalgias, anorexia, malaise, headache, and fever)
- unilateral or bilateral parotitis
- respiratory symptoms
Complications:
- meningitis,
- encephalitis,
- orchitis,
- oophoritis,
- pancreatitis
- deafness
Transmission:
- direct contact with respiratory droplets or saliva
- incubation period 12 to 26 days
Diagnostic testing:
- virus isolation/detection from buccal or throat swab + urine collection
- serology (IgM and IgG for mumps)
A classic case of "brain rot"
We had a particularly entertaining Morning Report last Friday where we discussed the case of an elderly woman with subacute onset of memory disturbances, incontinence, ataxia and multiple focal neurologic deficits. Pending brain biopsy, her preliminary diagnosis is ...
HSV ENCEPHALITIS
Click the link below for a review of viral encephalitis:
http://journals1.scholarsportal.info.myaccess.library.utoronto.ca/tmp/10753946288144476016.pdf
("Brain rot" is not a term routinely used to describe HSV encephalitis, but rather was thrown out there by our MR facilitator and I found it somewhat amusing..)
HSV ENCEPHALITIS
Click the link below for a review of viral encephalitis:
http://journals1.scholarsportal.info.myaccess.library.utoronto.ca/tmp/10753946288144476016.pdf
("Brain rot" is not a term routinely used to describe HSV encephalitis, but rather was thrown out there by our MR facilitator and I found it somewhat amusing..)
Tuesday, August 9, 2011
Doctor my back hurts!
Today in Morning Report we reviewed a case of a 60F with acute onset of low back pain.
Remember the Red Flags of Back Pain:
1. Saddle anesthesia
2. Bowel/bladder changes
3. Constitutional symptoms (fever, chills, sweat, anorexia, weight loss)
4. Prior or current history of malignancy
5. Night pain
6. Hx of IVDU
7. Older age> 65 with new onset back pain
Why do we care about these red flags?
- Impending neurologic compromise
- Malignancy
- Abscess
The role of imaging in the management of low back pain: bottom line - in the absence of red flags, imaging for LBP doesn't significantly influence management and is associated with substantial cost.
http://www.ncbi.nlm.nih.gov.myaccess.library.utoronto.ca/pubmed/15031430 (use your UtorID for access)
A systematic review published in the Annals of Internal Medicine in 2004 concluded that in adults < 50 years old with no systemic symptoms (or red flags), symptomatic therapy without imaging is appropriate. In adults > 50 years, or those with systemic symptoms, routine bloodwork and plain radiographs are usually sufficient to rule out underlying systemic disease.
http://www.ncbi.nlm.nih.gov.myaccess.library.utoronto.ca/pubmed/12353946
Friday, August 5, 2011
Aphasia
Today in Morning Report we talked about a woman with acute onset of word-finding difficulties and recognition. Here is simple approach to aphasia:
*Remember: APHASIA = impairment in language. DYSARTHRIA = motor speech problem.
Broca's area and Wernicke's area are the main language areas located in the perisylvian language area, they are joined by the arcuate fasciculus.
*All aphasias have naming problems.
1) Can the patient repeat? (Assess repetition)
- Repeat after me: "no ifs, ands, or buts"
- if yes: perisylvian language area intact, therefore lesion in area around perisylvian language area = transcortical aphasia
- 2) Is the patient able to comprehend? (Assess comprehension, simple commands)
- easy questions: close your eyes, to more difficult: point to your nose with your right hand
- If yes: "Transcortical motor aphasia"
- If no: "Transcortical sensory aphasia"
- if no repetition: lesion within perisylvian language area
- 2) Is the patient able to comprehend?
- If yes: "Broca's aphasia"
- If no: "Wernicke's aphasia"
Summary:
Broca's Aphasia
- can understand, cannot repeat ("patient is frustrated")
- not fluent
Wernicke's Aphasia
- cannot comprehend, cannot repeat
- fluent (but non-sensical speech, not coherent) - word salad ("examiner is frustrated")
Transcortical Motor Aphasia
- like Broca's aphasia but CAN repeat
- usually lesion near Broca's area but not in the perisylvian area (in the frontal cortex)
Transcortical Sensory Aphasia
- like Wernicke's aphasia but CAN repeat
Global Aphasia
- cannot comprehend, cannot repeat, not fluent, cannot read, cannot write (usually mute)
- suggests large lesion affecting both Broca's and Wernicke's areas (ex. Large MCA stroke)
Anomic Aphasia
- difficulty naming but no other deficits
- does not localize
Conduction Aphasia
- cannot repeat, but everything else intact
- lesion in the Arcuate Fasciculus (the fibers that connect Broca's and Wernicke's); the two main areas are intact but the listening and the speaking parts of the brain can't connect
Thursday, August 4, 2011
"Rapid Fire" MR
August 4, 2011 - Today we had "rapid fire" post-call morning report and reviewed several cases from last night. Here are some synopses:
Case 1. 57M mucosal bleeding. PMHx: APLA, ITP with splenectomy. Meds: Prednisone 15mg daily, no warfarin. O/E: petechiae, ecchymosis, cushingoid.
What do you think is causing his bleeding?
Investigations: Plt 285, INR 1.0, PTT 25.7, bleeding time >15s, U/A 2+ blood, creat 78
Does this change your differential diagnosis?
Remember the components of coagulation:
- factors, inhibitors (check via INR, PTT)
- Plt fxn (uremia, antiplt)
- fibrinogen
- vWF/factor 8 deficiency
Disorders of primary hemostasis:
- Acquired: antiplatelet agents (ASA, Plavix), thrombocytopenias (ITP, HIT, TTP), primary bone marrow diseases (myeloproliferative disorders, MDS, plasma cell dyscrasias), severe renal failure (so called "uremic platelets")
- Congenital: vWD, some platelet dysfunction disorders
Disorders of coagulation/fibrinolysis:
- Acquired: liver failure, Vit K deficiency, anticoagulant meds, factor inhibitors, scurvy
- Congenital: coagulation factor deficiencies (hemophilias), antiplasmin deficiency
Initial lab tests:
- CBC, liver enzymes, ABO blood group
- INR, aPTT, if abnormal: consider 1:1 mixing studies
- fibrinogen
- vWF antigen, ristocetin cofactor, factor VIII
- platelet aggregation test
- standardize bleeding time
***
Case 2. 58F 6-weeks post-THR (PMHx: JRA). Recent C. Diff treated with Flagyl, returning with worsening diarrhea, abdo pain.
C. diff recurrence - Definition: complete abatement of C. diff infection symptoms while on appropriate therapy, followed by subsequent reappearance of diarrhea and other symptoms after treatment has been stopped; must distinguish from persistent diarrhea without resolution during initial therapy.
Treatment of C. diff:
Initial episode: Flagyl 500 mg PO TID x 10 to 14 days
Alternative ($$$): Vanco 125 mg PO QID x 10 to 14 days
First relapse: repeat treatment as in initial episode (Flagyl)
Second relapse: tapering course of PO Vanco, +/- probiotics (Saccharomyces boulardii 500 mg orally twice daily).
***
Case 3. 78M from ICU post hypercapneic resp failure due to severe COPD
NB: The traditional teaching of supplemental oxygen decreasing the "drive to breathe" in CO2-retaining COPDers, is incorrect. The current thinking is that therapy with supplemental oxygen alters hypoxic pulmonary vasoconstriction and modulates the Haldane effect (decreased carriage of CO2 by oxyhemoglobin when compared with reduced hemoglobin), resulting in changes in physiologic deadspace and worsening hypercarbia.
Published in:
Hanson, C William III et al. Causes of hypercarbia with oxygen therapy in patients with chronic obstructive pulmonary disease. Crit Care Med 1996; 24(1): 23-28.
***
Case 4. 50F 6-week abdo pain, diarrhea. CT abdo shows: Terminal ileitis.
What is your differential diagnosis?
DDx terminal ileitis:
- Crohns (#1, 2, 3!)
- infectious (especially Yersinia, TB)
- spondyloarthropathies
- vasculitides
- ischemia
- neoplasm
- medication-induced (especially NSAIDS)
- eosinophilic enteritis
Case 1. 57M mucosal bleeding. PMHx: APLA, ITP with splenectomy. Meds: Prednisone 15mg daily, no warfarin. O/E: petechiae, ecchymosis, cushingoid.
What do you think is causing his bleeding?
Investigations: Plt 285, INR 1.0, PTT 25.7, bleeding time >15s, U/A 2+ blood, creat 78
Does this change your differential diagnosis?
Remember the components of coagulation:
- factors, inhibitors (check via INR, PTT)
- Plt fxn (uremia, antiplt)
- fibrinogen
- vWF/factor 8 deficiency
Disorders of primary hemostasis:
- Acquired: antiplatelet agents (ASA, Plavix), thrombocytopenias (ITP, HIT, TTP), primary bone marrow diseases (myeloproliferative disorders, MDS, plasma cell dyscrasias), severe renal failure (so called "uremic platelets")
- Congenital: vWD, some platelet dysfunction disorders
Disorders of coagulation/fibrinolysis:
- Acquired: liver failure, Vit K deficiency, anticoagulant meds, factor inhibitors, scurvy
- Congenital: coagulation factor deficiencies (hemophilias), antiplasmin deficiency
Initial lab tests:
- CBC, liver enzymes, ABO blood group
- INR, aPTT, if abnormal: consider 1:1 mixing studies
- fibrinogen
- vWF antigen, ristocetin cofactor, factor VIII
- platelet aggregation test
- standardize bleeding time
***
Case 2. 58F 6-weeks post-THR (PMHx: JRA). Recent C. Diff treated with Flagyl, returning with worsening diarrhea, abdo pain.
C. diff recurrence - Definition: complete abatement of C. diff infection symptoms while on appropriate therapy, followed by subsequent reappearance of diarrhea and other symptoms after treatment has been stopped; must distinguish from persistent diarrhea without resolution during initial therapy.
Treatment of C. diff:
Initial episode: Flagyl 500 mg PO TID x 10 to 14 days
Alternative ($$$): Vanco 125 mg PO QID x 10 to 14 days
First relapse: repeat treatment as in initial episode (Flagyl)
Second relapse: tapering course of PO Vanco, +/- probiotics (Saccharomyces boulardii 500 mg orally twice daily).
***
Case 3. 78M from ICU post hypercapneic resp failure due to severe COPD
NB: The traditional teaching of supplemental oxygen decreasing the "drive to breathe" in CO2-retaining COPDers, is incorrect. The current thinking is that therapy with supplemental oxygen alters hypoxic pulmonary vasoconstriction and modulates the Haldane effect (decreased carriage of CO2 by oxyhemoglobin when compared with reduced hemoglobin), resulting in changes in physiologic deadspace and worsening hypercarbia.
Published in:
Hanson, C William III et al. Causes of hypercarbia with oxygen therapy in patients with chronic obstructive pulmonary disease. Crit Care Med 1996; 24(1): 23-28.
***
Case 4. 50F 6-week abdo pain, diarrhea. CT abdo shows: Terminal ileitis.
What is your differential diagnosis?
DDx terminal ileitis:
- Crohns (#1, 2, 3!)
- infectious (especially Yersinia, TB)
- spondyloarthropathies
- vasculitides
- ischemia
- neoplasm
- medication-induced (especially NSAIDS)
- eosinophilic enteritis
Wednesday, August 3, 2011
Elevated CK
Rhabdomyolysis August 2nd, 2011 - Morning Report
Definition: the rapid breakdown of striated muscle with subsequent release of cellular contents into the extracellular fluid and circulation.
Fun fact:
First description of Rhabdomyolysis is thought to be in the Book of Numbers (Bible or Torah) after the Israelites ate quail and were poisoned. Scholars believe this to be due to cicutoxin from the Hemlock plant that the quail were believed to feed on.
Elevated CK
- CK-MM muscle
- CK-MB heart
- CK-BB brain
DDx for elevated CK-MM (rhabdo)
1. Crush: compartment syndrome; lying on ground immobile
2. Drugs:(statins - risk significantly increases with co-use of fibrates, ecstasy, heroin, cocaine, neuroleptics - NMS), malignant hyperthermia
3. Ischemia: DVT with compartment syndrome, arterial embolus
4. Exertion: seizure, marathoners, muscle builders (think fit vs non-fit)
5. Inflammatory: polymyositis (personal or famil hx of autoimmune disease?), dermatomyositis (look for an underlying tumor)
6. Infection (especially viruses like EBV, coxsackie), Legionnaire's disease
7. Genetic: most common is McArdle's disease (congenital myophosphorylase deficiency), Tarui disease (phosphofructokinase disease), carnitine deficiency
8. Endocrine: hypo > hyperthyroid
First description of Rhabdomyolysis is thought to be in the Book of Numbers (Bible or Torah) after the Israelites ate quail and were poisoned. Scholars believe this to be due to cicutoxin from the Hemlock plant that the quail were believed to feed on.
Elevated CK
- CK-MM muscle
- CK-MB heart
- CK-BB brain
DDx for elevated CK-MM (rhabdo)
1. Crush: compartment syndrome; lying on ground immobile
2. Drugs:(statins - risk significantly increases with co-use of fibrates, ecstasy, heroin, cocaine, neuroleptics - NMS), malignant hyperthermia
3. Ischemia: DVT with compartment syndrome, arterial embolus
4. Exertion: seizure, marathoners, muscle builders (think fit vs non-fit)
5. Inflammatory: polymyositis (personal or famil hx of autoimmune disease?), dermatomyositis (look for an underlying tumor)
6. Infection (especially viruses like EBV, coxsackie), Legionnaire's disease
7. Genetic: most common is McArdle's disease (congenital myophosphorylase deficiency), Tarui disease (phosphofructokinase disease), carnitine deficiency
8. Endocrine: hypo > hyperthyroid
*The schematic above showing the causes and complications of rhabdomyolysis was taken from the article: Cervellin G, Comelli I, Lippi G. Rhabdomyolysis: historical background, clinical, diagnostic and therapeutic features. Clin Chem Lab Med. 2010 Jun;48(6):749-56.
Clinical features:
Clinical features:
- classic triad: muscle pain, brown pigmented urine (myoglobinuria), weakness seen in <10% of patients
- can be asymptomatic with only elevated CK
- myalgias, pain, pigmented urine, fever, malaise, tachycardia, nausea/vomiting
- AKI can be seen if CK>5000
- complications: renal failure, DIC, and death in ~5% of cases
- urine myoglobin is not useful in diagnosis
- CK is the biochemical gold standard
- other investigations: elevated AST>ALT, LDH, UA
Treatment:
- FLUIDS!
- little support for the use of mannitol, Lasix, or bicarb
- manage the electrolyte derangements (hyperkalemia, hypocalcemia)
- severe hyperkalemia may require dialysis - shifting with insulin may not work if extensive tissue damage led to rhabdo
Moderate-intensity exercise (HR 55-90% max) is enough to elevate CK levels to the mid-thousands, particularly if "eccentric muscle contractions" like weight lifting or running downhill. More info can be found in the article:
Moderate-intensity exercise (HR 55-90% max) is enough to elevate CK levels to the mid-thousands, particularly if "eccentric muscle contractions" like weight lifting or running downhill. More info can be found in the article:
Latham J, Campbell D, Nichols W, Mott T. Clinical inquiries. How much can exercise raise creatine kinase level--and does it matter? J Fam Pract. 2008 Aug;57(8):545-7.
Geripsych Morning Report
This morning we discussed some common geripsych issues...
Form 1
- any physician can fill out within 7 days of seeing a patient
- mandates mental health assessment, can hold patient up to 72 hrs to do this
- mental health assessment does not have to be done by a psychiatrist; can be done by any physician comfortable with this assessment
- if patient deemed unsafe, next steps either: 1) put on Form 3 if involuntary, or 2) patient can stay voluntarily
- rarely use Box B (except psychiatrists who know the patient well because addresses patient's history)
- must give pt the Form 42: notifies the patient of why they're being held and by what authority (otherwise illegal to detain them)
Agitation
- clarify what agitation means and whether it warrants treatment
- treatment responsive versus non-treatment responsive
- treatment non-responsive: example -> wandering doesn't warrant treatment - there's no specific treatment except zonking them out
- treatment responsive: yelling, behavior driven by psychosis, striking/violence
- non-pharmacologic therapy: some "agitated" patients just need something to do like fold towels or stuff envelopes
- pharmacotherapy:
1. Atypical antipsychotics: mainly oral
- Risperidone: highest EPS, least sedating, ex: 0.25 OD or BID
- Olanzapine: most anticholinergic therefore avoid in elderly, mid EPS, mid sedating
- Quetiapine: Lowest EPS, most sedating, causes orthostatic hypotension (huge variation in dose, 6.25-200mg! Start low go slow, first couple days will have sedation)
Here is the Results portion of the article: L.B. Ozbolt; M.A. Paniagua ; R.M. Kaiser Atypical Antipsychotics for the Treatment of Delirious Elders. Journal of the American Medical Directors Association (January 2008), 9 (1), pg. 18-28
"Results: Risperidone, the most thoroughly studied atypical antipsychotic, was found to be approximately 80% to 85% effective in treating the behavioral disturbances of delirium at a dosage of 0.5 to 4 mg daily. Studies of olanzapine indicated that it was approximately 70% to 76% effective in treating delirium at doses of 2.5 to 11.6 mg daily. Very few studies have been conducted using quetiapine; it also appears to be a safe and effective alternative to high-potency antipsychotics. In comparison to haloperidol, the frequency of adverse reactions and side effects was found to be much lower with the use of atypical antipsychotic medications. In the limited number of trials comparing atypical antipsychotics to haloperidol, haloperidol consistently produced a higher rate (an additional 10% to 13%) of extrapyramidal side effects."
2. Typical
- Haldol: can be given po/im so gives you options, most EPS, least anticholinergic (ex 0.5-1mg po q4h prn); NB Haldol iv better for EPS but less safe from cardiac perspective ie long Qt
- Loxapine: slightly sedating, available in liquid form
3. Other
- Trazadone: good for nighttime restlessness
Stimulants in Depression:
- use for depression in the medically ill elderly who are anergic (apathetic) as opposed to sad, ex: flat affect, fatigued, low energy, no interest in eating in patient with no history of depression
- one week to titrate up and if it's going to work you expect it to work quickly within first week
- options: Buproprion or SSRIs
- NB: can use mirtazapine to stimulate appetite but caution because can increase cholesterol
Form 1
- any physician can fill out within 7 days of seeing a patient
- mandates mental health assessment, can hold patient up to 72 hrs to do this
- mental health assessment does not have to be done by a psychiatrist; can be done by any physician comfortable with this assessment
- if patient deemed unsafe, next steps either: 1) put on Form 3 if involuntary, or 2) patient can stay voluntarily
- rarely use Box B (except psychiatrists who know the patient well because addresses patient's history)
- must give pt the Form 42: notifies the patient of why they're being held and by what authority (otherwise illegal to detain them)
Agitation
- clarify what agitation means and whether it warrants treatment
- treatment responsive versus non-treatment responsive
- treatment non-responsive: example -> wandering doesn't warrant treatment - there's no specific treatment except zonking them out
- treatment responsive: yelling, behavior driven by psychosis, striking/violence
- non-pharmacologic therapy: some "agitated" patients just need something to do like fold towels or stuff envelopes
- pharmacotherapy:
1. Atypical antipsychotics: mainly oral
- Risperidone: highest EPS, least sedating, ex: 0.25 OD or BID
- Olanzapine: most anticholinergic therefore avoid in elderly, mid EPS, mid sedating
- Quetiapine: Lowest EPS, most sedating, causes orthostatic hypotension (huge variation in dose, 6.25-200mg! Start low go slow, first couple days will have sedation)
Here is the Results portion of the article: L.B. Ozbolt; M.A. Paniagua ; R.M. Kaiser Atypical Antipsychotics for the Treatment of Delirious Elders. Journal of the American Medical Directors Association (January 2008), 9 (1), pg. 18-28
"Results: Risperidone, the most thoroughly studied atypical antipsychotic, was found to be approximately 80% to 85% effective in treating the behavioral disturbances of delirium at a dosage of 0.5 to 4 mg daily. Studies of olanzapine indicated that it was approximately 70% to 76% effective in treating delirium at doses of 2.5 to 11.6 mg daily. Very few studies have been conducted using quetiapine; it also appears to be a safe and effective alternative to high-potency antipsychotics. In comparison to haloperidol, the frequency of adverse reactions and side effects was found to be much lower with the use of atypical antipsychotic medications. In the limited number of trials comparing atypical antipsychotics to haloperidol, haloperidol consistently produced a higher rate (an additional 10% to 13%) of extrapyramidal side effects."
2. Typical
- Haldol: can be given po/im so gives you options, most EPS, least anticholinergic (ex 0.5-1mg po q4h prn); NB Haldol iv better for EPS but less safe from cardiac perspective ie long Qt
- Loxapine: slightly sedating, available in liquid form
3. Other
- Trazadone: good for nighttime restlessness
Stimulants in Depression:
- use for depression in the medically ill elderly who are anergic (apathetic) as opposed to sad, ex: flat affect, fatigued, low energy, no interest in eating in patient with no history of depression
- one week to titrate up and if it's going to work you expect it to work quickly within first week
- options: Buproprion or SSRIs
- NB: can use mirtazapine to stimulate appetite but caution because can increase cholesterol
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