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Earl Karyl F. Galvez
PCGH Level 1 Resident
Atrial fibrillation
OBJECTIVES
Review the risk factors for atrial fibrillation
Understand the guidelines for anticoagulation
and other pharmacologic drugs where there is
latitude for physician decision making
Be able to determine when patients should be
evaluated for curative ablation versus treatment
with medical therapy
Clinical Case
General Data
●C.R.B.
●53 years old
●male
●Married
●Filipino
●Pasig City
●Pasig City General Hospital 7/30/2023.
Chief Complaint
Difficulty of Breathing
History of Present Illness
DOB
Dyspnea on
exertion
Few
hours
Consult
DOB
DYSPNEA ON
EXERTION
PALPITATION
3 day
1 week
Past Medical History
UNREMARKABLE
Illness Previous
Hospitalization
s, Accidents,
Surgeries
NONE
Allergies and
Blood
Transfusion
NONE
MEDICATION
UNREMARKABLE
Family History
● Both parents: With HISTORY OF DM, HTN, CAD
● No other heredofamilial diseases
Personal and Social History
➔ Highschool student
➔ Company employee
➔ Non Smoker
➔ Non-alcoholic beverage drinker.
Review of Systems
General
HEENT
(-) weight loss (-) fever (-) chills (-) loss of appetite (-) malaise
(-) Dizziness (-) eye pain (-) blurring of vision (-) diplopia
(-) ear discharge (-) tinnitus (-)epistaxis (-) hoarseness (-) lacrimation
Respiratory
(-) hemoptysis (-) back pain (-) orthopnea (-) difficulty of breathing
(-) cough (-) sputum production
Cardiovascular
(-) edema (-) cyanosis (-) syncope (-) paroxysmal nocturnal dyspnea
(-) palpitation (-) chest pain,
Gastrointestinal
(-) dysphagia (-) diarrhea (-) hematochezia (-) melena (-) dysphagia
(-) hematemesis (-) abdominal enlargement (-) loose stool
(-) abdominal pain
Review of Systems
Genitourinary
Musculoskeletal
(-) incontinence (-) discharge
(-) edema (-) swelling of joints (-) stiffness (-) numbness
(-) muscle pain (-) muscle weakness (-) muscular atrophy
Neuropsychiatric
(-) loss of consciousness (-) paralysis (-) numbness (-) paresthesia (-
) speech disorder (-) tremors (-) depression
Endocrine (-) intolerance to heat and cold (-) abnormal growth
Hematopoietic (-) bleeding (-) easy bruising (-) pallor
Physical Examination
Findings
General Survey Patient is awake, conscious, coherent and cooperative. The patient is properly groomed, and with no visible gross
deformities. No visible involuntary movements
Vital Signs and
Anthropometric
Measurement
BP=130/80
PR=164
RR=23
Temp=36.6
O2sat = 98% room air
Weight = 50 kg
Height = 5ff
Waist: 34 inches (86.36 cm)
BMI 23 (normal)
HEENT Anicteric Sclerae, (-) Tonsillopharyngeal Congestion, moist lips, moist buccal mucosa, Pale palpebral
conjunctivae
(-) Naso-Aural Discharge, (-) Cervical Lymphadenopathy
Chest & Lungs (-) Retractions, (-) Chest Lag, Clear Breath Sounds
Cardiovascular Adynamic precordium, No Heaves, No Thrills, Irregular Rate and Rhythm,
Abdomen Globular, No striae, No spider angioma, Normoactive Bowel Sounds, Non tender, (-) Shifting dullness test, (-)
Fluid wave test
Physical Examination
Findings
Genitourinary N/A
Extremities No Cyanosis, No Bony deformities, No redness, bulging and depression. No Muscular atrophy.
Capillary Refill Time <2s
Physical Examination
Neurologic Findings
Cerebrum Patient is conscious, coherent, alert, cooperative with intact remote, recent and immediate memory. Oriented to
time, person and place.
Cranial Nerves I
II, III
III, IV, VI
V
VII
VIII
IX, X
XI
XII
Not assessed
Pupils are 2mm wide, equally reactive to direct and consensual lighting
Intact and full extraocular movements. No nystagmus
Intact V1-V3. Can clench both temporalis and masseter muscles. Intact Corneal reflex
Able to demonstrate different facial expressions such as by raising eyebrows, open and closing eyes,
frown, smile, wrinkle forehead, pout, purse lip, and puffing of cheeks.
Able to hear and relay whispered words on both ears.
Uvula in midline. Palate symmetrically rising. Intact Gag reflex
Able to shrug shoulders and rotate the head against resistance.
Tongue at midline moves with ease upon retraction and protrusion, can move from side to side
Cerebellum Able to do finger to nose test. Able to do alternate and supination movement of the hand to thigh.
Sensory
Function
100% on both left and right upper extremities,
Able to distinguish sharp sensation and dull sensation on bilateral lower extremities
Physical Examination
Neurologic Findings
Motor Function Muscle strength is 5/5 on lower extremities and 5/5 on upper extremities
Reflexes Biceps = +2
Triceps = +2
Babinski sign: Negative
Meningeal Negative for nuchal rigidity, Negative for Brudzinski sign and Negative for Kernig's sign.
Sensory
100% 100%
100% 100%
Motor
5/5 5/5
5/5 5/5
DTR
++ ++
++ ++
Salient Features
DOB
Dyspnea on exertion
Palpitation
CR: 164
RR: 23
Irregular Rate and Rhythm
Diet: Food rich in Oil
and fats / fast food
Both parents: Diabetic
and HTN
Primary Working Impression
Atrial Fibrillation In RVR
Differential Diagnosis
Reason for ruling in Reason for ruling out
Hyperthyrodism Palpitation
Tachycardia
Tachypnea
FATIGUE
HEAT INTOLERANCE
SEXUAL DYSFUNCTION
PROTRUDING EYES
Differential Diagnosis
Reason for ruling in Reason for ruling out
CHF DOB
PALPITATION
DYSPNEA ON
EXERTION
AGE: 53
BIPEDAL EDEMA
CHEST PAIN
COUGH
SOB
Differential Diagnosis
Reason for ruling in Reason for ruling out
COPD DOB
ORTHOPNEA ON
EXERTION
NO HISTORY OF
ASTHMA/COPD
NO COUGH
NON SMOKER
21
ER LEVEL
22
SUBJECTIVE OBJECTIVE DIAGNOSTIC
(+) DOB
(+)Palpitation
(+) DYSPNEA ON EXERTION
(-) DOB
(-) Chest pain
(-) Cough
AS Paled Conjuctiva
Irregular Rate and Rhythm
SCE (-) Crackles, (-) rales
Globular abdomen, Non
tender, (-) no direct/indirect
tenderness nor rovsing sign
noted
GNE (-) cyanosis and edema
Vital signs
Bp 130/80
CR 164
RR 23
T 36.6
O2 sat 99 room air
CBC pc, Serum electrolytes
BUN, CREA, ASL, ALT
CBG---143mg/DL
UA
CXR
ECG 12 lead
FBS, lipid profile
Na, k, Mg
Trop I
2decho with DS
23
CBC 7/27/23
HGB 157
HCT 0.47
PLT 154
WBC 7.9
N 0.60
L 0.15
Chemistry 7/27/23
BUN 5.77
CREA 129
Na 132
K 3.9
MG ----
CA ----
Cl ----
ASL 198
ALT 261
U/A
Color yellow
PH TURBID
SG 1.025
PUS 20-30
RBC 3-5
Ketone +3
Albumin +1
Sugar Negative
Trop I 133.5
24
- Cardiomegaly
Chest X-RAY
25
ECG
26
ECG
27
ECG
31
PLAN
IVF: PNSS 1L x 80cc/hr----Heplock
DIET: Low Salt, Low Fat
1. Aspirin 80mg tab OD
2. Clopidogrel 75mg tab OD
3. Enoxaparin 0.6cc Sq BID
4. Lactulose 30cc ODHS
5. Atorvastation 80mg tablet ODHS
6. Carvedilol 6.25mg tablet ½ tablet BID—Metropolol 50g tablet OD
7. Captopril 25mg tablet ¼ tablet BID
8. Spirolactone 25mg tablet OD
32
Discussi
on
Atrial fibrillation (AF) is the most common sustained
arrhythmia encountered in clinical practice.
It accounts for 1/3 of hospital admissions for cardiac rhythm
disturbances.
AF is a global epidemic and has adverse effects on long term
morbidity and mortality.
There is a significant difference in the incidence of AF in
various populations.
Studies reported a lower incidence of AF in Indian , Asians and
African Americans as compared with White populations.
8 Jun 2020https://doi.org/10.1161/CIRCRESAHA.120.316340Circulation Research. 2020;127:4–20
The worldwide age-adjusted prevalence of AF is estimated at
0.596% in men and 0.373% in women ,a total of 33 million.
Studies from India have shown that the mean age of patients
with AF is nearly a decade younger than the Western cohort.
The commonest underlying etiology in Indian patients with AF
in the IHRS-AF registry was also reported to be RHD in 47.8%.
Studies from India reported that RHD was present in nearly 61%
to 75% of AF patients below 50years of age.
A study by Rao et al further observed that hypertension and
ischemic heart disease was more frequent after 50 years of age.
8 Jun 2020https://doi.org/10.1161/CIRCRESAHA.120.316340Circulation Research. 2020;127:4–20
The prevalence of AF varies with the complexity of rheumatic heart disease in Indian
population study :
16% with isolated MR.
29% with MS.
52% with coexisting MR and MS.
70% with mixed mitral and tricuspid valve disease.
8 Jun 2020https://doi.org/10.1161/CIRCRESAHA.120.316340Circulation Research. 2020;127:4–20
ESC guidelines 2012 defined VALVULAR AF as rheumatic valvular
disease (predominantly mitral stenosis) or prosthetic heart valves.
2014 AHA/ACC/ HRS guidelines defined non-valvular AF as AF in the absence of rheumatic
mitral stenosis or a mechanical heart valve, but added bioprosthetic heart valves or mitral
valve repair within the “valvular heart disease” group.
LONE and “IDIOPATHIC” AF generally refer to younger AF patients who have no clinical or
echo evidence of cardiopulmonary disease, hypertension, or diabetes mellitus.
LONE/IDIOPATHIC : However, this categorization is being abandoned since the category of
lone AF no longer has mechanistic or clinical utility.
Similarly, the term “chronic AF” has variable definitions and should not
be used to describe populations of patients with AF.
Mechanism of Atrial Fibrillation
Two concepts of the underlying mechanism of AF :
• Factors that trigger AF.
• Factors that maintain the arrhythmia.
In general, patients with frequent, self-terminating episodes of AF
are likely to have a predominance of factors that trigger AF.
Whereas patients with AF that does not terminate spontaneously
are more likely to have a predominance of perpetuating factors.
TRIGGERS
AF triggering factors include
Sympathetic or parasympathetic stimulation.
Bradycardia
PACs - This may be the most common cause
Atrial flutter
Supraventricular tachycardias
Acute atrial stretch
Catheter ablation of the initiating PACs or SVT can be curative in such patients.
PV TRIGGERS Triggering foci of rapidly firing cells within the sleeves of
atrial myocytes extending into the pulmonary veins is the underlying
mechanism in most cases of PAROXYSMAL AF
90% of AF triggering foci that are mapped during EP studies in patients
with PAROXYSMAL AF occur in the PVs
NON-PV TRIGGERS foci within the SVC, small muscle bundles in the
ligament of Marshall, and the musculature of the CS have been identified
The BASIC Concept is that the site of origin is often within a venous
structure that connects to the atrium
Mechanism of Maintenance of Atrial Fibrillation
Multiple wave re entry hypothesis : AF is sustained by multiple
randomly wandering wavelets in both atria that collide with each other and
extinguish themselves or create new, daughter wavelets that continually re excite
the atria and perpetuate the arrhythmia.
It has been suggested that at least four to six independent wavelets are required to maintain AF.
Localized source hypothesis : This hypothesis suggests that AF
is intermittently maintained by a small number of localized (spatially
stable) high-frequency sources with periods of self-sustaining
disorganization.Rotors and focal sources exhibit 1 : 1 activation within their
spatial domain, with peripheral disorganization.
VAGALLY MEDIATED AF : In some patients with structurally normal hearts, AF is precipitated
during conditions of high-parasympathetic tone, such as during sleep and following meals.
Avoidance of drugs, such as digoxin, that enhance parasympathetic tone has been suggested in
these patients.
ADRENERGIC MEDIATED AF : Adrenergic stimulation, such as that during exercise, can also
provoke AF in some patients by causing Triggered activity.
Adrenergic system causes excess intracellular Ca+2 and trigger automaticity.
The Pathophysiological Triangle in Atrial Fibrillation
Unmodifiable Risk Factors
Age : The prevalence of AF increases with advancing age.
AF occurs in less than 1% of individuals younger than 60 years
6% of those older than 65 years
In more than 10% of those older than 80 years.
Unmodifiable Risk Factors
• Gender. The age-adjusted annual incidence of AF is higher in men
compared with women (3.8 vs. 1.6 per 1000 person-years).
• Race. The age-adjusted risk of developing AF is higher in whites as
compared to blacks, Asians, and Hispanics.
RISK
FACTORS
FOR AF
RISK
FACTORS
FOR AF
RISK
FACTORS
FOR AF
CLINICAL
SYMPTOMS
OF AF
CLINICAL
SYMPTOMS
OF AF
TREATMENT
87
Ward Level
88
SUBJECTIVE OBJECTIVE DIAGNOSTIC
(+) PALPITATION
(-) DOB
(-) ORTHOPNEA
(-) chest pain
(-) Fever
AS Pale Palpebral Conjunctiva
(+) IRREGULARR RATE AND
RHYTHM
SCE (-) Crackles, (-) rales
Globular abdomen, no Epigastric
tenderness, (-) no direct/indirect
tenderness nor rovsing sign noted
GNE (-) cyanosis and edema
Vital signs
Bp 110/70
CR 122
RR 22
T 36.6
O2 sat 97 room air
PT PTT INR
2DECHO WITH DS
SERUM NA K AND MG
ECG 12 LEAD MONITORING Q6
89
Problems:
1.AF in RVR
2.ACS NSTEMI
90
PLAN
Diet: LSLF
IVF: HEPLOCK
ECG 12 LEAD MONITORING Q6
VS q 4
I&O Q shift
Medication:
1. ASA 80MG TAB OD
2. CLOPIDOGREL 75MG TAB OD
3. ENOXAPARIN 0.6CC SQ TO COMPLETE 5 DAYS
4. ATORVASTATIN 40MG TAB ODHS
5. LACTULOSE 30CC ODHS
6. OMEPRAZOLE 40MG CAP OD
7. METROPOLOL 25MG TABLET OD
97
DISCHARGE PLANNING
Home Medication:
1. METROPOLOL 25MG TABLET OD
2. CLOPIDOGREL 75MG TABLET OD
3. ATORVASTATIN 40MG
FOR CONSULTATION TO PHC FOR ASSESSMENT AND FUTHER
WORKUP
FF UP AT IM OPD AFTER 2 WEEKS
98
MGH
Final Diagnosis
ATRIAL FIBRILLATION IN CVR
99
22/Female + Type I DM
100
Epigastric tenderness
Vomiting
Dizzines
tachycardic
Tachypneic
Dry lips
Pale conjuctiva
History of DM since 9 yrs
old
History of Hospitalization
Both parents: Diabetic
On keto diet
Glucose Utilization(muscle
Gluconeogenesis
Glycogenolysis
Ketogenesis Free fatty Acids
Hyperglycemia Metabolic Acidosis
101
Hyperglycemia Ketogenesis
Glucosuria
Ketoacidosis
Ketonuria
Dehydration
Admission
Take Home Message
• DKA is a life-threatening complication of diabetes mellitus
• Fluid therapy and insulin remains the key factors for
managing DKA and frequent monitoring is essential
• DKA can be prevented through patient education and
adherence to medication
References:
1.https://www.ahajournals.org/doi/10.1161/CIRCRESA
HA.120.316340
103
THANK YOU

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Risk Factors and Treatment Guidelines for Atrial Fibrillation

  • 1. Earl Karyl F. Galvez PCGH Level 1 Resident Atrial fibrillation
  • 2. OBJECTIVES Review the risk factors for atrial fibrillation Understand the guidelines for anticoagulation and other pharmacologic drugs where there is latitude for physician decision making Be able to determine when patients should be evaluated for curative ablation versus treatment with medical therapy
  • 4. General Data ●C.R.B. ●53 years old ●male ●Married ●Filipino ●Pasig City ●Pasig City General Hospital 7/30/2023.
  • 6. History of Present Illness DOB Dyspnea on exertion Few hours Consult DOB DYSPNEA ON EXERTION PALPITATION 3 day 1 week
  • 7. Past Medical History UNREMARKABLE Illness Previous Hospitalization s, Accidents, Surgeries NONE Allergies and Blood Transfusion NONE MEDICATION UNREMARKABLE
  • 8. Family History ● Both parents: With HISTORY OF DM, HTN, CAD ● No other heredofamilial diseases
  • 9. Personal and Social History ➔ Highschool student ➔ Company employee ➔ Non Smoker ➔ Non-alcoholic beverage drinker.
  • 10. Review of Systems General HEENT (-) weight loss (-) fever (-) chills (-) loss of appetite (-) malaise (-) Dizziness (-) eye pain (-) blurring of vision (-) diplopia (-) ear discharge (-) tinnitus (-)epistaxis (-) hoarseness (-) lacrimation Respiratory (-) hemoptysis (-) back pain (-) orthopnea (-) difficulty of breathing (-) cough (-) sputum production Cardiovascular (-) edema (-) cyanosis (-) syncope (-) paroxysmal nocturnal dyspnea (-) palpitation (-) chest pain, Gastrointestinal (-) dysphagia (-) diarrhea (-) hematochezia (-) melena (-) dysphagia (-) hematemesis (-) abdominal enlargement (-) loose stool (-) abdominal pain
  • 11. Review of Systems Genitourinary Musculoskeletal (-) incontinence (-) discharge (-) edema (-) swelling of joints (-) stiffness (-) numbness (-) muscle pain (-) muscle weakness (-) muscular atrophy Neuropsychiatric (-) loss of consciousness (-) paralysis (-) numbness (-) paresthesia (- ) speech disorder (-) tremors (-) depression Endocrine (-) intolerance to heat and cold (-) abnormal growth Hematopoietic (-) bleeding (-) easy bruising (-) pallor
  • 12. Physical Examination Findings General Survey Patient is awake, conscious, coherent and cooperative. The patient is properly groomed, and with no visible gross deformities. No visible involuntary movements Vital Signs and Anthropometric Measurement BP=130/80 PR=164 RR=23 Temp=36.6 O2sat = 98% room air Weight = 50 kg Height = 5ff Waist: 34 inches (86.36 cm) BMI 23 (normal) HEENT Anicteric Sclerae, (-) Tonsillopharyngeal Congestion, moist lips, moist buccal mucosa, Pale palpebral conjunctivae (-) Naso-Aural Discharge, (-) Cervical Lymphadenopathy Chest & Lungs (-) Retractions, (-) Chest Lag, Clear Breath Sounds Cardiovascular Adynamic precordium, No Heaves, No Thrills, Irregular Rate and Rhythm, Abdomen Globular, No striae, No spider angioma, Normoactive Bowel Sounds, Non tender, (-) Shifting dullness test, (-) Fluid wave test
  • 13. Physical Examination Findings Genitourinary N/A Extremities No Cyanosis, No Bony deformities, No redness, bulging and depression. No Muscular atrophy. Capillary Refill Time <2s
  • 14. Physical Examination Neurologic Findings Cerebrum Patient is conscious, coherent, alert, cooperative with intact remote, recent and immediate memory. Oriented to time, person and place. Cranial Nerves I II, III III, IV, VI V VII VIII IX, X XI XII Not assessed Pupils are 2mm wide, equally reactive to direct and consensual lighting Intact and full extraocular movements. No nystagmus Intact V1-V3. Can clench both temporalis and masseter muscles. Intact Corneal reflex Able to demonstrate different facial expressions such as by raising eyebrows, open and closing eyes, frown, smile, wrinkle forehead, pout, purse lip, and puffing of cheeks. Able to hear and relay whispered words on both ears. Uvula in midline. Palate symmetrically rising. Intact Gag reflex Able to shrug shoulders and rotate the head against resistance. Tongue at midline moves with ease upon retraction and protrusion, can move from side to side Cerebellum Able to do finger to nose test. Able to do alternate and supination movement of the hand to thigh. Sensory Function 100% on both left and right upper extremities, Able to distinguish sharp sensation and dull sensation on bilateral lower extremities
  • 15. Physical Examination Neurologic Findings Motor Function Muscle strength is 5/5 on lower extremities and 5/5 on upper extremities Reflexes Biceps = +2 Triceps = +2 Babinski sign: Negative Meningeal Negative for nuchal rigidity, Negative for Brudzinski sign and Negative for Kernig's sign. Sensory 100% 100% 100% 100% Motor 5/5 5/5 5/5 5/5 DTR ++ ++ ++ ++
  • 16. Salient Features DOB Dyspnea on exertion Palpitation CR: 164 RR: 23 Irregular Rate and Rhythm Diet: Food rich in Oil and fats / fast food Both parents: Diabetic and HTN
  • 17. Primary Working Impression Atrial Fibrillation In RVR
  • 18. Differential Diagnosis Reason for ruling in Reason for ruling out Hyperthyrodism Palpitation Tachycardia Tachypnea FATIGUE HEAT INTOLERANCE SEXUAL DYSFUNCTION PROTRUDING EYES
  • 19. Differential Diagnosis Reason for ruling in Reason for ruling out CHF DOB PALPITATION DYSPNEA ON EXERTION AGE: 53 BIPEDAL EDEMA CHEST PAIN COUGH SOB
  • 20. Differential Diagnosis Reason for ruling in Reason for ruling out COPD DOB ORTHOPNEA ON EXERTION NO HISTORY OF ASTHMA/COPD NO COUGH NON SMOKER
  • 22. 22 SUBJECTIVE OBJECTIVE DIAGNOSTIC (+) DOB (+)Palpitation (+) DYSPNEA ON EXERTION (-) DOB (-) Chest pain (-) Cough AS Paled Conjuctiva Irregular Rate and Rhythm SCE (-) Crackles, (-) rales Globular abdomen, Non tender, (-) no direct/indirect tenderness nor rovsing sign noted GNE (-) cyanosis and edema Vital signs Bp 130/80 CR 164 RR 23 T 36.6 O2 sat 99 room air CBC pc, Serum electrolytes BUN, CREA, ASL, ALT CBG---143mg/DL UA CXR ECG 12 lead FBS, lipid profile Na, k, Mg Trop I 2decho with DS
  • 23. 23 CBC 7/27/23 HGB 157 HCT 0.47 PLT 154 WBC 7.9 N 0.60 L 0.15 Chemistry 7/27/23 BUN 5.77 CREA 129 Na 132 K 3.9 MG ---- CA ---- Cl ---- ASL 198 ALT 261 U/A Color yellow PH TURBID SG 1.025 PUS 20-30 RBC 3-5 Ketone +3 Albumin +1 Sugar Negative Trop I 133.5
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  • 31. 31 PLAN IVF: PNSS 1L x 80cc/hr----Heplock DIET: Low Salt, Low Fat 1. Aspirin 80mg tab OD 2. Clopidogrel 75mg tab OD 3. Enoxaparin 0.6cc Sq BID 4. Lactulose 30cc ODHS 5. Atorvastation 80mg tablet ODHS 6. Carvedilol 6.25mg tablet ½ tablet BID—Metropolol 50g tablet OD 7. Captopril 25mg tablet ¼ tablet BID 8. Spirolactone 25mg tablet OD
  • 33. Atrial fibrillation (AF) is the most common sustained arrhythmia encountered in clinical practice. It accounts for 1/3 of hospital admissions for cardiac rhythm disturbances. AF is a global epidemic and has adverse effects on long term morbidity and mortality. There is a significant difference in the incidence of AF in various populations. Studies reported a lower incidence of AF in Indian , Asians and African Americans as compared with White populations. 8 Jun 2020https://doi.org/10.1161/CIRCRESAHA.120.316340Circulation Research. 2020;127:4–20
  • 34. The worldwide age-adjusted prevalence of AF is estimated at 0.596% in men and 0.373% in women ,a total of 33 million. Studies from India have shown that the mean age of patients with AF is nearly a decade younger than the Western cohort. The commonest underlying etiology in Indian patients with AF in the IHRS-AF registry was also reported to be RHD in 47.8%. Studies from India reported that RHD was present in nearly 61% to 75% of AF patients below 50years of age. A study by Rao et al further observed that hypertension and ischemic heart disease was more frequent after 50 years of age. 8 Jun 2020https://doi.org/10.1161/CIRCRESAHA.120.316340Circulation Research. 2020;127:4–20
  • 35. The prevalence of AF varies with the complexity of rheumatic heart disease in Indian population study : 16% with isolated MR. 29% with MS. 52% with coexisting MR and MS. 70% with mixed mitral and tricuspid valve disease. 8 Jun 2020https://doi.org/10.1161/CIRCRESAHA.120.316340Circulation Research. 2020;127:4–20
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  • 38. ESC guidelines 2012 defined VALVULAR AF as rheumatic valvular disease (predominantly mitral stenosis) or prosthetic heart valves. 2014 AHA/ACC/ HRS guidelines defined non-valvular AF as AF in the absence of rheumatic mitral stenosis or a mechanical heart valve, but added bioprosthetic heart valves or mitral valve repair within the “valvular heart disease” group. LONE and “IDIOPATHIC” AF generally refer to younger AF patients who have no clinical or echo evidence of cardiopulmonary disease, hypertension, or diabetes mellitus. LONE/IDIOPATHIC : However, this categorization is being abandoned since the category of lone AF no longer has mechanistic or clinical utility. Similarly, the term “chronic AF” has variable definitions and should not be used to describe populations of patients with AF.
  • 39. Mechanism of Atrial Fibrillation Two concepts of the underlying mechanism of AF : • Factors that trigger AF. • Factors that maintain the arrhythmia. In general, patients with frequent, self-terminating episodes of AF are likely to have a predominance of factors that trigger AF. Whereas patients with AF that does not terminate spontaneously are more likely to have a predominance of perpetuating factors.
  • 40. TRIGGERS AF triggering factors include Sympathetic or parasympathetic stimulation. Bradycardia PACs - This may be the most common cause Atrial flutter Supraventricular tachycardias Acute atrial stretch Catheter ablation of the initiating PACs or SVT can be curative in such patients.
  • 41. PV TRIGGERS Triggering foci of rapidly firing cells within the sleeves of atrial myocytes extending into the pulmonary veins is the underlying mechanism in most cases of PAROXYSMAL AF 90% of AF triggering foci that are mapped during EP studies in patients with PAROXYSMAL AF occur in the PVs NON-PV TRIGGERS foci within the SVC, small muscle bundles in the ligament of Marshall, and the musculature of the CS have been identified The BASIC Concept is that the site of origin is often within a venous structure that connects to the atrium
  • 42. Mechanism of Maintenance of Atrial Fibrillation Multiple wave re entry hypothesis : AF is sustained by multiple randomly wandering wavelets in both atria that collide with each other and extinguish themselves or create new, daughter wavelets that continually re excite the atria and perpetuate the arrhythmia. It has been suggested that at least four to six independent wavelets are required to maintain AF. Localized source hypothesis : This hypothesis suggests that AF is intermittently maintained by a small number of localized (spatially stable) high-frequency sources with periods of self-sustaining disorganization.Rotors and focal sources exhibit 1 : 1 activation within their spatial domain, with peripheral disorganization.
  • 43. VAGALLY MEDIATED AF : In some patients with structurally normal hearts, AF is precipitated during conditions of high-parasympathetic tone, such as during sleep and following meals. Avoidance of drugs, such as digoxin, that enhance parasympathetic tone has been suggested in these patients. ADRENERGIC MEDIATED AF : Adrenergic stimulation, such as that during exercise, can also provoke AF in some patients by causing Triggered activity. Adrenergic system causes excess intracellular Ca+2 and trigger automaticity.
  • 44. The Pathophysiological Triangle in Atrial Fibrillation
  • 45. Unmodifiable Risk Factors Age : The prevalence of AF increases with advancing age. AF occurs in less than 1% of individuals younger than 60 years 6% of those older than 65 years In more than 10% of those older than 80 years.
  • 46. Unmodifiable Risk Factors • Gender. The age-adjusted annual incidence of AF is higher in men compared with women (3.8 vs. 1.6 per 1000 person-years). • Race. The age-adjusted risk of developing AF is higher in whites as compared to blacks, Asians, and Hispanics.
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  • 88. 88 SUBJECTIVE OBJECTIVE DIAGNOSTIC (+) PALPITATION (-) DOB (-) ORTHOPNEA (-) chest pain (-) Fever AS Pale Palpebral Conjunctiva (+) IRREGULARR RATE AND RHYTHM SCE (-) Crackles, (-) rales Globular abdomen, no Epigastric tenderness, (-) no direct/indirect tenderness nor rovsing sign noted GNE (-) cyanosis and edema Vital signs Bp 110/70 CR 122 RR 22 T 36.6 O2 sat 97 room air PT PTT INR 2DECHO WITH DS SERUM NA K AND MG ECG 12 LEAD MONITORING Q6
  • 90. 90 PLAN Diet: LSLF IVF: HEPLOCK ECG 12 LEAD MONITORING Q6 VS q 4 I&O Q shift Medication: 1. ASA 80MG TAB OD 2. CLOPIDOGREL 75MG TAB OD 3. ENOXAPARIN 0.6CC SQ TO COMPLETE 5 DAYS 4. ATORVASTATIN 40MG TAB ODHS 5. LACTULOSE 30CC ODHS 6. OMEPRAZOLE 40MG CAP OD 7. METROPOLOL 25MG TABLET OD
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  • 97. 97 DISCHARGE PLANNING Home Medication: 1. METROPOLOL 25MG TABLET OD 2. CLOPIDOGREL 75MG TABLET OD 3. ATORVASTATIN 40MG FOR CONSULTATION TO PHC FOR ASSESSMENT AND FUTHER WORKUP FF UP AT IM OPD AFTER 2 WEEKS
  • 100. 22/Female + Type I DM 100 Epigastric tenderness Vomiting Dizzines tachycardic Tachypneic Dry lips Pale conjuctiva History of DM since 9 yrs old History of Hospitalization Both parents: Diabetic On keto diet Glucose Utilization(muscle Gluconeogenesis Glycogenolysis Ketogenesis Free fatty Acids Hyperglycemia Metabolic Acidosis
  • 102. Take Home Message • DKA is a life-threatening complication of diabetes mellitus • Fluid therapy and insulin remains the key factors for managing DKA and frequent monitoring is essential • DKA can be prevented through patient education and adherence to medication