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Title: ground rand 4


1
HUBERT KAIRUKI MEMORIAL UNIVERSITYDEPARTMENT
OF INTERNAL MEDICINEGRAND ROUND PRESENTATION
  • PRESENTERSFATMA MSUYA,CELESTINA MSUBA,
  • ELIZABETH MSITA,ABDULRAHIM ,MSINDE NELSON
    MSANGI
  • FACILITATORS SR SARA DR NEEMA

2
PATIENT PARTICULARS
  • Name Kidawa .H. Said
  • Age66 years old
  • Sex Female
  • Address Kijitonyama
  • Tribe Kaguru
  • Religion Muslim
  • Marital status Married
  • Next of kin daughter
  • Informant herself
  • Occupation Petty trader
  • Education level grade 4
  • Referral status self from home
  • Date of admission 5th jan,2024 Date of
    clerkship 6th jan, 2024
  • Number of days in the ward 1 days

3
CHIEF COMPLAINT
  • Difficulty in breathing 7days

4
HISTORY OF PRESENTING ILLNESS
  • The patient presented with of DIB for 7 days , of
    gradual onset after being in a dusty environment,
    more marked at night .
  • Aggravated by dust, perfume use and cold.
  • Relieved by use of salbutamol inhaler and resting
    thereafter her DIB was progressive and not
    relieved by use of inhaler(Salbutamol) that she
    used before
  • DIB associated with
  • chest tightness, dry cough, whistling sounds,
  • inability to complete a sentence.
  • central chest pain that does not radiate to the
    jaw, shoulder and back , difficulty in breathing
    when lying flat
  • lower limb swelling
  • Easy fatigability
  • No history of
  • awareness of heartbeat, air hunger at night

5
REVIEW OF THE OTHER SYSTEMS
  • EENT (Ears ,eyes , nose and throat)
  • No ear pain or discharge
  • No eye pain or discharge
  • No nasal pain or discharge
  • No throat pain or swelling
  • Gastrointestinal system
  • No of loss of appetite
  • No weight loss
  • No difficulty in swallowing
  • No painful swallowing
  • No heartburn
  • No abdominal pain
  • No vomiting
  • No passage of lose stools
  • No difficulty in passing stool

6
ROS cont
  • Genitourinary system
  • No genital itching
  • No Excessive urination
  • No painful urination
  • No blood in urine
  • No urine urgency
  • No inability to control urine
  • No blood in urine

7
  • Endocrine system
  • no excessive thirst
  • no excessive sweating
  • no weight loss or gain
  • no cold or heat intolerance
  • no excessive hair growth
  • Nervous system
  • No headache
  • No convulsions
  • No dizziness
  • No loss of consciousness
  • No Numbness or tingling sensation
  • No blurry vision

8
ROS cont
  • Musculoskeletal system
  • No muscle pain, weakness or stiffness
  • No joint pain , swelling or stiffness
  • Hematopoietic system
  • No easy bruising
  • No prolonged bleeding tendencies
  • Integumentary
  • No skin rashes
  • No skin itching and redness
  • No skin swelling
  • No hair and nail loss

9
PAST MEDICAL HISTORY
  • This is her 4th admission ,
  • 1st at Lugalo hospital 14 years ago,
  • diagnosed with fibroid
  • underwent hysterectomy, treated and was
    discharged with no complication.
  • 2nd at Kairuki hospital 3 years ago due to
    severe headache
  • Diagnosed with HTN DM Kept on medication T.
    Glimepiride Metformin Tablets (2mg and 500mg )
    BD x 1/12 T. candesartan 16mg od x 1/12,T.
    spironolactone 25mg od for 1/12 and discharged
  • 3rd at kairuki hospital, 2 years ago due to
    diabetic mellitus complication ,
  • Was treated ,recovered to continue with
    medication at home

10
Cont.
  • She is a known
  • asthmatic patient diagnosed about 25 years ago
  • on salbutamol inhaler and tablets.
  • DM patient diagnosed
  • 3 years ago at Kairuki Hospital
  • currently on T. Glimepiride Metformin Tablets
    (2mg and 500mg ) BD x 1/12
  • HTN diagnosed 3 years ago, currently on
  • T. candesartan 16mg od x 1/12,
  • T. spironolactone 25mg od for 1/12

11
Cont
  • She has h/o surgery hysterectomy
  • due to fibroids
  • She has h/o multiple OPD visit for
  • drug refill of HTN,DM and ASTHMA
  • She has h/o using powdery herbal
  • medications twice a day for 1/12
  • as she believed she could cure asthma
  • She had no
  • h/o blood transfusion
  • h/o food and drug allergy
  • h/o trauma

12
GYNAECOLOGICAL HISTORY
  • She is 14 years post menopausal woman who is
    P5L4 with no h/o
  • painful coitus and post coitus bleeding
  • She has no history of contraceptive use

13
FAMILY HISTORY
  • 2nd born out of 5 children
  • Parents are alive and well.
  • All other siblings are alive and well.
  • Has h/o HTN on paternal side- her aunt.
  • has no h/o
  • other known familial disease asthma, sickle
    cell ,epilepsy
  • Sudden death in the family

14
SOCIAL HISTORY
  • Married and living with her husband
  • Has 5children ,
  • 1 died due to severe abdominal pain 4 alive
  • She has no h/o
  • alcohol use, cigarette smooking and illicit use
    of drugs
  • She lives in a well ventilated house,
  • windows allow air and light in and out
  • She uses charcoal stove for cooking

15
DIETARY HISTORY
  • She takes 3 meals in a day
  • Morning tea and brown bread
  • Afternoon roasted bananas or potatoes,
  • with meat and vegetables.
  • Boiled fish with vegetables
  • Evening she usually has fried banana and fruits
  • She drinks about 2-3 liters of water per day.
  • She uses salt in her diet
  • Diet is not satisfactory to diabetic and
    hypertension.

16
SUMMARY 1
  • K.H.S a 66 year old female who is a
  • known asthmatic, hypertensive and diabetic on
    medication,
  • presented with DIB for 7 days,
  • with
  • chest tightness, central chest pain, dry cough,
  • wheezes, inability to complete sentences,
  • orthopnea and bilateral lower limbs swelling.
  • With no palpitation, paroxysmal nocturnal dyspnea

17
CLINICAL DIAGNOSIS BASED ON HISTORY
  • DIAGNOSIS 1
  • ACUTE SEVERE ASTHMA
  • Reasons
  • Known asthmatic patient
  • Increasing chest tightness
  • wheezing dyspnea not relieved by salbutamol
    inhaler
  • cannot complete a sentence in 1 breath or too
    breathless to talk.
  • DIFFERENTIAL DIAGNOSIS
  • 1. COPD
  • Reason for chest tightness, wheezing, DIB,
    cough,
  • Reason against no h/o cigarrete smoking,
  • 2. Community acquired pneumonia
  • reasons for-difficult in breathing,
    cough, chest pain
  • reasons against-presence wheezes
    no hx fever

18
DIAGNOSIS
  • 2. CONGESTIVE CARDIAC FAILURE secondary to HTN
  • Reasons Orthopnea ,Central chest pain,
    Bilateral LL edema, dry cough
  • -known HTN patient
  • DIFFENTIAL DIAGNOSIS
  • Myocardial Infarction
  • Reasons for Central chest pain
  • -difficult in breathing
  • Reasons against chest pain does not radiate jaw
    and left arm, gradual onset of DIB

19
DIAGNOSIS
  • OTHER DIAGNOSIS
  • Type 2 diabetes mellitus
  • Hypertension

20
PHYSICAL EXAMINATION
  • GENERAL EXAMINATION
  • Conscious, ill looking with non-rebreather oxygen
    mask
  • Pink cannula on the dorsum of left thumb for IV
    medications
  • urinary catheter with urine output of 500mls
    collected over the past six hours.
  • normal hair texture ,colour and distribution
    which were not easily pluckable
  • She was not pale, not jaundiced, not cyanosed
  • No Eye, Nose and Ear swelling ,discharge nasal
    bleeding.

21
GENERAL EXAMINATION
  • She had no
  • angular stomatitis, angular cheilitis and
    atrophic glossitis
  • Janeway lesions,Oslers nodes, splinter
    haemorrhage,
  • Palmar Erythema, Koilonychia, Leukonychia, finger
    clubbing
  • Normal Capillary refill less than 2 seconds
  • No palpable peripheral Lymph nodes
  • Bilateral Pitting LL oedema at pedal and pretibial

22
VITALS
  • Temperature 36.5C
  • Pulse rate 108bpm
  • Respiratory rate 30 b/m
  • Blood pressure 138/92mmHg
  • Spo2 on 15L/min 99
  • SP02 ON RA 75-84
  • CONCLUSION
  • She was tachycardic, tachypnoeic and desaturating
    in RA

23
SYSTEMIC EXAMINATION
  • 1. Respiratory Examination
  • On inspection-
  • Patient had an oxygen mask for breathing
  • Normal chest contour that moves with respiration
  • Respiratory rate- 30 B/MIN
  • No traditional or therapeutic marks on the
    chest.
  • Symmetrical chest movement
  • Uses accessory muscles and has intercostal
    recession

24
SYSTEMIC EXARESP CONTI
  • Palpation
  • Supraclavicular, axillary and cervical LNs
  • were not palpable
  • Trachea was centrally located
  • No palpable superficial mass tenderness,
  • Apex beat was located at 6th intercostal space
    lateral to the Mid clavicular line
  • Normal tactile vocal fremitus and chest
    expansion on both anterior and posterior.

25
SYSTEMIC EXA.RESP CONT.
  • Percussion
  • Both lungs were resonant on percussion
  • Auscultation
  • wheezes
  • bilateral crackles on the bases of the lungs
  • Normal vocal resonance
  • Negative whispering pectoriloquy

26
CARDIOVASCULAR SYSTEM
  • Right Radial pulse was 108 beats per minute
  • Regular rhythm and strong in volume.
  • The pulse was
  • non-collapsing synchronous to peripheral
    pulses. radial, femoral, carotid
  • The blood pressure was 138/92 mmHg
  • Heard at Korotkoff phase 1 to 5.
  • The state of arterial walls was normal
  • Neck veins were not distended.
  • Negative abdominal jugular reflux

27
CARDIOVASCULAR SYSTEM
  • Precordial examination
  • Inspection
  • there were no surgical or traditional scars.
  • There was no precordial hyperactivity or bulging.
  • There was no prominent superficial veins
  • Palpation
  • The apex beat was located on the 6th ICS
    lateral to the mid clavicular line
  • It was non tapping and non heaving.-
  • There were no heaves and thrills.

28
CARDIOVASCULAR SYSTEM
  • Auscultation
  • S1 and S2 were audible in
  • aortic, pulmonary, tricuspid and mitral areas.
  • No added sounds like gallop rhythm were heard
  • Bilateral fine crackles were heard on lung bases
  • No palpable tender liver.
  • liver span 15cm

29
GASTROINTESTINAL SYSTEM
  • Oral examination
  • No oral thrush, angular cheilitis/stomatitis
    dental erosion
  • Per abdomen
  • Inspection
  • Normal abdominal contour Symmetrical
  • move with respiration.
  • The umbilicus is inverted and retracted
  • There was healed sub umbilical scar
  • There were no any distended veins

30
Cont.
  • Palpation
  • There was no tenderness or any palpable mass
    during superficial palpation
  • On deep palpation liver, spleen, left and right
    kidneys were not palpable
  • No muscle guarding no rebound tenderness
  • Percussion
  • Tympanic note was heard.
  • Liver span was 15cm
  • Auscultation
  • Bowel sounds were heard normally 3 bowel sounds
    per minute.
  • There were no abdominal bruits heard

31
NERVOUS SYSTEM EXAMINATION
  • Higher centres
  • The patient was conscious with GCS 15/15
  • both long and short-term memories were intact
  • Fluent speech and coherent language
  • Had good concentration
  • she was oriented to person place and time

32
Cranial nerve examination
  • CN 1 (olfactory)
  • The patient could smell an orange peel with each
    nostril
  • CN2 (OPTIC)
  • She was able to see clearly objects from
  • the distance and from near through both eyes
  • She responded positively pupillary constriction
    upon light
  • She was able to see sideway objects while looking
  • forward object(pen) with both eyes and on one eye
    closed
  • CN3, 4, 6 (OCULOMOTOR, TROCHLEAR, ABDUCENS)
  • The patient tracked an object (pen) in a H
    shaped track
  • The patient was able to move eyes in all direction

33
Cranial nerves
  • CN V. TRIGEMINAL
  • Motor root The patient could clench the
    teeth,open jaw against resistance
  • Sensory roots the patient responded to light
    touch on
  • ophthalmic, maxillary and mandibular areas
  • CN VII. FACIAL
  • The patient could
  • wrinkle the forehead, raise eyebrows, show teeth,
    blow both cheeks on resistance
  • shut both eyes and open against resistance
  • Sensory
  • The patient was able to detect
  • sweet, salt, sour bitter when tested with sugar
    and salt

34
Cranial nerves
  • CN 8 (vestibulocochlear)
  • Able to hear normal sound and whisper
  • Air conduction was better than bone conduction
    in both ears
  • as demonstrated by Rinnes tests. - Webers test
    was negative as
  • she heard equally on both ears.
  • CN 9 and 10 (glossopharyngeal, vagus) -
  • Patient could swallow Uvula was not deviated.
  • CN 11 (accessory)
  • The patient could
  • shrug her shoulders against turn her neck
    sideways against resistance.
  • CN 12 (hypoglossal)
  • The patient could
  • protrude her tongue and move it side to side with
    no deviations present.

35
PERIPHERAL NERVOUS SYSTEM
  • Motor examination
  • Coordination was intact she performed the finger
    nose and heel shin test

R.U.L L.U.L R.L.L L.L.L
Bulk NORMAL NORMAL NORMAL NORMAL
Involuntary movements NIL NIL NIL NIL
Gait Not assessed - - -
Tone NORMAL NORMAL NORMAL NORMAL
Power 5/5 5/5 5/5 5/5
36
Motor examination
  • Reflexes
  • SUPERFICIAL REFLEXES Abdominal reflexes present

DEEP TENDON RIGHT SIDE LEFT SIDE
BICEPS REFLEX NORMAL NORMAL
TRICEPS REFLEX NORMAL NORMAL
PATELLA REFLEX NORMAL NORMAL
ACHILLES REFLEX NORMAL NORMAL
BABINSKI DOWNWARD DOWNWARD
37
Sensory examination
  • She could sense
  • pain, pressure and crude touch on
  • both upper and lower limbs
  • She could perceive vibrations and fine touch on
  • both upper and lower limb.
  • Meningeal signs
  • No neck stiffness
  • Kernings and Brudzinski's sign negative

38
SUMMARY 2
  • K.H.S a 66 year old female who is a known
  • asthmatic, hypertensive and diabetic on
    medication, presented with DIB for 7 days,
  • With chest tightness, central chest pain, dry
    cough, wheezes, inability to complete sentences,
    orthopnea and lower limb swelling.
  • She denied palpitation, PND

39
Cont.
  • she had bilateral pitting edema
  • With labored breathing (tachypneic, tachycardiac
    and desaturating in RA),
  • using accessory muscles and had intercostal
    recession
  • with wheezes and bilateral fine crackles at lung
    bases
  • Displaced cardiac apex beat to 6th ics lateral
    to MCL

40
Clinical diagnosis based on history and physical
examination
  • 1. ACUTE SEVERE ASTHMA
  • Reasons forKnown asthmatic patient ,chest
    tightness, wheezing dyspnea not relieved
    salbutamol inhaler ,cannot complete a sentence in
    1 breath or too breathless ,tachycardic,
    tachypneic, desaturating in RA, with generalized
    wheezes.
  • DIFFERENTIAL DIAGNOSIS
  • 1. COPD
  • Reason for chest tightness, wheezing, DIB,
    cough, labored breathing with (tachypnea and
    tachycardic and desaturate in RA) and use
  • Reason against no h/o cigarrete smoking,
  • 2. Community acquired pneumonia
  • Reasons for-difficult in
    breathing,cough,chest pain, tachypnea, use of
    accessory muscles and intercostal recession
  • Reasons against-presence wheezes ,no hx
    fever

41
Diagnosis
  • 2.CONGESTIVE CARDIAC FAILURE secondary HTN
  • Reasons Orthopnea, Lower limb oedema,Cardiomegaly
    due to shifting of the CAB,bilateral fine
    crackles at lung bases
  • DIFFERENTIAL DIAGNOSIS
  • 2. Dilated cardiomyopathy
  • Reason for known HTN ,orthopnea, central chest
    pain, known htn patient, tachypneic,tachychardic
    ,displaced cardiac apex beat to 6th ics lateral
    to mcl
  • Reason againstno PND,

42
Management
  • INVESTIGATION DONE IN THE WARD
  • FBP
  • ESR
  • CRP
  • Serum electrolyte
  • Serum troponin
  • D dimer
  • Liver enzymes
  • Serum urea and creatinine
  • Chest X-ray

43
FBP
44
CRP ESR
  • ESR 10.230 NORMAL
  • CPR 1-3 mg/l

45
SERUM TROPONIN I D.DIMER
  • Troponin I normal ranges0-0.04ng/ml

46
SERUM UREA LEs
  • AST normal range 8-48 u/l
  • ALT normal range 7-55 u/l

47
SERUM CREATININE
48
SERUM ELECTROLYTES
49
CHEST X-RAY
50
ECHOCARDIOGRAPHY
51
INVESTIGATIONS TO BE ADDED
  • ECG
  • ABG
  • Lipid profile
  • spirometry

52
TREATMENT
  • Non-pharmacological
  • Oxygen support-high flow oxygen 15l/min
  • Pharmacological
  • Inj aminophylline 250mg start
  • Nebulization with budesonide twice a day for 1/7
  • Inj hydrocortisone 100mg tds for 1/7
  • Inj amoxiclav 1.2mg bd for 5/7
  • Inj furosemide 20mg tds for 2/7
  • T.spirolactone 25mg od for 5/7
  • T. Glimepiride Metformin Tablets (2mg and
    500mg ) BD x 1/12
  • T. candesartan 16mg od x 1/12

53
PREVENTION
  • Avoiding exposure to allergens dust, cold air,
    pollen, perfumes
  • Maintaining good indoor air quality
  • Health education
  • Use the charcoal burner outdoors
  • Exercises
  • Diet modification
  • Adherence to prescribed medication

54
ASTHMA
  • PRESENTERS Sr Sara Deogratius
  • Dr Neema Lweno

55
Bronchial asthma
  • A chronic disorder of airways involving a complex
    interaction of
  • airway inflammation,
  • airflow obstruction
  • bronchial hyperresponsiveness
  • following exposure to stimuli
  • Commonly co exist with COPD
  • Episodic reversible broncho constriction but
  • in some there may be a degree of irreversible
    obstruction.

56
Types of Asthma
  • Two types
  • Extrinsic/Atopic/Allergic
  • associated with exogenous substance
  • Intrinsic /non atopic

57
Pathophysiology of asthma
  • Involves three components
  • Airway inflammation
  • Intermittent airflow obstruction
  • Bronchial hyper responsiveness

58
Pathophysiology of asthma
  • Airway Inflammation
  • Antigen presenting cell, dendritic cell, present
  • to naïve T-lymphocyte with help of IL2 and IL12,
  • T-Helper cause cell mediated immunity
  • and neutrophilic inflammation
  • Mediator of inflammation
  • e.g. Histamine and Prostaglandins are released
  • with help of IgE, mast cell basophils, and
    eosinophilis
  • leading to airway inflammation

59
Pathophysiology of asthma
  • Airflow Obstruction
  • Caused by acute
  • bronchoconstriction, airway edema,
  • chronic mucus plug formation and airway
    remodeling
  • Acute bronchoconstriction is a consequence of
  • IgE-dependant mediator release after exposure
  • to aeroallergens early asthmatic response
  • Chronic mucus plug formation consists of exudate
  • of serum proteins cell debris that may take
    weeks to resolve

60
Pathophysiology of asthma
  • Bronchial Hyper responsiveness
  • ??Bronchoconstrictor response to
  • multiple inhaled triggers that would have
  • no effect on normal airways.
  • Linked to the frequency of episodes
  • Most of the triggers seem to act indirectly
  • by causing release of Bronchoconstrictors from
    mast cells.

61
Risk factors
  • Environmental allergens
  • E.g. dust, cat, dog hair, pollen
  • Viral respiratory tract infection
  • (infancy rhinovirus illness)
  • Gastro esophageal reflux disease
  • (via vagal acid in esophagus?
  • ?airway resistance and reactivity)
  • Obesity especially infancy rapid weight gain
  • Environmental pollutant, smoke
  • Emotional factors

62
Clinical features
  • Characteristic symptoms
  • Wheezing
  • Dyspnea
  • Cough
  • Worse at night with early morning awakening.
  • Increased mucus production which is thick and
  • difficult to expectorate.
  • Use of accessory muscles of ventilation
  • due to increased ventilation

63
Clinical features
  • Physical findings
  • Rhonchi (expiratory gt inspiratory)
  • Hyperinflation
  • No findings if asthma is under control

64
Pulmonary Function Tests
  • ?? FEV1, FEV1/FVC ratio
  • Reversibility
  • demonstrated by gt 12 and 200 ml increased
  • in FEV1 15 minutes after an inhaled short-acting
    ß2-agonist
  • Exercise testing may demonstrate post
  • exercise broncho constriction if there is
  • history of Exercise induced Asthma

65
Other investigations
  • Hematological Tests
  • Total serum IgE and specific IgE to inhaled
    allergens
  • may be measured
  • Skin tests
  • Skin prick tests to common allergens are positive
  • in allergic asthma but negative in intrinsic
    asthma
  • This may help convince patients to avoid certain
    allergens
  • Imaging
  • Chest imaging may show hyper inflated lungs
  • In exacerbations, there may be evidence
    ofpneumothorax

66
Management of Asthma
  • The ultimate goal
  • prevent symptoms
  • minimize morbidity from acute episodes and
  • prevent functional and psychological morbidity to
    provide near health lifestyle
  • Pharmacological rx is achieved by 2 groups of
    drugs
  • Bronchodilators (Relievers) rapid relief of
    symptoms
  • Controllers reduces the underlying inflammation

67
Management of Asthma
  • Bronchodilators
  • Act on the airway smooth muscle and
  • reverse the broncho constriction
  • Consists of
  • ß2-agonists
  • anticholinergics
  • theophylline.

68
Management of Asthma
  • ß2-agonists
  • Given by inhalation to reduce side effects.
  • SABAs
  • salbutamol (albuterol) and terbutaline
  • duration of action of about 3-6 hours.
  • LABAs
  • E.g salmeterol
  • longer duration of action (12 hours)
  • given with ICS(inhaled corticosteroids)
  • to reduce exacerbations.

69
Management of Asthma
  • Anticholinergics
  • Muscarinic receptor antagonists such as
    ipratropium bromide
  • prevent cholinergic nerve-induced
    bronchoconstriction
  • and mucus secretion
  • Usually given after therapy with ß2-agonists has
    failed.
  • Theophylline
  • Used after therapy with ß2-agonists is not
    sufficient
  • In low doses, it has anti-inflammatory effects
    and
  • is additive to the effects of ICS
  • IV aminophylline
  • used in severe exacerbations but has been
    replaced by
  • high doses of inhaled SABAs, but is still used
    in asthma
  • refractory to SABAs

70
Management of Asthma - Controllers
  • Inhaled Corticosteroids
  • The most effective controller
  • Given once or twice a day depending on severity.
  • Long term use can help control airway
  • hyper responsiveness
  • First-line to prevent persistent asthma, but it
    is usual
  • to add a LABA when symptoms are not controlled
    with
  • ICS alone. Eg budesonide,

71
Management of Asthma - Controllers
  • Systemic Corticosteroids
  • IV formulations are used for acute severe asthma
  • OCS for 5-10 days are effective for acute
  • exacerbations without the need for tapering
  • About 1 of patients may require OCS
  • for maintenance treatment. E.g prednisolone.
  • Antileukotrienes
  • Include montelukast and zafirlukast
  • Used as an add-on therapy in patients
  • not responding to low dose ICS,
  • but are less effective than LABA

72
Management of Asthma - Controllers
  • Cromones
  • Cromolyn sodium and nedocromil sodium inhibit
  • mast cell activation and therefore useful in EIA
    and
  • allergen and Sulphur dioxide-induced asthma
  • Short duration of action (four times daily
    dosage)
  • and hence replaced by ICS
  • Anti-IgE
  • Omalizumab inhibits IgE-mediated reactions
  • Limited to those that do not respond to
  • maximum doses of inhaler therapy
  • Given as subcutaneous injection every 2-4 weeks
  • Objective benefit is seen after 3 4 month
    therapy

73
Treatment of asthma according to severity
  • Based on category of severity of asthma rx
    consists of
  • Preventing the inflammation leading to
    bronchospasm
  • Controllers- ICS e.g Beclomethasone
  • Relieving bronchospasm
  • Short acting beta 2 agonists i.e salbutamol

74
Treatment of asthma according to severity
  • STEP 1
  • Intermittent asthma 
  • Intermittent symptoms once/week symptomatic
  • Night time symptoms twice/month
  • Normal physical activity
  • Treatment
  • Inhaled Salbutamol when symptomatic.
  • No long-term treatment

75
Treatment of asthma according to severity
  • STEP 2
  •  Mild persistent asthma
  • Symptomsgt once/week but lt once/day
  • Night time symptoms gt twice/month
  • Symptoms may affect activity
  •  Treatment
  • Continuous treatment with inhaled
    Beclomethasone
  • 100-250mcg twice daily
  • -Inhaled Salbutamol when symptomatic

76
Treatment of asthma according to severity
  • STEP 3 
  • Moderate persistent asthma
  • Daily symptoms
  • Night time symptoms once/week
  • Symptoms affect activity
  • Daily use of Salbutamol
  • Treatment
  • Continuous treatment with inhaled
  • Beclomethasone 250-500mcg twice daily
  • Inhaled Salbutamol 1-2 puffs 4times/day

77
Treatment of asthma according to severity
  • STEP 4
  • Severe persistent asthma
  • Daily symptoms
  • Frequent night time symptoms
  • Physical activity limited by symptoms
  • Treatment
  • Continuous treatment with inhaled
  • Beclomethasone 500mcg twice daily
  • Inhaled Salbutamol 1-2 puffs 4-6 times/day

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Acute Severe Asthma - Diagnosis
  • Increasing chest tightness, wheezing and dyspnea
  • that is not relieved by regular reliever inhaler
    therapy.
  • Patients can become so breathless that they are
    unable
  • to complete sentences and may become cyanotic
  • Examination shows
  • increased ventilation, hyperinflation and
    tachycardia.
  • Marked reduction in
  • spirometry values and PEF (peak expiratory flow)
    rate
  • ABG shows hypoxemia and low PCO2 due to
    hyperventilation
  • A rising PCO2 indicates impending respiratory
    failure
  • Chest imaging may show pneumothorax or pneumonia

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Acute Severe Asthma - Treatment
  • High concentration of oxygen by face mask to
  • achieve saturations of gt90
  • Use high dose SABAs delivered by
  • nebulizer or MDI(metered dose inhaler) with
    spacer.
  • IV formulations may be used in severely ill
    patients
  • Anticholinergics may be added if there
  • is no response, as there are additive effects
  • IV aminophylline has been shown to be useful in
  • refractory cases
  • Magnesium sulphate can be added to SABAs
  • but is not routinely recommended

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81
Acute Severe Asthma - Treatment
  • Prophylactic intubation may be done
  • in patients with impending respiratory failure
  • In respiratory failure, patients should be
  • intubated an anesthetic may be considered
  • if bronchodilator therapy has failed
  • Sedatives should be avoided as they
  • suppress ventilation
  • Antibiotics can be given if there are signs of
    pneumonia

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Refractory Asthma
  • About 5 of patients will not respond to
  • maximal inhaler therapy.
  • Some of these may be require OCS maintenance
  • Mechanisms
  • Noncompliance, especially to ICS
  • Over exposure to allergens or unidentified
    occupational agents
  • Upper airway disease
  • Drugs e.g. beta-blockers, aspirin, COX-inhibitors
  • Premenstrual worsening
  • Thyroid disease

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Refractory Asthma
  • Differentials
  • Vocal cord dysfunction
  • COPD
  • Brittle Asthma Unpredictable changes in lung
    functions
  • Type 1 Persistent variability requiring OCS or
    IV ß2-agonists infusion
  • Type 2 Normal lung function with sudden falls in
    lung function resulting in death
  • Rx Subcutaneous epinephrine
  • Some patients may have corticosteroid-resistant
    asthma

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Aspirin-Sensitive Asthma
  • About 1 5 become worse with
  • aspirin and other COX-inhibitors
  • There is usually a history of
  • perennial rhinitis and nasal polyps in nonatopic
    patients
  • Onset is late in life
  • Even in small doses, aspirin causes
  • rhinorrhea, conjunctival irritation, facial
    flushing wheezing
  • Responds to usual therapy with ICS

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Asthma in the Elderly
  • Asthma may begin very late in life
  • Principles of management are the same but
  • the SE need more careful attention such as
  • muscle tremors with ß2-agonists and systemic
    side effects with ICS
  • Due to the presence of comorbidities,
  • drug interactions need to be monitored such as
  • with ß-blockers, COX-inhibitors etc.
  • COPD may coexist in this population

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Asthma Complications
  • Pneumonia
  • Lung collapse
  • Metabolic acidosis
  • Electrolyte disturbance
  • Respiratory failure

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PREVENTION
  • Controlling /avoiding the
  • known triggering agents (dust, cold, fumes,
    pollen etc.)
  • Providing self -management plan
  • On how to manage asthma attacks.
  • Adequate supply of medications to use at home.
  • Regular check up
  • to see the progress and changing ,
  • reducing or adding dose.
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