Travel Medicine

Question 1

From what age can someone be vaccinated against Hepatitis A

Answer 1

12 months

Question 2

What kind of virus is hepatitis A

Answer 2

RNA

Question 3

How long can the hepatitis A virus survive outside of a host?

Answer 3

Weeks in water, marine sediment, shellfish or soil

Several hours on hands, longer in food kept at room temperature

Question 4

Is the hepatitis A virus susceptible to heat or freezing?

Answer 4

No

Question 5

Transmission of hepatitis A

Answer 5

Foecal-oral route

Can also occur (mostly through this route) via direct person-to-person contact, sexual contact and blood transfusions

Question 6

Incubation period of hepatitis A

Answer 6

15-50 days

Question 7

How does the outcome of hepatitis A infection differ between children and adults?

Answer 7

Children are generally asymptomatic whereas 75% of infected adults will develop icteric disease

This is why in areas with high endemic rates, children tend to be infected early thus clinical disease is uncommon in locals

Question 8

Most common causes of hepatitis A infection in Australians

Answer 8

Travel to an area with higher rates

Common outbreaks from contaminated food/water

Question 9

Should we check for natural immunity against hepatitis A prior to vaccination?

Answer 9

Yes - in those born prior to 1950 and in those with a past history of unexplained hepatitis or jaundice

(If anti-HAV IgG present, vaccination not required)

Question 10

Presentation of hepatitis A

Answer 10

Prodromal phase:
	- Lasts 4-10 days
	- Fever, malaise, weakness
	- Anorexia, nausea and vomiting
Acute hepatitis phase:
	- Dark urine often first sign
	- Jaundice and pale stools 1-2 days later
	- Associated with gradual resolution of systemic prodromal symptoms
	- Hepatic pain and pruritus may occur

Liver function returns to normal within a month usually
10% can have prolonged or relapsing symptoms over 6-9 months, however chronic infection does not occur

Question 11

Management of hepatitis A

Answer 11

Supportive only

Vaccination not required in someone who has been infected

Question 12

Contraindications to hepatitis A vaccination

Answer 12

Allergy to previous HAV vaccine or components
Allergy to Yeast if giving HepA/B combination vaccine

Safe in all others (including pregnancy, immunosuppression etc. - though seroconversion rates may be lower)

Question 13

Who should you recommend Hepatitis A vaccination to?

Answer 13

• ATSI children (routine vaccination schedule)
• Travellers to intermediate or high endemicity areas (Asia, Africa, South America, SouthEast Europe and Middle East)
• Those living in remote areas
• Occupational risk (healthcare workers, especially in ATSI communities)
• Those with lifestyle risk (IVDU, MSM)
• Pre-existing chronic liver disease or chronic hep B/C infection
• those with intellectual disabilities

Question 14

How many doses required to complete Hepatitis A primary vaccination course?

Answer 14

2
1st provides at least 12 months immunity
2nd should be given 6-18 months after first (recommendation depends on brand)

Boosters not considered to be necessary at current

Question 15

What pathogens cause enteric fever

Answer 15

S. typhi or S. paratyphi

Question 16

Where are the highest endemic rates of typhoid/paratyphoid

Answer 16

Indian subcontinent

Also high in Asia (except Japan and Singapore), Africa and Middle East

Question 17

What is the risk of a traveller contracting enteric fever

Answer 17

1:3000 for a traveller spending 4+ weeks in a high risk area

Question 18

How common is it to develop carrier status after typhoid fever

Answer 18

Up to 5% will continue to shed the pathogen for >1y

Question 19

Typical incubation period for typhoid/paratyphoid

Answer 19

7-14 days (range 3-60)

Question 20

Clinical presentation of typhoid/paratyphoid (enteric fever)

Answer 20

Fever - increases with disease progression
Dull frontal headache
Malaise
Myalgia
Anorexia
Dry cough

Less commonly:
Constipation (sometimes diarrhoea in children)
Abdo pain
Relative bradycardia
Splenomegaly
Rash "Rose spots"

Question 21

What is the typical typhoid rash

Answer 21

Rose spots

• erythematous blanching papules, mostly on anterior trunk (also on back and proximal limbs)
• 2-3mm in diameter
• each lasts 3-5 days

Question 22

Potential complications of typhoid

Answer 22

(Typically occurring after 14 days of illness)

• GI bleeding
• bowel perforation (most commonly ileal)
• typhoid encephalopathy

Question 23

Tests to diagnose typhoid

Answer 23

No test is really ideal

Gold standard is blood culture

May also be sporadically cultured in urine or stool

Question 24

To whom would you recommend a typhoid vaccination

Answer 24

Anyone >2y travelling to moderate-high risk countries

Question 25

How soon before travel should typhoid vaccination be provided

Answer 25

At least 2 weeks prior to travel

Question 26

Are repeat doses required for typhoid vaccination?

Answer 26

Only 3 yearly boosters are required. The primary course is just the one dose.

Question 27

Treatment of typhoid

Answer 27

Azithromycin
OR ciprofloxacin (as long as not acquired in India or SouthEast Asia)

Note that fever takes 3-5 days to subside despite antibiotic therapy, and patients may feel worse during this time

Question 28

High risk areas for malaria

Answer 28

Highest risk generally: Africa, Oceania
Moderate: Asia, South America
Low: Central America

Question 29

Most common malarial parasite in Africa v Asia

Answer 29

Africa; Plasmodium falciparum

Asia/Pacific: Plasmodium vivax

Question 30

Different malaria parasites and their incubation periods

Answer 30

P. falciparum 9-14 days (non-relapsing)
P. Malariae 18-40 days (non-relapsing)
P. vivax 12-18 days usually, some strains up to 10 months (relapsing)
P. ovale 12-18 days (relapsing)

Question 31

Recommendations for non-medical prophylaxis against malaria

Answer 31

Personal protection methods from dusk to dawn (when anopheles mosquito is active)

• light, loose, long clothing covering arms and legs
• Insect repellent containing 20-40% DEET
• mosquito nets +/- permethrin impregnantion

Question 32

Main malaria chemoprophylaxis options

Answer 32

Doxycycline 100mg/day from 2 days prior to exposure to 4 weeks after
Mefloquine 250mg/week for 2-4 weeks prior, for 4 weeks after
Malarone 1 tab daily from 1 day prior to 1 week after

Question 33

Contraindications to doxycycline

Answer 33

Age <8y
Pregnancy
Breastfeeding

Question 34

Common side effects to doxycycline

Answer 34

Nausea, indigestion, photosensitivity, vaginal candidiasis

Question 35

Benefits of using doxycycline as malarial chemoprophylaxis

Answer 35

Cheap
Protects against some other tropical diseases
Can be commenced at short notice
Suitable for long term use

Question 36

Downfalls of using doxycycline as malarial chemoprophylaxis

Answer 36

Contraindications

Unsuitable for use in children <8y

Question 37

Contraindications to mefloquine

Answer 37

1st trimester of pregnancy
Children <5kg
History of epilepsy
Psychiatric illness (including anxiety and depression)
Cardiac conduction disorders
Other medications that prolong QT

Question 38

Common side effects of mefloquine

Answer 38

Headache
Nausea
Sleep disturbance
Vivid dreams
Dizziness
Rarely: precipitate depression/anxiety/psychosis

Question 39

Benefits of using mefloquine as malarial chemoprophylaxis

Answer 39

Can be used long term

Suitable for children

Question 40

Downfalls of mefloquine as malarial chemoprophylaxis

Answer 40

Cost
Potential side effects
Contraindications
Needs to be started 2-4 weeks prior to travel

Question 41

Contraindications to malarone

Answer 41

Pregnancy, breastfeeding

Question 42

Common side effects of malarone

Answer 42

Headache, nausea

Question 43

Benefits of using malarone as malaria chemoprophylaxis

Answer 43

Minimal side effects
Paediatric dose available
Can be commenced at short notice (1 day prior to exposure)

Question 44

Downfalls of using malarone as malaria chemoprpphylaxis

Answer 44

Very expensive

Not licensed for use long term (due to lack of data, not known risks)

Question 45

Clinical presentation of malaria

Answer 45

Fever in returned traveller - may come and go or be constant
PLUS influenza-like symptoms mostly
- chills
- headache
- myalgia/arthralgia
- malaise
- profuse sweating
- nausea, lack of appetite
- diarrhoea
- abdominal pain
- cough
- anaemia +/- jaundice
Symptoms CAN occur intermittently

Question 46

Signs of severe malaria

Answer 46

Seizures
Confusion
Kidney failure
Acute respiratory distress syndrome
Coma

Question 47

Incubation period of malaria

Answer 47

7 days to several months or more after being bitten by infected mosquito (depends on specific parasite)

Question 48

Diagnosis of malaria

Answer 48

Blood smear microscopy: parasitised red cells
OR rapid diagnostic tests (less accurate, cannot differentiate between different species and cannot quantify)
PCR testing - takes a long time, but more sensitive than microscopy

Question 49

First line treatment of malaria

Answer 49

Artemether + lumefantrine (though there are additional considerations for specific species)

IV treatment for severe disease

Daily parasite count until negative
Repeat CBE and microscopy at 7 days and 28 days post treatment completion

Question 50

Individuals at highest risk for severe/complicated traveller’s diarrhoea

Answer 50

• insulin dependent diabetics
• congestive heart failure
• advanced cancer
• HIV infection
• Inflammatory bowel disease/other bowel abnormalities
• reactive arthritis
• reduced gastric acidity
• HLA-B27 positive individuals

Question 51

Most common causes for traveller’s diarrhoea

Answer 51

Bacterial (50-80%)
- ETEC most common
- EIEC
- EAEC
- Shigella
- Campylobacter
- Salmonella
Norovirus (10-20%)
Protozoans only should be considered in those with diarrhoea >14 days or >72 hours despite 3 days antibiotics

Question 52

How effective is the cholera vaccine?

Answer 52

> 90% effective against vibrio cholera only

No significant evidence for reduction of traveller’s diarrhoea overall or of ETEC

Question 53

Recommendations for giving cholera vaccine

Answer 53

Consider in individuals with increased risk of severe of complicated traveller’s diarrhoea, OR in people travelling to an area with recent epidemic

Question 54

Recommendations for self-management of traveller’s diarrhoea

Answer 54

Hydration maintenance is main goal!
Oral rehydration solution always if diarrhoeal illness + loperamide
If symptoms worsen or persist >24 hours, add in antibiotics

If moderate-severe from the start, loperamide + antibiotics as initial management

Question 55

Recommended loperamide dose in setting of traveller’s diarrhoea

Answer 55

2 tabs (4mg) stat, then 1 tablet (2mg) after each bowel motion to max of 8 tabs per day

Question 56

Recommended antibiotics and dosing for self-management of traveller’s diarrhoea

Answer 56

Ciprofloxacin 500mg stat OR BD for 72 hours
Norfloxacin 400mg stat or BD for 72 hours
Azithromycin 500mg daily for 3 days

Kids:
Azithro 10-25mg/kg (make sure the pharmacist does not mix it up, give sterile water and instructions on how to doso)daily for 3 days OR
cipro/norflox 10mg/kg BD

Usually single dose is adequate, but if symptoms continue, continue for up to 3 days (if still persisting then take Tinidazole 2g stat in case of protozoa)

Question 57

Another name for schistosomiasis

Answer 57

Bilharzia

Question 58

Where is schistosomiasis sfound

Answer 58

Throughout Africa (mostly sub-Saharan), parts of Asia, South America, the Caribbean, the Middle East

Question 59

Typical incubation period of schistosomiasis

Answer 59

14-84 days (many people subclinical or asymptomatic)

Question 60

Where does schistosomiasis lodge

Answer 60

S. mansoni and S. japonicum lodge in the mesenteric venous plexus of the liver
S. haemtobium lodges in the venous plexus of the lower urinary tract

Note that Africa has both Mansoni and haematobium species endemic

Question 61

Route of infection with schistosomiasis

Answer 61

Direct skin contact with contaminated fresh water - even if only for 1 minute

Question 62

Advising travellers to prevent risk of schistosomiasis

Answer 62

• advise no swimming in freshwater or wading through wetlands barefoot etc. in endemic areas EVEN FOR 1 MINUTE
• Don’t listen to locals who claim the water is “safe”
• DON’T listen to locals/other travellers who advise to take an immediate dose of praziquantel (ineffective and can worsen things)
• encourage serological testing 3 months after exposure if does swim in the water, even if asymptomatic
• warn of the serious complications (myocarditis, pericarditis, seizures, ataxia, motor paralysis)

Question 63

Presentation of acute schistosomiasis

Answer 63

AKA Katayama fever (tends to occur in travellers from non-endemic countries)
Few weeks after exposure
- abdopain
- diarrhoea
- cough
- fever
- fatigue
\+/- hepatosplenomegaly 
\+/- eosinophilia
Spontaneous resolution over weeks

Question 64

Earliest symptom

of schistosomiasis

Answer 64

Mild itching/papular dermatitis at sign of parasite penetration 12-24 hours after infection
“Swimmer’s itch”

Question 65

Symptoms of chronic schistosomiasis infestation

Answer 65

Tends to occur more in persons from endemic areas
Depends on the species
S. mansoni and S. Japonicum (as they lodge in the liver vessels);
- diarrhoea/constipation
- blood in stool
- abdo pain
- colonic polyposis/portal hypertension, pulmonary hypertension can occur

S. haemotobium lodges in vessels of LUT

• dysuria/cystitis
• haematuria
• long term: infertility, ureteral obstruction, hydronephrosis, bladder cancer

Question 66

Serious complications of acute schistosomiasis disease

Answer 66

Myocarditis
Pericarditis
Neurological manifestations (seizures, motor paralysis, ataxia)

Question 67

Diagnosis of schistosomiasis

Answer 67

In acute disease: based on exclusion of other infections and a thorough exposure history

Chronically:

• test stool and/or END sample urine for ova
• can also check serology, but can be difficult to interpret

Question 68

Who should be tested for chronic schistosomiasis infestation

Answer 68

All travellers to endemic areas who have had ANY freshwater exposure (3 months after return)
Migrants from endemic areas

Question 69

Treatment of schistosomiasis

Answer 69

Acute disease:
- supportive, need to discuss with ID specialist (mostly prednisolone, +/- antimalarials but they may worsen disease, so need to check with specialist!)

Periodic serological testing should then be undertaken

Chronic:
Praziquantel 20mg/kg per dose, 2 doses 4h apart
If had positive urine/stool, repeat samples 2-3 months after treatment
Serological testing should not be used as proof of cure
CBE can be repeated >12 weeks to ensure eosinophilia resolves

Question 70

Countries where Japanese Encephalitis occurs

Answer 70

Most Asian countries (except Singapore), Papua New Guinea, outer Torres Strait Islands of Australia

Occurs particularly in rural areas

Question 71

Months of most likely transmission of Japanese Encephalitis

Answer 71

India and SouthEast Asia (including Bali): year round
May-September in China, Korea and Japan
March - October in the further sound subtropical areas

Question 72

morbidity and mortality rate in Japanese Encephalitis

Answer 72

30% fatality rate of symptomatic infections in humans

60% of survivors (especially children) will have permanent neurological sequelae

Question 73

Risk factors of contracting Japanese Encephalitis

Answer 73

Dawn, dusk, or night visits to rice growing areas
Living in villages near rice paddies and farm animals
Soldiers/aid workers/missionaries/students/researchers in endemic areas in the wet season

Question 74

Risk factors for developing severe infection with japanese encephaltisi

Answer 74

Age >50y or child
Dual neurological infection (e.g. with mumps)
Compromised blood-brain barrier (e.g. Cochlear implants, shunts)
Pregnancy
Chronic conditions (solid organ transplants, hypertension, CVD, DM, CKD)

Question 75

Risk of Japanese encephalitis while pregnant

Answer 75

Risk of miscarriage in the first and second trimesters

Question 76

Pathogen/mosquito responsible for japanese encephalitis

Answer 76

Culex mosquito + specific flavivirus.
Enzootic cycle between vertebrate hosts (mostly pigs and egrets) and the mosquito

Feeds outdoors from dusk to dawn and breeds in flooded rice paddies and marsh environments

No person-to-person transmission

Question 77

Prevention of Japanese Encephalitis

Answer 77

Mosquito precautions
Avoidance of high risk activities (e.g. visiting rice fields dusk-dawn)
Advice about the disease to traveller to endemic areas
Advice about risks and benefits of vaccination

Question 78

Vaccines available for Japanese Encephalitis

Answer 78

Jespect/Ixiaro OR Imojev

Jespect/Ixiaro:

• inactivated vaccine
• 2 doses given 28 days apart (can try accelerated course 7 days apart if necessary)
• Approved from 18y, can be given from 2mo
• booster 1-2 years after primary course
• Safe in pregnancy
• approx $150 per dose

Imojev:

• recombinant live vaccine (attenuated strain of yellow fever virus with JE genes)
• single dose
• booster maybe needed after 5y
• booster for kids 1-2 yearsa fter primary dose
• not suitable for children <9 mo

Question 79

Clinical features of Japanese Encephalitis

Answer 79

Widespread encephalomyelitis of white matter, thalamus, brainstem and spinal cord

In adults:
- headache
- meningism
- fever
- confusion/altered consciousness
(Can present as simple febrile illness, acute flaccid paralysis or aseptic meningitis)
Children often present with seizures (75%)

Question 80

Treatment of Japanese Encephalitis

Answer 80

Supportive management only

• close observation
• fluids, analgesia, antipyretics

Question 81

Diagnosis of Japanese Encephalitis

Answer 81

Serum or CSF specific anti-JE IgM antibodies

Question 82

Highest risk countries for rabies (11)

Answer 82

India, Nepal, Sri Lanka, Thailand, Philippines, Vietnam, El Salvador, Guatemala, Peru, Colombia, Ecuador

Question 83

Factors affecting how quickly rabies virus is taken up into CNS (thus how high risk a lesion is)

Answer 83

Density of nerve endings in bitten area (highest in the hands)
Proximity of bite site to CNS (highest in the face)
Severity of bite

Question 84

Incubation period of rabies

Answer 84

Ranges from 1-12 weeks to several years - dependent on site and severity of bite

Question 85

Clinical features of Rabies

Answer 85

Prodromal symtpoms:
(Non-specific)
fever, anorexia, cough, headache myalgia, sore throat, fatigue, vomiting, anxiety/agitation/apprehension
Parasthesiae or fasciculations can occur in proximity of the wound

“Furious encephalitic rabies” - classic, most common form
- aerophobia/hydrophobia
- disorientation
- bizarre or hyperactive behaviour
- autonomic instability (hypersalivation, hyperthermia, hyperventilation)
Death occurs within 12 days

“Paralytic/dumb rabies” - 30% of cases

• more protracted and less distinctive
• loss of sensation
• weakness
• pain
• progressive flaccid paralysis

Question 86

Travel advice to prevent rabies

Answer 86

Avoid approaching stray animals
Stay aware of surroundings to avoid surprising stray dogs
Avoid carrying or eating food around monkeys
Avoid contact with bats (esp. cavers)

Question 87

Who should be offered rabies pre-exposure vaccination

Answer 87

High risk adults (veterinarians, animal handlers, wildlife officers, people living in or travelling to rabies endemic areas esp if >1 month)
Children living in or visiting rabies areas
People travelling to isolated regions with limited access to appropriate medical care

Question 88

Pre-exposure rabies vaccinations

Answer 88

Same as post-exposure vaccine but different delivery schedule
2 avail in Aus:
- Human diploid cell rabies vaccine (HDCV): inactivated virus, contains inactivated virus, neomycin and human serum albumin
- Purified chick embryo cell vaccine (PCECV): contains inactivated virus, neomycin, bovine gelatin, egg protein, chlortetracycline and amphotericin B

Both are given IM to deltoid if >12 mo
3x doses at 0, 7 and 28 days
Serological testing required for people with impaired immunity 2-3 weeks later
Safe in pregnancy

HDCV should be used for people with anaphylaxis to eggs

Question 89

Post-exposure wound care for possible rabies

Answer 89

Thorough wound cleansing and disinfection (lots of soap/detergent and water, followed by betadine)
Delay suturing where possible - infiltrate with HRIG and delay for at least several hours
ADT/Antibiotics as indicated

Question 90

Post-exposure prophylaxis to

rabies management in someone who does NOT have documented pre-exposure vaccination

Answer 90

rabies immunoglobulin should be instilled into the wound no later than 7 days after first rabies vaccine dose - give the remaining into the opposite side deltoid

Give rabies vaccine on day 0, 3, 7, 14, 28-30 (5 doses in total)

Question 91

Post-exposure rabies prophylaxis in someone who DOES have documented pre-exposure vaccination

Answer 91

Appropriate wound management
RIG not necessary
2x doses IM vaccine booster doses on days 0 and 3

Question 92

Altitude at which altitude sickness starts to occur

Answer 92

Unlikely to occur <2500m

Question 93

Large cities that travellers may not recognise are at risk of altitude sickness developing

Answer 93

Cusco, Peru (3400m)
Lhasa, Tibet (3600m)
La Paz, Bolivia (3700m)

Question 94

Physiological changes that occur with high altitude

Answer 94

Initial:

• hyperventilation
• increased sympathetic tone ( increase HR, BP and cardiac output)
• vasoconstriction of pulmonary vasculature
• cerebral vasodilation secondary to hypoxia

Later changes:

• increased EPO -> increased Hb production
• diuresis -> increased haematocrit
• decreased muscle mass
• increased vascularity

Question 95

Risk factors for altitude illness

Answer 95

• ascending to >2800m in one day
• prior history of AMS ascending >2800m
• anyone ascending >500m/day at altitudes >3000m
• Anyone with history of severe AMS or HAPE/HACE

Not related to physical fitness, alcohol, cigarettes, gender, load carried, recent respiratory illness etc.

Question 96

Absolute contraindications to high altitude travel

Answer 96

Severe COPD
Unstable asthma
Severe IHD
Severe or uncontrolled heart failure
Pulmonary hypertension
Complicated pregnancy

Question 97

Relative contraindications to high altitude travel

Answer 97

Moderate COPD
Stable angina
Previous cerebrovascular disease
Poorly controlled DM
Recurrent arrhythmias
Uncomplicated pregnancy >36 weeks gestation

Question 98

Recommendations to prevent altitude illness in travellers

Answer 98

• slow ascent to allow for acclimatisation (300-500m/day >3000m altitude)
• A day’s rest every 3-4 days
• Resting in first 48h of arriving at places of high altitude
• 24h delay after uncomplicated dive (1 week minimum after recompression therapy)

Question 99

Common high altitude conditions and other risks at high altitude

Answer 99

High altitude headache (HAH)
Acute Mountain Sickness (AMS)
High altitude cerebral oedema (HACE)
High altitude pulmonary oedema (HAPE)
DVT more common at high altitudes (same recommendations as for flying)

Question 100

Medications that can be used for the PREVENTION of altitude illness

Answer 100

High altitude headache: Ibuprofen 600mg TDS (yes, 600 is not a typo)

Acute mountain sickness: Acetazolamide 125mg BD (off label use)

High altitude pulmonary oedema: Nifedipine SR 60mg daily (either 30mg 12 hourly or 20 mg 8 hourly) - does not reduce AMS

Question 101

Presentation and immediate management of high altitude conditions:

Answer 101

HAH: headache at high altitude, settles after 10-15 minutes wit oxygen, resolves with regular NSAID and decrease in altitude

AMS: Headache within 6-36 hours of high altitude PLUS either GI upset, fatigue/weakness, dizziness, difficulty sleeping. Usually resolves with 2-4 days rest and no further altitude rise, if severe needs O2 and dexamethasone to prevent HACE

HACE: AMS symptoms 24-36 hours after high altitude arrival PLUS impaired mental state and/or ataxia. Medical emergency: immediate reduction in altitude of at least 300m, IV dex and O2

HAPE: can develop independently of AMS 2-4 days after high altitude. Cough/dyspnoea/reduced exercise tolerance/chest tightness, creps/high RR and HR, cyanosis
Urgent rapid descent of 1000m at least, O2, nifedipine