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DYNAMICS OF DISEASE
TRANSMISSION
Dr. Sanat Rathod
Assistant Professor
GMERS Medical College
Gotri
Vadodara
2
1st - The Infectious Agent
-any disease-causing
microorganism
(pathogen)
Infectivity
Pathogenicity
Virulence
3
2nd: Source or Reservoir
• The starting point for the occurrence of a communicable
disease
• Source of infection :
• the person, animal, object or substance from which an
infectious agent passes or is disseminated to the host
(immediate source)

• RESERVOIR:
• “any person, animal, arthropod, plant, soil, or
substance, or a combination of these, in which
an infectious agent normally lives and multiplies,
on which it depends primarily for survival, and
where it reproduces itself in such a manner that
it can be transmitted to a susceptible host.
It is the natural habitat of the infectious agent.” 4
Types of Reservoirs

Human
reservoir

Animal
reservoir

Non-living
reservoir
•5
cases

•Primary case
•Index case
•Secondary cases

•Clinical cases
(mild/severe-typical/atypical)
•Sub-clinical cases
•Latent infection cases

:Type
•Incubatory
•Convalescent
•healthy

Duration:
•Temporary
•Chronic

carriers
:Portal of exit
•Urinary
•Intestinal
•Respiratory
•others

6
“A person in the population or
study group
Identified as having particular
disease, health disorder or
condition
Under investigation”

7
The clinical illness maybe mild or moderate,
typical or atypical, severe or fatal.
Epidemiologicall y, mild cases may be
mor e impor tant sour ces of
infection than severe cases because they
are ambulant and spread the infection
wherever they go, whereas severe cases
usually confined to bed.

8
Subclinical cases
Inapparent, Covert, Missed or Abortive Cases
• disease agent multiply in the host but does
not manifest by S/S.
• But contaminates the environment in the
same way as clinical cases.
•

Subclinical cases play a dominant role in maintaining the
chain of infection in the community.
9
detected only by
laboratory
tests

subclinical cases

occurs in most
infectious disease.
Eg







Rubella,
Mumps,
Polio,
Hepatitis A and B,
Influenza,
Diphtheria
10
Latent infection
• infectious agent lies in a non-infectious formdormant within the host without symptoms with
no shedding (and often without demonstrable
presence in blood, tissues or bodily secretions
of the host)



eg.

HSV and VZV: nerve ganglia cells,
CMV: kidney and salivary glands cells,

EBV: lymphocytes
11


Index Case

◦ Person that comes to the
attention of public health
authorities



Primary Case

◦ First case of a communicable
disease introduced into the
population unit bring studied
◦ Attack rate



Secondary Case

◦ Person who acquires the disease
from an exposure to the primary
case
◦ Secondary attack rate
12
Carriers


An infected person or animal that harbors a
An infected person or animal that harbors a
specific infectious agent in the absence of
specific infectious agent in the absence of
discernible (visible) clinical disease and
discernible (visible) clinical disease and
serves as a potential source of infection to
serves as a potential source of infection to
others
others

Reason :

due to inadequate treatment or immune response
the disease agent is not completely eliminated
leading to a carrier state.

13
Three elements in a carrier state:

14
CARRIERS
As a rule carriers are less infectious than cases,
but epidemiologically, they are more
dangerous than cases
because
◦ escape recognition
◦ continuing to live a normal life among population
or community
◦ readily infect the susceptible individuals
◦ over a wider area and longer period of time under
favorable conditions.

15
Classification of Carrier

Incubatory

Carriers: those who shed the

infectious agent during the incubation period.
This usually occurs during last few days of IP
 Measlesthe period of communicability is 4 days before the rash.
 Mumpsusually 4-6 days before onset of symptoms
 Polio7-10 days before onset of symptoms
 Hepatitis Bfor a month before jaundice
 Pertusis
 Influenza
 Diphtheria

16
Carrier May Be Classified :
By Type

Convalescent Carriers:

 those who continue to shed the disease agent during the
period of convalescence
 In the disease, clinical recovery does not coincide with
bacteriological recovery.
 Serious threat to HH members
 Highlights importance of bacteriological surveillance of
carriere state after recovery
◦
◦
◦
◦
◦

typhoid fever
cholera,
diphtheria,
bacillary dysentery
pertusis
17
Carrier may be classified :
BY TYPE

Healthy Carriers:
 victims

of subclinical infection who have
developed carrier state without suffering from
overt disease, but are nevertheless shedding the
disease agent
◦
◦
◦
◦
◦

poliomyelitis,
cholera,
meningococcal meningitis,
salmonellosis,
diphtheria.

Note:- Person whose infection remains subclinical may or may not act as
carrier (eg.- in polio inf may remain subclinical but person act as temp carrier
due to shedding of virus in stool..while TB most of us with +ve Mt, do not
disseminate bacillie- so not labelled as carrier.
18
Temporary

carriers are those who shed the
infectious agent for short period of time.

Chronic

carriers are those who excretes the
infectious agent for indefinite periods

19
Chronic carriers
Chronic carriers are far more important sources of
infection than cases.
The longer the carrier state, the greater the risk of
community-- reintroduce disease into areas which
are otherwise free of infection
The duration of the carrier state varies with the
disease.
 In typhoid fever and hepatitis B, the chronic
carrier state may last for several years.
 In chronic dysentery it may last for year or longer.
 In diphtheria, the carrier state is associated with
infected tonsils, in typhoid fever with gall bladder
disease.
20






Mary Mallon (1869 –1938), better
known as Typhoid Mary, was the
first person in the US identified as
an asymptomatic carrier of the
pathogen associated with
typhoid fever.
She was presumed to have
infected some 50 people, three of
whom died, over the course of her
career as a cook.
She was forcibly isolated twice by
public health authorities and died
after a total of nearly three
decades in isolation.
21
Carrier classified :
By Portal Of Exit of Infectious Agent



Respiratory carrier: e.g. influenza



Fecal (intestinal) carrier: e.g. typhoid, cholera



Blood carrier: e.g. hepatitis B and HIV



Urinary : e.g. Typhoid



sexual Carrier: gonococcus and HIV

22
Animal reservoirs
• infection that is transmissible under
natural conditions from animals to
man.
• e.g.
–
–
–
–
–

Bacterial: Leptospira, plague from Rat.
Viral : Rabies from dog.
Protozoa: Leishmaniasis from dog.
Helminths : Hydatid disease from dog
Tape worms : Cattle , Pig.

•23
Reservoir in non-living
things
Some organisms are able to
survive and multiply in
nonliving environments
such as soil and water
Clostridium that causes tetanus
and botulism can survive many
years in the soil
Hookworms deposit their eggs
into the soil
Water contaminated by human
or animal feces cause GI tract
disease (list includes bacteria,
viruses, protozoa)

•24
3rd - The Portal of Exit
• Route of escape of the pathogen from
the reservoir-IA enters into surrounding
reservoir
env-transfer to host at their portal of entry

Examples:

respiratory secretions,
GI
blood exposure,
breaks in skin

25
4th –Mode of Transmission

Direct
transmission
Direct contact
Droplet infection
Contact with soil
Inoculation into skin or mucosa
vertical

Indirect
transmission
Vehicle-borne
:Vector-borne •

Air-borne
Fomite-born
Unclean hands
and fingers
26
Direct Transmission

•27
Direct Contact
•Inf spread by direct contact of
skin-skin, skin mucosa, mucosamucosa of same or other person

•by touching, kissing,,
bites, or sexual intercourse
•Direct & immediate transfer of IA
from reserviour –host (no intermediate
agency)

•So it introduces larger dose of IA
•No time interval of survival in
environment..
•Overcrowded place or where
place with lack of ventilation

Scabies
Pediculosis

STD’s
Skin/eye inf
leprosy
•28
Droplet spread:
•

Direct projection of
droplets of
saliva/nasopharynge
al secretion by
Sneezing, Speaking,
Coughing

•

Droplets directly
impinge on
conjunctiva, nasal
mucosa or skin

•29
•
•
•
•

H1N1
Tubercle bacilli
Measles •30
Chickenpox
Inoculation:
Pathogen injected into tissues.

•
–
–

Tetanus spores
Arboviruses (Insects).

•31
Vertical transmission

Transplacental

 To R C H
 HIV
 HBV
15

•32
Indirect Transmission
5 ‘F’

food, flies, fomite, finger, fluid

33
Vehicle transmission
•
•

Water: Cholera, H A V , H E V, Typhoid etc.
FOOD: Staphylococci, Cl. Botulinum.

•
•

Blood/serum-HIV, HBV,HCV
Organ-cmv




Clustering of cases
Distance bw secondary cases more
Common source can be traced
34
Vectorinsects
Mechanical
Hf

Biological

Diarrhea
Dysentery
Typhoid
Trachoma

Propagative
Only multiplication
No developmental
Plague bacilli in rat
flea

Cyclo propagative
Multiplication
developmental
Malaria parasites in
mosquito

Cyclodevelopmental
No multiplication
developmental
Filaria parasite
In mosquito

35
Trans-ovarian transmission
 Inf agent vertical transmitted from female
mosquito to her progeny
◦
◦
◦
◦
◦

Scrub typhus
Rickettsial pox
Indian tick typhus
Q fever
RMSF

Trans-stadial transmission Lyme disease, infects tick vector as a larva, and the
infection is maintained when it molts to a nymph and
later develops as an adult
36
 host

feeding preference
 infectivity-ability to transmit disease agent
 susceptibility – ability to become infected
 survival rate of vectors in environment
 Domesticity
 Seasonal factors…

37
Fomites :
Contaminated Nonliving Objects like Cup, towel,
napkin, linen, Clothing, glass, Toys, Pencils, door handle,
surgical instruments, syringes, dressing materials…

Ex:

Diphtheria,
Trachoma
influenza
scabies
38
5th - The Portal of Entry
-route through which the
pathogen enters its new
host

•39
Respiratory System
io
t
la
a
h n
in

 Upper respiratory tract
Diphtheria
 Lower respiratory tract
Tuberculosis

•40
Gastrointestinal System

Infectious agent excreted in faeces
& transmitted to the oral
portal of entry through
􀂃 contaminated food, water, milk,
drinks
􀂃 hands
•
•
•
•
•
•

􀁺 Typhoid fever
􀁺 Shigella
􀁺 Cholera
􀁺 Polio
􀁺 Rotavirus
􀁺 Hepatitis A, Hepatitis E

ingestion

Feco-Oral Route

•41
Se
co x
nt ua
ac l
t

Urinary & Reproductive
Tracts
Gonorrhea
Syphilis
HIV

•42
Breaks in Protective Skin
Barrier
 Percutaneous
Leptospirosis
 Percutaneous
(bite of arthropod)
Yellow fever

•43
6th - The Susceptible Host
A person or an animal that afford
lodgment to an infectious agent
under natural conditions.
•Accepts the pathogen

44

•The support of pathogen life & its
reproduction depend on the degree of the
host’s resistance.
•Cancer Patients
•HIV-AIDS Patients
•Transplant
Patients
•On steroids..
•Infant & Elderly
Patients

45
HOST

Obligate host :
hos

the only host

Eg: Man in measles & typhoid
Primary /definitive host: in which
parasite attains maturity or passes
its sexual stage
Secondary or intermediate hosts:
the parasite is in a larval or asexual
state

•46
Life cycle
Sporozoits

Liver
Mature

Salivary
Gland

Marozoits

RBC

Schizont

Oocyte

Mature

Ring Trophozoits

Ookinete
Zygote

Mosquito

Exflagellation

Gametocyte
Male / Female
THE TIME INTERVAL BETWEEN INVASION BY
AN INFECTIOUS AGENT AND APPEARANCE OF
THE FIRST SIGN OR SYMPTOM OF THE
DISEASE IN QUESTION
 DOSE

OF INOCULUM
 SITE OF MULTIFICATION
 RATE OF MULTIFICATION
 HOST DEFENCE MECHANISM
No of cases
Median incubation time

15

2

3

10
5
0
1 2 3 4 5 6 7 8 9 10 11 12 1314 15 16 17 18 19 20 21 22

Probable exposure

50%

1

50%

Time
Period From Disease Initiation To
Disease Detection
For NCDs
GENERATION TIME
INTERVAL OF TIME BETWEEN RECEIPT OF
INFECTION BY A HOST AND MAXIMAL
INFECTIVITY OF THAT HOST
No of cases
10

Generation
time

5

0
1

2 3

4

5

6 7

8

9 10 11 12 13 14 15 16 17 18 19 20 21 22 Zeit
THE GAP IN TIME BETWEEN
THE ONSET OF THE
PRIMARY CASE AND THE
SECONDARY CASE
It is defined as the time during which
an infectious agent may be transferred
directly or indirectly from an infected
person to another person, from an
infected animal to man , or from an
infected person to an animal, including
arthropods
Ate the food (exposed)
Did not eat the food (not exposed)
Ill
Well
Total
Well
Total
Attack
Ill
Attack
Rate
Rate
10

3

13

76%

7

4

Attack Rate = Ill / (Ill + Well) x 100 during a time period

Attack rate = (10/13) x 100 = 76%
( 7/11) x 100 = 64%

11

64%
It is defined as the number of exposed
persons developing the disease within the
range of the incubation period, following
exposure to the primary case
Total number of cases – initial case(s)

SAR (%) =

Number of susceptible persons in the group –
initial case(s)

x 100



Used to estimate to the spread of disease in a
family, household or other group environment.



Measures the infectivity of the agent and the
effects of prophylactic agents (e.g. vaccine)
58
Thank You

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Dynamics of disease transmission

  • 1. DYNAMICS OF DISEASE TRANSMISSION Dr. Sanat Rathod Assistant Professor GMERS Medical College Gotri Vadodara
  • 2. 2
  • 3. 1st - The Infectious Agent -any disease-causing microorganism (pathogen) Infectivity Pathogenicity Virulence 3
  • 4. 2nd: Source or Reservoir • The starting point for the occurrence of a communicable disease • Source of infection : • the person, animal, object or substance from which an infectious agent passes or is disseminated to the host (immediate source) • RESERVOIR: • “any person, animal, arthropod, plant, soil, or substance, or a combination of these, in which an infectious agent normally lives and multiplies, on which it depends primarily for survival, and where it reproduces itself in such a manner that it can be transmitted to a susceptible host. It is the natural habitat of the infectious agent.” 4
  • 6. cases •Primary case •Index case •Secondary cases •Clinical cases (mild/severe-typical/atypical) •Sub-clinical cases •Latent infection cases :Type •Incubatory •Convalescent •healthy Duration: •Temporary •Chronic carriers :Portal of exit •Urinary •Intestinal •Respiratory •others 6
  • 7. “A person in the population or study group Identified as having particular disease, health disorder or condition Under investigation” 7
  • 8. The clinical illness maybe mild or moderate, typical or atypical, severe or fatal. Epidemiologicall y, mild cases may be mor e impor tant sour ces of infection than severe cases because they are ambulant and spread the infection wherever they go, whereas severe cases usually confined to bed. 8
  • 9. Subclinical cases Inapparent, Covert, Missed or Abortive Cases • disease agent multiply in the host but does not manifest by S/S. • But contaminates the environment in the same way as clinical cases. • Subclinical cases play a dominant role in maintaining the chain of infection in the community. 9
  • 10. detected only by laboratory tests subclinical cases occurs in most infectious disease. Eg       Rubella, Mumps, Polio, Hepatitis A and B, Influenza, Diphtheria 10
  • 11. Latent infection • infectious agent lies in a non-infectious formdormant within the host without symptoms with no shedding (and often without demonstrable presence in blood, tissues or bodily secretions of the host)  eg.  HSV and VZV: nerve ganglia cells, CMV: kidney and salivary glands cells,  EBV: lymphocytes 11
  • 12.  Index Case ◦ Person that comes to the attention of public health authorities  Primary Case ◦ First case of a communicable disease introduced into the population unit bring studied ◦ Attack rate  Secondary Case ◦ Person who acquires the disease from an exposure to the primary case ◦ Secondary attack rate 12
  • 13. Carriers  An infected person or animal that harbors a An infected person or animal that harbors a specific infectious agent in the absence of specific infectious agent in the absence of discernible (visible) clinical disease and discernible (visible) clinical disease and serves as a potential source of infection to serves as a potential source of infection to others others Reason : due to inadequate treatment or immune response the disease agent is not completely eliminated leading to a carrier state. 13
  • 14. Three elements in a carrier state: 14
  • 15. CARRIERS As a rule carriers are less infectious than cases, but epidemiologically, they are more dangerous than cases because ◦ escape recognition ◦ continuing to live a normal life among population or community ◦ readily infect the susceptible individuals ◦ over a wider area and longer period of time under favorable conditions. 15
  • 16. Classification of Carrier Incubatory Carriers: those who shed the infectious agent during the incubation period. This usually occurs during last few days of IP  Measlesthe period of communicability is 4 days before the rash.  Mumpsusually 4-6 days before onset of symptoms  Polio7-10 days before onset of symptoms  Hepatitis Bfor a month before jaundice  Pertusis  Influenza  Diphtheria 16
  • 17. Carrier May Be Classified : By Type Convalescent Carriers:  those who continue to shed the disease agent during the period of convalescence  In the disease, clinical recovery does not coincide with bacteriological recovery.  Serious threat to HH members  Highlights importance of bacteriological surveillance of carriere state after recovery ◦ ◦ ◦ ◦ ◦ typhoid fever cholera, diphtheria, bacillary dysentery pertusis 17
  • 18. Carrier may be classified : BY TYPE Healthy Carriers:  victims of subclinical infection who have developed carrier state without suffering from overt disease, but are nevertheless shedding the disease agent ◦ ◦ ◦ ◦ ◦ poliomyelitis, cholera, meningococcal meningitis, salmonellosis, diphtheria. Note:- Person whose infection remains subclinical may or may not act as carrier (eg.- in polio inf may remain subclinical but person act as temp carrier due to shedding of virus in stool..while TB most of us with +ve Mt, do not disseminate bacillie- so not labelled as carrier. 18
  • 19. Temporary carriers are those who shed the infectious agent for short period of time. Chronic carriers are those who excretes the infectious agent for indefinite periods 19
  • 20. Chronic carriers Chronic carriers are far more important sources of infection than cases. The longer the carrier state, the greater the risk of community-- reintroduce disease into areas which are otherwise free of infection The duration of the carrier state varies with the disease.  In typhoid fever and hepatitis B, the chronic carrier state may last for several years.  In chronic dysentery it may last for year or longer.  In diphtheria, the carrier state is associated with infected tonsils, in typhoid fever with gall bladder disease. 20
  • 21.    Mary Mallon (1869 –1938), better known as Typhoid Mary, was the first person in the US identified as an asymptomatic carrier of the pathogen associated with typhoid fever. She was presumed to have infected some 50 people, three of whom died, over the course of her career as a cook. She was forcibly isolated twice by public health authorities and died after a total of nearly three decades in isolation. 21
  • 22. Carrier classified : By Portal Of Exit of Infectious Agent  Respiratory carrier: e.g. influenza  Fecal (intestinal) carrier: e.g. typhoid, cholera  Blood carrier: e.g. hepatitis B and HIV  Urinary : e.g. Typhoid  sexual Carrier: gonococcus and HIV 22
  • 23. Animal reservoirs • infection that is transmissible under natural conditions from animals to man. • e.g. – – – – – Bacterial: Leptospira, plague from Rat. Viral : Rabies from dog. Protozoa: Leishmaniasis from dog. Helminths : Hydatid disease from dog Tape worms : Cattle , Pig. •23
  • 24. Reservoir in non-living things Some organisms are able to survive and multiply in nonliving environments such as soil and water Clostridium that causes tetanus and botulism can survive many years in the soil Hookworms deposit their eggs into the soil Water contaminated by human or animal feces cause GI tract disease (list includes bacteria, viruses, protozoa) •24
  • 25. 3rd - The Portal of Exit • Route of escape of the pathogen from the reservoir-IA enters into surrounding reservoir env-transfer to host at their portal of entry Examples: respiratory secretions, GI blood exposure, breaks in skin 25
  • 26. 4th –Mode of Transmission Direct transmission Direct contact Droplet infection Contact with soil Inoculation into skin or mucosa vertical Indirect transmission Vehicle-borne :Vector-borne • Air-borne Fomite-born Unclean hands and fingers 26
  • 28. Direct Contact •Inf spread by direct contact of skin-skin, skin mucosa, mucosamucosa of same or other person •by touching, kissing,, bites, or sexual intercourse •Direct & immediate transfer of IA from reserviour –host (no intermediate agency) •So it introduces larger dose of IA •No time interval of survival in environment.. •Overcrowded place or where place with lack of ventilation Scabies Pediculosis STD’s Skin/eye inf leprosy •28
  • 29. Droplet spread: • Direct projection of droplets of saliva/nasopharynge al secretion by Sneezing, Speaking, Coughing • Droplets directly impinge on conjunctiva, nasal mucosa or skin •29
  • 31. Inoculation: Pathogen injected into tissues. • – – Tetanus spores Arboviruses (Insects). •31
  • 32. Vertical transmission Transplacental  To R C H  HIV  HBV 15 •32
  • 33. Indirect Transmission 5 ‘F’ food, flies, fomite, finger, fluid 33
  • 34. Vehicle transmission • • Water: Cholera, H A V , H E V, Typhoid etc. FOOD: Staphylococci, Cl. Botulinum. • • Blood/serum-HIV, HBV,HCV Organ-cmv    Clustering of cases Distance bw secondary cases more Common source can be traced 34
  • 35. Vectorinsects Mechanical Hf Biological Diarrhea Dysentery Typhoid Trachoma Propagative Only multiplication No developmental Plague bacilli in rat flea Cyclo propagative Multiplication developmental Malaria parasites in mosquito Cyclodevelopmental No multiplication developmental Filaria parasite In mosquito 35
  • 36. Trans-ovarian transmission  Inf agent vertical transmitted from female mosquito to her progeny ◦ ◦ ◦ ◦ ◦ Scrub typhus Rickettsial pox Indian tick typhus Q fever RMSF Trans-stadial transmission Lyme disease, infects tick vector as a larva, and the infection is maintained when it molts to a nymph and later develops as an adult 36
  • 37.  host feeding preference  infectivity-ability to transmit disease agent  susceptibility – ability to become infected  survival rate of vectors in environment  Domesticity  Seasonal factors… 37
  • 38. Fomites : Contaminated Nonliving Objects like Cup, towel, napkin, linen, Clothing, glass, Toys, Pencils, door handle, surgical instruments, syringes, dressing materials… Ex: Diphtheria, Trachoma influenza scabies 38
  • 39. 5th - The Portal of Entry -route through which the pathogen enters its new host •39
  • 40. Respiratory System io t la a h n in  Upper respiratory tract Diphtheria  Lower respiratory tract Tuberculosis •40
  • 41. Gastrointestinal System Infectious agent excreted in faeces & transmitted to the oral portal of entry through ô€‚ƒ contaminated food, water, milk, drinks ô€‚ƒ hands • • • • • • ô€ş Typhoid fever ô€ş Shigella ô€ş Cholera ô€ş Polio ô€ş Rotavirus ô€ş Hepatitis A, Hepatitis E ingestion Feco-Oral Route •41
  • 42. Se co x nt ua ac l t Urinary & Reproductive Tracts Gonorrhea Syphilis HIV •42
  • 43. Breaks in Protective Skin Barrier  Percutaneous Leptospirosis  Percutaneous (bite of arthropod) Yellow fever •43
  • 44. 6th - The Susceptible Host A person or an animal that afford lodgment to an infectious agent under natural conditions. •Accepts the pathogen 44 •The support of pathogen life & its reproduction depend on the degree of the host’s resistance.
  • 46. HOST Obligate host : hos the only host Eg: Man in measles & typhoid Primary /definitive host: in which parasite attains maturity or passes its sexual stage Secondary or intermediate hosts: the parasite is in a larval or asexual state •46
  • 48. THE TIME INTERVAL BETWEEN INVASION BY AN INFECTIOUS AGENT AND APPEARANCE OF THE FIRST SIGN OR SYMPTOM OF THE DISEASE IN QUESTION
  • 49.  DOSE OF INOCULUM  SITE OF MULTIFICATION  RATE OF MULTIFICATION  HOST DEFENCE MECHANISM
  • 50.
  • 51. No of cases Median incubation time 15 2 3 10 5 0 1 2 3 4 5 6 7 8 9 10 11 12 1314 15 16 17 18 19 20 21 22 Probable exposure 50% 1 50% Time
  • 52. Period From Disease Initiation To Disease Detection For NCDs
  • 53. GENERATION TIME INTERVAL OF TIME BETWEEN RECEIPT OF INFECTION BY A HOST AND MAXIMAL INFECTIVITY OF THAT HOST No of cases 10 Generation time 5 0 1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17 18 19 20 21 22 Zeit
  • 54. THE GAP IN TIME BETWEEN THE ONSET OF THE PRIMARY CASE AND THE SECONDARY CASE
  • 55. It is defined as the time during which an infectious agent may be transferred directly or indirectly from an infected person to another person, from an infected animal to man , or from an infected person to an animal, including arthropods
  • 56. Ate the food (exposed) Did not eat the food (not exposed) Ill Well Total Well Total Attack Ill Attack Rate Rate 10 3 13 76% 7 4 Attack Rate = Ill / (Ill + Well) x 100 during a time period Attack rate = (10/13) x 100 = 76% ( 7/11) x 100 = 64% 11 64%
  • 57. It is defined as the number of exposed persons developing the disease within the range of the incubation period, following exposure to the primary case
  • 58. Total number of cases – initial case(s) SAR (%) = Number of susceptible persons in the group – initial case(s) x 100  Used to estimate to the spread of disease in a family, household or other group environment.  Measures the infectivity of the agent and the effects of prophylactic agents (e.g. vaccine) 58

Editor's Notes

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