Speakers bureaus: astrazeneca, genentech

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SPEAKERS BUREAUS: ASTRAZENECA, GENENTECH

SPEAKERS BUREAUS: ASTRAZENECA, GENENTECH
RESEARCH GRANTS: NOVARTIS, GLAXOSMITHKLINE, PFIZER, MERCK
ASSOCIATE EDITOR: ANNALS OF ALLERGY, ASTHMA & IMMUNOLOGY
ASSOCIATIONS: AAAAI, ACAAI, CAAS
NO CONFLICTS OF INTEREST PERTAINING TO SUBJECT MATTER OF THIS TALK

Mucous membranes and skin of hay fever sufferers sensitive to pollen not seen in normal individuals

Mucous membranes and skin of hay fever sufferers sensitive to pollen not seen in normal individuals
Injection of pollen into animals rises neutralizing “antitoxin”
Specific precipitation of pollen extracts by patient’s serum
Pollen extract prepared by freezing and thawing, followed by ten minutes of boiling, then sealing

Believed pollen contained toxin and subcutaneous injection of pollen extract induced production of antitoxin

Believed pollen contained toxin and subcutaneous injection of pollen extract induced production of antitoxin
Phleum pratense (timothy grass) extract most potent
Sensitivity defined by conjunctival challenge
6-10 fold decrease in sensitivity could be induced by increasing doses of 3-6 sub-Q injections

Further observations on the treatment of hay fever by hypodermic inoculations of pollen vaccine. Lancet Sept 16, 1911

Further observations on the treatment of hay fever by hypodermic inoculations of pollen vaccine. Lancet Sept 16, 1911

Twenty subjects with >2 pre-seasonal injections, with final increased strength from 1.1 to 500 fold higher
15 did well; 3 considered failure, “disappointing” or inconclusive; 1 improved clinically but significant adverse reaction to highest dose; 1 from Canada with autumnal sxs

Vaccination against hay fever: Report of results during the last three years. Lancet April 25, 1914

Vaccination against hay fever: Report of results during the last three years. Lancet April 25, 1914

84 patients with English hay fever inoculated with Phleum pratense pollen preseasonally
18 in 1911; 25 in 1912; 41 in 1913
30.1% cured or insignificant sxs; 34.5% markedly improved; 23.9% minimal improvement; 11.5% no better (two patients worse)
“Patients with marked constitutional disturbances, including asthma, do better”
“Patients with an inherited tendency do better”
“Age makes no difference to the benefit derived from treatment”

1904 Dunbar & Prausnitz – Pollen “toxin” injections

1904 Dunbar & Prausnitz – Pollen “toxin” injections
1911 Noon – Prophylactic inoculations against hayfever
1911 Freeman - Further observations
1930 Freeman - “Rush” inoculations
1932 A Brown – Superiority of perennial over pre-seasonal administration of immunotherapy
1932-1935 GT Brown – Maximum dosage pollen therapy
1933 Colmes & Rackemann – Skin reactivity changes with immuotherapy

1935 Cooke, Barnard, Hebold & Stull - Serologic evidence of immunity

1935 Cooke, Barnard, Hebold & Stull - Serologic evidence of immunity
1940 Sherman, Stull & Cooke – Serologic changes in hay-fever with treatment over years
1943 Loveless - Relationship of thermostable antibody & clinical immunity
1948 Alexander, Johnson & Bukantz – Lack of correlation between thermostable antibody titer and degree of clinical protection

“Leisurely Desensitisation:” (c. 1909) single injections @ weekly intervals off-season

“Leisurely Desensitisation:” (c. 1909) single injections @ weekly intervals off-season
“inoculations were given weekly merely because our out-patients at St. Mary’s were in the habit of coming every week.”
“Intensive Desensitisation:” (c. 1924) single injections every day with increasing doses (10-20% increase)
Used initially for horse dandruff sensitive asthmatics with success
Increasingly adapted to hay-fever patients (c. 1926)

“Rush Desensitisation:” (c. 1928) multiple injections q1.5-2h throughout 14 hour day; completed in 2-4 days

“Rush Desensitisation:” (c. 1928) multiple injections q1.5-2h throughout 14 hour day; completed in 2-4 days
Patient in “hospital or some such institution” – treatment continued through symptoms of urticaria, headache, throat & nasal congestion, and treatment with adrenalin
Used in dust asthma, fish allergy, horse dander, hay-fever

A= good night

A= good night
B= local reaction
C= generalized rash
D= sneezing
E= throat & nasal congestion
F= headache & drowsy
G= restless night
H= generalized rash & eyelid swelling
I= adrenalin
?= out of hospital

Advantages of the “rush” method

Advantages of the “rush” method

Saving of time
Convenient scheduling – “one may even wait till the patient is in real distress – always a good time for getting a patient to do what he is told.”
Closer observation of reactions with more expeditious therapy
Doses can be more readily adapted

“In choosing a system of desensitisation, one need not, of course, adhere rigidly to the leisurely, intensive, or “rush” methods; an intelligent blend may serve one’s turn better.”

“In choosing a system of desensitisation, one need not, of course, adhere rigidly to the leisurely, intensive, or “rush” methods; an intelligent blend may serve one’s turn better.”
“The ‘rush’ method of desensitisation offers many advantages when used either alone or in combination with other systems. To get successful and safe results, however, it is just as necessary as ever to be cautious.”

Rhinitis Asthma

Rhinitis Asthma
*Northern grasses *Northern grasses
*Short ragweed *House dust
*Ragweed Amb a 1 *Ragweed Amb a 1
*Mountain cedar *Mountain cedar
*Birch/Alder/Hazel *Birch/Alder/Hazel
Parietaria *D. pteronyssinus
Cladosporium Cladosporium
Alternaria Alternaria
Dog dander
*Cat dander
Hymenoptera Allergy
*Venom *(1954-1984)

1954 Frankland & Augustin – First DBPC efficacy study with grass hay-fever & asthma

1954 Frankland & Augustin – First DBPC efficacy study with grass hay-fever & asthma
1965 Lowell & Franklin – First DBPC short ragweed hay-fever study
1967 Franklin & Lowell – Dosage comparison in ragweed immunotherapy
1971 Aas – First DBPC house dust asthma study
1976 Pence et al – Mountain cedar rhinitis & asthma study
1978 Warner et al – D. pteronyssinus house dust mite asthma study

Hollister-Stier

Hollister-Stier

Staphylococcus aureus 6 x108/cc; Staphylococcus albus 6 x108/cc; Streptococcus viridans/pyogenes 2 x108/cc; H. influenzae 1.5 x108/cc

Danish

S. aureus 9 x107/cc; S. viridans/pyogenes 6 x107/cc; D. pneumoniae 3 x108 /cc; H. influenzae 12.5 x108/cc; K. pneumoniae 2 x107 /cc; Neisseria 8 x107/cc

Frankland, Hughes, Gorrill, 1955: Autogenous

Frankland, Hughes, Gorrill, 1955: Autogenous
Johnstone, 1959: Autogenous, Stock, or Staphylococcal toxin
Aas et al, 1963: Stock vaccine
Barr et al, 1964: Stock vaccine

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Speakers bureaus: astrazeneca, genentech

SPEAKERS BUREAUS: ASTRAZENECA, GENENTECH

SPEAKERS BUREAUS: ASTRAZENECA, GENENTECH

RESEARCH GRANTS: NOVARTIS, GLAXOSMITHKLINE, PFIZER, MERCK

ASSOCIATE EDITOR: ANNALS OF ALLERGY, ASTHMA & IMMUNOLOGY

ASSOCIATIONS: AAAAI, ACAAI, CAAS

NO CONFLICTS OF INTEREST PERTAINING TO SUBJECT MATTER OF THIS TALK

Mucous membranes and skin of hay fever sufferers sensitive to pollen not seen in normal individuals

Mucous membranes and skin of hay fever sufferers sensitive to pollen not seen in normal individuals

Injection of pollen into animals rises neutralizing “antitoxin”

Specific precipitation of pollen extracts by patient’s serum

Pollen extract prepared by freezing and thawing, followed by ten minutes of boiling, then sealing

Believed pollen contained toxin and subcutaneous injection of pollen extract induced production of antitoxin

Believed pollen contained toxin and subcutaneous injection of pollen extract induced production of antitoxin

Phleum pratense (timothy grass) extract most potent

Sensitivity defined by conjunctival challenge

6-10 fold decrease in sensitivity could be induced by increasing doses of 3-6 sub-Q injections

Further observations on the treatment of hay fever by hypodermic inoculations of pollen vaccine. Lancet Sept 16, 1911

Further observations on the treatment of hay fever by hypodermic inoculations of pollen vaccine. Lancet Sept 16, 1911

Vaccination against hay fever: Report of results during the last three years. Lancet April 25, 1914

Vaccination against hay fever: Report of results during the last three years. Lancet April 25, 1914

1904 Dunbar & Prausnitz – Pollen “toxin” injections

1904 Dunbar & Prausnitz – Pollen “toxin” injections

1911 Noon – Prophylactic inoculations against hayfever

1911 Freeman - Further observations

1930 Freeman - “Rush” inoculations

1932 A Brown – Superiority of perennial over pre-seasonal administration of immunotherapy

1932-1935 GT Brown – Maximum dosage pollen therapy

1933 Colmes & Rackemann – Skin reactivity changes with immuotherapy

1935 Cooke, Barnard, Hebold & Stull - Serologic evidence of immunity

1935 Cooke, Barnard, Hebold & Stull - Serologic evidence of immunity

1940 Sherman, Stull & Cooke – Serologic changes in hay-fever with treatment over years

1943 Loveless - Relationship of thermostable antibody & clinical immunity

1948 Alexander, Johnson & Bukantz – Lack of correlation between thermostable antibody titer and degree of clinical protection

“Leisurely Desensitisation:” (c. 1909) single injections @ weekly intervals off-season

“Leisurely Desensitisation:” (c. 1909) single injections @ weekly intervals off-season

“inoculations were given weekly merely because our out-patients at St. Mary’s were in the habit of coming every week.”

“Intensive Desensitisation:” (c. 1924) single injections every day with increasing doses (10-20% increase)

Used initially for horse dandruff sensitive asthmatics with success

Increasingly adapted to hay-fever patients (c. 1926)

“Rush Desensitisation:” (c. 1928) multiple injections q1.5-2h throughout 14 hour day; completed in 2-4 days

“Rush Desensitisation:” (c. 1928) multiple injections q1.5-2h throughout 14 hour day; completed in 2-4 days

Patient in “hospital or some such institution” – treatment continued through symptoms of urticaria, headache, throat & nasal congestion, and treatment with adrenalin

Used in dust asthma, fish allergy, horse dander, hay-fever

A= good night

A= good night

B= local reaction

C= generalized rash

D= sneezing

E= throat & nasal congestion

F= headache & drowsy

G= restless night

H= generalized rash & eyelid swelling

I= adrenalin

?= out of hospital

Advantages of the “rush” method

Advantages of the “rush” method

“In choosing a system of desensitisation, one need not, of course, adhere rigidly to the leisurely, intensive, or “rush” methods; an intelligent blend may serve one’s turn better.”

“In choosing a system of desensitisation, one need not, of course, adhere rigidly to the leisurely, intensive, or “rush” methods; an intelligent blend may serve one’s turn better.”

“The ‘rush’ method of desensitisation offers many advantages when used either alone or in combination with other systems. To get successful and safe results, however, it is just as necessary as ever to be cautious.”

Rhinitis Asthma

Rhinitis Asthma

*Northern grasses *Northern grasses

*Short ragweed *House dust

*Ragweed Amb a 1 *Ragweed Amb a 1

*Mountain cedar *Mountain cedar

*Birch/Alder/Hazel *Birch/Alder/Hazel

Parietaria *D. pteronyssinus

Cladosporium Cladosporium

Alternaria Alternaria

Dog dander

*Cat dander

Hymenoptera Allergy

*Venom *(1954-1984)

1954 Frankland & Augustin – First DBPC efficacy study with grass hay-fever & asthma

1954 Frankland & Augustin – First DBPC efficacy study with grass hay-fever & asthma

1965 Lowell & Franklin – First DBPC short ragweed hay-fever study

1967 Franklin & Lowell – Dosage comparison in ragweed immunotherapy

1971 Aas – First DBPC house dust asthma study

1976 Pence et al – Mountain cedar rhinitis & asthma study

Northern grasses Northern grasses

Short ragweed House dust

Ragweed Amb a* 1 Ragweed Amb a* 1

Mountain cedar Mountain cedar

Birch/Alder/Hazel Birch/Alder/Hazel

Parietaria **D. pteronyssinus*

Venom (1954-1984)

**1978 Warner et al – D. pteronyssinus house dust mite asthma study**