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You are here: Parliament home page > Parliamentary business > Publications and Records > Lords
Publications > Lords Hansard > Daily Hansard
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Written Answers
Thursday, 9th October 2003.
Whether they are now able to respond in full to the Written Question tabled by the Lord Morris of
Manchester on 22 January (HL 1248) on the vaccines used during the 199091 Gulf War.[HL4737]
The Parliamentary Under-Secretary of State, Ministry of Defence (Lord Bach): I wrote to you on 9 October, and the full text of my letter is
as follows:
"Further to my letter of 17 September (reference: D/MIN(DP)/WB PQ 1280N), I am writing in answer to your Parliamentary
Question of 4 February (Official Report, Col. WA 26) about the medical countermeasures used to protect our personnel during
the 199091 Gulf Conflict. Again, I would like to say how sorry I am that you have had to wait for so long for me to do so.
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You asked about the anthrax vaccine personnel received in 1991. At Annex A, I have set out a detailed history of our use of
the vaccine, the guidance accompanying its use and how this has evolved. As you will see, anthrax vaccine has been licensed
in the UK since 1979. The statement referred to by Lord Hunt (Official Report, 20 January 2003, WA 79, that the anthrax
"vaccine should be used alone") was not in place in 1991 and was not included in the anthrax vaccine product licence until
1998. The anthrax vaccine patient information leaflet (PIL) was not introduced until April 1999.
You also asked whether any other vaccines administered in 199091 were to be "used alone". The table at Annex B lists the
main vaccines offered for the 199091 Gulf conflict and summarises the information currently available regarding
co-administration. Furthermore, at the time of the conflict, a joint service publication provided guidance to service medical
staff on vaccinations, including the need to ensure that the individual to be vaccinated was not undergoing radiotherapy or
treatment with corticosteroids and that the appropriate time interval after any previous immunisation had elapsed.
As you know, personal medical records (F Med 4) were generally not taken to the Gulf during the 199091 conflict, and were
therefore unavailable for the recording of vaccination details. However, the names of those who received vaccinations should
have been recorded on temporary nominal rolls compiled in theatre. Whenever possible, details should also have been
recorded on form B Med 27, but many personnel who deployed to the Gulf did not carry these documents. The details
The nerve agent pre-treatment sets (NAPS) tablets designed to protect troops in the event of exposure to chemical warfare
agents each contained pyridostigmine bromide. The instructions for taking NAPS tablets were not subject to a restriction on
co-administration and never have been.
In my Written Answer to Lord Clement-Jones (Official Report, 7 March 2003, Col. WA 134), I undertook to publish this letter
to you in the Official Report. This was confirmed in my letter to you of 25 March (reference: D/MIN(DP)/WB 1105/03/C) and
is in hand. I have also arranged for a copy of this letter to be placed in the Library of the House and one to be sent to Lord
Clement-Jones." Annex A Administration of Anthrax Vaccine offered to UK Military Personnel1990 to 2003 Background 1.
Anthrax is an infectious disease that can kill. It has a number of characteristics that make it an obvious choice as a biological
weapon (BW). The best single way to protect against many diseases is via immunisation but no vaccine guarantees absolute
protection. An anthrax vaccine has been produced in the UK by the Centre for Applied Microbiology and Research (CAMR) 1
since 1956. It has been used routinely to protect those at risk from anthrax since 1963 and has been licensed in the UK since
26 November 1979. Many thousands of people, including laboratory workers, veterinary surgeons, abattoir workers and
military personnel, have been immunised. The anthrax vaccine used in the UK is a sterile product made from a type of anthrax
that does not cause the disease. It does not contain any anthrax bacteria and it is therefore impossible to contract anthrax from
the vaccine. August 1990 2. When Iraq invaded Kuwait in August 1990, an international coalition was formed to which the
UK contributed Armed Forces, initially to prevent any further Iraqi aggression and subsequently to liberate Kuwait. The UK
military threat assessment was that Iraq had a BW capability that included the ability to use anthrax as a weapon. It was
therefore necessary for the Ministry of Defence (MoD) to provide the best available protection for its personnel deploying to
the region.
CAMR's predecessor was the Microbiological Research Establishment. CAMR is now a component part of the Health
Protection Agency which is a new Special Health Authority, established on 1 April 2003.
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The vaccine was not however recommended for use in adults and it was not licensed for use as an adjuvant 5 to anthrax
vaccine. There were competing demands on this source of pertussis vaccine and MoD's full requirement could not be met by
Wellcome. A French manufacturer, Institut Merieux (now Aventis Pasteur MSD), was identified which had sufficient stock
available. NovemberDecember 1990 4. In November 1990, MoD placed an order, through the Procurement Unit of the
Department of Health (DH), for 40,000 doses 6 of Institut Merieux pertussis vaccine. This vaccine was not licensed for use in
the UK but was in France as Vaxicoq. At the recommendation of the DH, the UK's National Institute for Biological Standards
and Control (NIBSC) 7 carried out toxicity tests on the imported pertussis vaccine and reported that the test results showed the
batches to be within specifications according to procedures used at NIBSC as specified in the release criteria of the Product
Licence for paediatric vaccine. 5. In late 1990, the NIBSC also tested the effects of administering anthrax alone, pertussis
alone and both vaccines simultaneously in mice 8 and in guinea pigs 9 . Staff at NIBSC had not been asked by MoD to
undertake this work, but had deduced that MoD was planning to use pertussis as an adjuvant and therefore decided that a
check for interactions might be helpful. 6. The initial screening test experiment undertaken at NIBSC used 1 standard human
dose (SHD) of vaccines. In a mouse, a SHD of vaccine equates to approximately 160 times the human(10) equivalent on the
basis of body weight.
Turnbull et al, "Protection conferred by microbiologically-supplemented UK and purified PA vaccines", Proceedings of the
International Workshop on Anthrax, Winchester, April 1113 1989: pp8991. Salisbury Medical Bulletin, Special Supplement,
No. 68.
NIBSC is the UK's Official Medicines Control Laboratory for biological medicines.
Balb/c mice.
(10) Pertussis given to infants from 2 months of age. Average male infant at age 2 months = 4kg, laboratory mouse = 25gms.
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1997 paper made clear, there is no material on the MoD departmental record which shows whether the NIBSC's research
findings were taken into account by MoD when formulating the policy on the use of pertussis vaccine, although the general
issue of possible side effects was addressed in guidance concerning the MoD's anti-BW immunisation programme. 2 January
1991End March 1991 9. MoD's anti-BW immunisation programme, which included co-administration of anthrax and
pertussis vaccine, began on 2 January 1991 and ended on about 20 March 1991. The vaccines were to be co-administered at an
initial date, then at three weeks and a third dose given at seven weeks. On each occasion, a 0.5ml anthrax vaccine
intramuscular dose was to be administered by injection into the deltoid muscle, accompanied by an intramuscular injection
into an adjacent site on the same deltoid muscle of 0.5ml of pertussis vaccine. The prescribed primary dosing schedule in
1991, as now, involves four doses of vaccinea first injection, a second three weeks after the first, a third three weeks after
the second and a fourth six months after the third. Using this protracted thirty-two week immunisation schedule would have
risked leaving personnel unprotected during the 199091 Gulf conflict, hence the requirement to devise ways of inducing
immunity to anthrax more rapidly. A paper(12) published by the MoD in January 2000 sets out further information on how the
anti-BW immunisation programme was implemented.
(11) MoD paper: Background to the Use of Medical Countermeasures to Protect British Forces during the Gulf War
(Operation GRANBY) dated October 1997. See: http://www.mod.uk/issues/gulfwar/info/medical/mcm/htm
(12) MoD paper: Implementation Of The Immunisation Programme Against Biological Warfare Agents For UK Forces During
the Gulf Conflict 19901991 dated 20 January 2000. See: http://www.mod.uk/issues/gulfwar/info/medical/bwa/ch1.htm
"We now have the re-test results from CAMR and also have completed our own toxicity tests. The results of toxicity testing
are satisfactory and show no evidence of any increase in acute specific or general toxicity. The tests used provide no
information on long term toxicity, however. There is evidence of some decline in potency as reflected by the protective activity
in guinea-pigs. Nevertheless the vaccine still retains protective activity although it is not possible to estimate how this would
relate to the response in human subjects. No studies were done on the effect of co-administering the vaccine with other
preparations and such a practice cannot be recommended.
Taking these observations into account, these vaccine batches appear to be within specification although it should be noted that
experience with product of this age is very limited. I would not recommend extension of shelf life beyond November 1998."
12. This precautionary advice to the MCA was given in the light of the NIBSC work on simultaneous administration of
anthrax and pertussis vaccines undertaken in late 1990. Account was taken too of the age of the vaccine which had been
manufactured in 1991. 13. The next day4 February 1998the MCA issued an approval letter to the DH for a variation to
PL 01511/0037, extending the shelf-life for anthrax vaccine batches 348/E, 349/E, 350/E and 351/E to the end of November
1998, and stated in their variation letter to DH: "The vaccine to be used alone. There is no evidence for safe use in
combination with other vaccines or medicinal products" which is a little clearer than the NIBSC letter. The NIBSC letter was
copied to CAMR and DH. At some point on or before 17 February 1998, the MCA letter was also copied to CAMR.
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with interactions with other vaccines; these would likely be local rather than ill-health manifestations." In any case, the AGMC
did not recommend the use of an adjuvant on this occasion. MoD Ministers subsequently accepted the recommendation of the
AGMC that UK forces due to deploy should again be offered immunisation against anthrax, with no adjuvant. 17 February
1998 15. On 17 February 1998, following discussion with a member of staff at the MoD's Medical Supplies Agency
(MSA)(14), the Head of Regulatory Affairs at CAMR faxed the NIBSC letter of 3 February 1998 and the MCA letter of 4
February 1998 to MSA. The main purpose of the fax was to notify the MSA that the MCA had granted a shelf life extension to
anthrax vaccine batches 348/E, 349/E, 350/E and 351/E held at CAMR. 16. The anthrax vaccine that had its shelf life extended
was still packaged with the original "For the Medical and Pharmaceutical Professions" leaflet at CAMR. At that time, the
MCA were in the middle of a phased implementation of the Patient Pack Initiative (PPI). The aim of the PPI was to create for
all licensed products two documents: a summary of product characteristics (SPC) and a patient information leaflet (PIL). The
SPC is part of the product licence and provides information on the indications for treatment, contra-indications, dose and
administration, warnings and precautions, adverse drug reactions, and pharmaceutical characteristics of the drug. When new
drug safety information becomes available, SPCs are routinely updated to include this information. PILs contain similar
information to SPCs but are written specifically for patients. PILs are also updated routinely. 17. In 1998, it was agreed
between the MCA and CAMR that the anthrax batches to be supplied to MoD (MSA) would be over-labelled only, with the
new expiry date. It was agreed there would be no re-write of the advice leaflet in the SPC/PIL format. This was because the
MCA allowed a period of up to six months for manufacturers to introduce new leaflets
(13) The AGMC is a non-Departmental public body affiliated to the MoD and made up of leading medical and medical ethics
specialists.
(14) The MSA is a supply agency, not a medical licensing or regulatory body.
(15) HoL, Official Report, 3 March 1998, Column WA154; HoC,. Official Report, 3 March 1998, Column 535.
(16) AVPWG, Chaired by the DH with representatives from CAMR, NIBSC, MSA, DH, MCA/MHRA and MoD.
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point (16 January 1999), the MCA requested DH, as the licence holder, to add the following additional warnings to the SPC
and PIL: "The vaccine should be used alone. There is no evidence for the safe use in combination with other vaccines or
medicinal products. The vaccine contains thiomersal and therefore it is possible that delayed hypersensitivity and sensitisation
reactions may occur". The approval date for this variation was 15 January 1999. The revised SPC and PIL information was to
apply to the anthrax vaccine batches not used and manufactured under PL 01511/0037 and future stocks to be manufactured
under PL 01511/0058. 23. The changes in the wording of PL 01511/0037 were conveyed to the manufacturer, CAMR. The
SPC and PIL were approved on 4 March 1999. The packaging was changed and new SPC and PIL documents were inserted
with doses of the vaccine. This was the first time (April 1999) that the SPC included the statement that the vaccine should be
"used alone". The reason for the gap between the decision in 1998 and the introduction of the SPC/PIL was that this was the
first time a new format SPC and PIL was issued and there was much consultation between all involved. These changes took
place while the MoD's VIP against anthrax was suspended. March 2001 24. In March 2001, newly manufactured anthrax
vaccine from CAMR became available for use under PL 01511/0058, the vaccine having passed release tests at NIBSC. May
2001Resumption of the VIP against Anthrax 25. MoD resumed its VIP against anthrax in May 2001 as new stock had
become available. The resumption of the VIP against anthrax was accompanied by a MoD Surgeon General's policy letter
(SGPL)(17) dated 21 May 2001. SGPL's are sent to all medical practitioners in the Defence Medical Services. This letter
stated: "All personnel who wish to accept the vaccine are to be immunised in accordance with the Department of Health (DH)
Anthrax Vaccine Datasheet and the DH Anthrax Patient Information Leaflet." These documents were reproduced as
Enclosures 1 and 2 respectively to the SGPL. Enclosure 1 included the instruction: "The vaccine should be used alone." 26.
The SGPL contained information on the timing of anthrax immunisations. The SGPL explained that the vaccine should be
given in four dosesinitial dose, at three, six and thirty-two weeks, and gave additional guidance on immunisation schedules
for those personnel who had already received one or more doses from before the programme was suspended.
"Ideally, anthrax vaccine should be given separately from other immunisations. However, there may be situations when several
immunisations have to be administered together for expediency. If this situation occurs, then the anthrax vaccine may be given
at the same time as other vaccines so long as a separate injection site is used (ideally the opposite arm). Notwithstanding, the
anthrax vaccine is not recommended to be administered at the same time as a live vaccine or gamma globulin (although this is
little used now) and at least five days should elapse between such immunisations. Anthrax vaccine is a sub-component vaccine
and so should not interfere with the efficacy of other vaccines or interact with them . . ." 28. This additional guidance,
developed for MoD by the AGMC was designed to clarify the "should be used alone" statement in the SPC. 29. The advice
contained in the 13 June 2002 SGPL repeated that of the 21 May 2001 SGPL regarding the timing of immunisations as set out
above. 2003The Lord Morris of Manchester's Parliamentary Question 30. On 22 January 2003, the Lord Morris of
Manchester tabled a Parliamentary Question (PQ)(20), which asked, inter alia, about the position on anthrax vaccine licensing
in 199091. This PQ prompted the MCA to ask the Committee on Safety of Medicines (CSM) to review the licensing
information on the administration of anthrax vaccine. The Vaccine Sub-Group of the CSM met on 10 February 2003 and
recommended that the restriction on co-administration promulgated in 1999 be removed. This recommendation was endorsed
by the CSM on 12 February 2003. 31. The then Secretary of State for Health asked the CSM to reconvene to further consider
this issue to ensure that the committee had taken account of all available scientific data (including the original 1990 NIBSC
animal studies). On 4 March 2003, a specially convened anthrax expert sub-group of the CSM met to review all available
evidence on the safety of anthrax vaccine. On 12 March 2003, the CSM reconsidered the advice it had given earlier in the light
of the recommendations of the expert sub-group, and
(18) Official Report, HoL, 13 June 2002, Column WA 46; Official Report, HoC, 13 June 2002, Column 1345W.
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Anthrax vaccine must not be mixed with any other vaccine or other medicinal product in the same syringe.
If necessary, anthrax vaccine may be given at the same time as other vaccines. Other injectable vaccines should be
administered by separate injections into different anatomical sites and, ideally, into different limbs.
Subjects who are receiving immuno-suppressive therapy, including high dose corticosteroids, may be given anthrax vaccine
but may not mount an adequate immune response. 33. The Licensing Authority (the MCA, now part of the Medicines and
Healthcare Products Regulatory Agency) approved this variation on 16 April 2003. The anthrax vaccine PL will be amended
accordingly and a revised SGPL will then be issued. 34. Further information about MoD's current VIP against anthrax can be
found on the Internet at: http://www.mod.uk/issues/anthrax/index.htm. Annex B Immunisations Offered for the 199091 Gulf
Conflict (Operation Granby)
Immunisation
Position in 199091
(Notes 1, 2 & 3)
Anthrax
Offered to all personnel deploying. To be co-administered with pertussis vaccine. No advice given in the
leaflet accompanying the anthrax vaccine for medical and pharmaceutical professions about the need to
avoid co-administration. Nothing on contra-indications.
Cholera
Offered to all personnel deploying. Not to be administered to a subject who has experienced a serious
reaction (e.g. anaphylaxis) to a previous dose of this vaccine or who is known to be hypersensitive to any
component thereof. Advisable to avoid vaccination during acute infection, or chronic illness.
Diptheria
Gamma
Globulin
Made up of human normal immunoglobulin (HNIG). Certain occupational groups, such as those handling
food and water supplies, may have been offered a Gamma Globulin immunisation. Must not be
administered intravenously. HNIG is for use as a single entry dose only: unused proportions should be
discarded. HNIG is not suitable for modifying reactions to measles vaccine. HNIG will not affect the
immune response to bacterial vaccines but could reduce the response to some virus vaccines and toxoids.
At least 4 weeks should elapse after the last dose of the following vaccines before HNIG is administered:
Polio (live or inactivated), Measles, Rubella, Diptheria or Tetanus. (This warning does not apply to Yellow
Fever vaccine as HNIG does not contain antibody to this virus).
MoD is aware of one individual who was part of a medical unit that served in Operation GRANBY who is
recorded as having received Gamma Globulin.
Hepatitis B
Meningococcal
meningitis
Vaccine must not be given to those who have previously experienced a serious reaction to the vaccine or
its components. Vaccination should be delayed if an acute infection is present.
In August 1990, immunisation against meningococcal meningitis strains A and C was recommended for
all personnel serving in the Gulf. By 15 September 1990, the immunisation was no longer recommended
except for medical personnel and personnel who may be at risk by way of frequent contact with host
nation personnel. Immunisation against meningococcal meningitis strains A and C involved one
vaccination which was effective against both strains.
Pertussis
Offered as adjuvant to all personnel deploying. The contra-indications relating to the UK sourced vaccine
only relate to administration to children. The datasheet for the vaccine manufactured in France says:
"Those of all vaccinations. The practicing physician remains the sole judge of the advisability of
vaccination."
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Plague
Offered to all personnel deploying. The manufacturers product safety leaflet said that "Plague Vaccine
should not be administered to anyone with a known hypersensitivity to any of the produce constituents,
such as beef protein, soya, casein, phenol, and formaldehyde. Patients who have had severe local or
systematic reactions to plague vaccine injections should not be revaccinated. Plague vaccine should not be
administered to patients who have severe thrombocytopenia or any coagulation disorder that would
contraindicate intramuscular injections."
Poliomyelitis
Offered to all non-immune personnel. Administered by mouth. Contraindications: The vaccine should not
be used in the presence of acute febrile illness or inter-current infection, diarrhoea, vomiting or other
gastrointestinal disturbance, neither should it be given in the presence of impaired immune response
including leukaemia, lymphoma, generalized malignancy or treatment with corticosteroids, cytotoxic
drugs or irradiation. Do not give to those known to be hypersensitive to neomycin.
Interactions with other medicaments and other forms of interaction: At least 3 weeks should normally
intervene between the administration of any two live vaccines. Poliomyelitis vaccines can, however, be
given simultaneously with measles, mumps and rubella vaccines. In this case the injectable vaccines
should be given at different sites
Effects on ability to drive and to use machines: Not applicable.
Other undesirable effects (frequency and seriousness): Paralysis temporally associated with vaccination
has been reported very rarely in recipients or contacts.
Use in pregnancy and lactation: Pregnant women should not be given oral poliomyelitis vaccine unless
they are at definite risk from poliomyelitis.
Other special warnings and precautions: The vaccine may contain trace amounts of penicillin and
streptomycin which should not contra-indicate its use except in those with a history of severe anaphylaxis
due to either antibiotic.
Overdose (symptoms, emergency procedures, antidotes): Not applicable.
Incompatibilities: none.
Tetanus
Offered to all personnel, administered with typhoid vaccine as one combined immunisation. Absorbed
Tetanus vaccine should not be administered intradermally. The vaccine should not be administered to a
subject who has experienced a serious reaction (e.g. anaphylaxis) to a previous dose of this vaccine or who
is known to be hypersensitive to any component thereof. It is advisable to avoid vaccination during an
acute infection.
Tuberculosis
Recruits without a BCG immunisation scar and who were not shown to be immune were offered BCG
immunisation. It was not to be given if the subject was receiving treatment with corticosteroids or other
immuno-suppressive treatment, including general radiation. No further immunisation should be given for
at least three months in the arm used for BCG immunisation because of the risk of regional infection of the
lymph nodes (glands) and lymph channels.
Typhoid
Offered to all personnel. Administered with tetanus vaccine as one combined immunisation. The vaccine
should not be administered to a subject who has experienced a serious reaction (e.g. anaphylaxis) to a
previous dose of this vaccine or who is known to be hypersensitive to any component thereof. It is
advisable to avoid vaccination during an acute infection.
Yellow Fever
Offered routinely to servicemen. Servicewomen were only to be immunised if they were travelling to a
region where yellow fever was endemic. However, MoD is aware of records for servicewomen who served
with a unit that deployed to the Gulf as routinely receiving Yellow Fever immunisation.
The datasheet said: The vaccine should not be administered to a subject who has experienced a serious
reaction (e.g. anaphylaxis) to a previous dose of this vaccine or who is known to be hypersensitive to any
component thereof. It is advisable to avoid vaccination during an acute infection. Since the vaccine is
prepared in chick embryos and contains small quantities of neomycin and polymyxin it should not be
administered to individuals who are hypersensitive to egg or chick protein or to these antibiotics. The
vaccine should not be given to those with impaired immune responsiveness, whether idiopathic or as a
result of treatment with steroids, radiotherapy cytotoxic drugs or other agents.
Note:
1. Vaccines listed in alphabetical order for ease of reference.
2. Other immunisations may have been offered on the basis of clinical need.
3. Summary of product characteristics (SPC) and patient information leaflets (PIL) were not introduced for UK licensed vaccines until after
the 199091 Gulf conflict.
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