http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=PubMed&list_uids=2054370&dopt=Abstract
 

: J Adolesc Health 1991 May;12(3):273-8

Related Articles,

Serological response to measles revaccination in a highly immunized military dependent adolescent population.

Veit BC, Schydlower M, McIntyre S, Simmons D, Lampe RM, Fearnow RG, Stewart J.

Department of Clinical Investigation, William Beaumont Army Medical Center, El Paso, Texas 79920-5001.

In the spring of 1986, there was a measles outbreak in the city of El Paso, Texas, with 92 cases reported to the City-County Health Department. Of those 92 cases, 31 (32%) occurred within a public high school's student population of 2524. A mass measles vaccination program was undertaken at that high school in order to limit the outbreak. The student enrollment included a military dependent population of 368 students. Despite documented histories of prior measles immunizations in this military dependent subgroup, three individuals contracted the disease. Since this subgroup of students represented a highly immunized adolescent population, it was of interest to serologically determine their immune status prior to and following reimmunization with the expectation that such a study would provide information relating to the level of "protective" immunity. Prevaccination and postvaccination sera were obtained from 95 students. Results of measuring anti-measles antibody activity by ELISA indicate that 13 (14%) students responded to revaccination and experienced a fourfold or greater rise in IgG antibody levels. There were no detectable IgM responses. All of the students who responded to revaccination produced an anamnestic response (IgG boost only). Since most of these individuals had received first immunizations at 15 months of age or older, these findings suggest that secondary vaccine failure (waning immunity) was responsible for the putative "lowered" immunity in these individuals, instead of primary vaccine failure (maternal antibody suppression). These findings support current recommendations for measles booster revaccination of school-age children and adolescents.

PMID: 2054370 [PubMed - indexed for MEDLINE]

AN: 91274326

http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=PubMed&list_uids=1831579&dopt=Abstract

 

DICP 1991 Jun;25(6):628-34

Related Articles,

Intradermal hepatitis B vaccination.

Rivey MP, Peterson J.

School of Pharmacy, University of Montana, Missoula 59812.

The availability of vaccine since 1982 for immunization against hepatitis B virus (HBV) has had minimal impact on the disease; mass immunization has been suggested. Intradermal vaccination, which has precedent in prophylaxis of other infectious diseases, has been investigated as a low-cost alternative to traditional intramuscular HBV vaccination. Results of open and comparative trials indicate similar seroconversion rates for intradermal and intramuscular HBV vaccination routes in healthy adults. However, antibody titers and, presumably, duration of antibody protection appear to be decreased with intradermal HBV vaccination. Limited data suggest that demographic factors such as age and gender may affect vaccine responsiveness to intradermal HBV vaccine. Adverse skin reactions are common but do not represent a deterrent to continued intradermal HBV vaccination. There is a need for large-scale prospective comparative trials to substantiate the value of intradermal HBV vaccination. Nevertheless, the potential economic and epidemiologic benefit of intradermal vaccination justifies continued investigation for prevention of HBV infection.

Publication Types:

• Review
• Review, Tutorial

PMID: 1831579 [PubMed - indexed for MEDLINE]

http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=PubMed&list_uids=1670725&dopt=Abstract

 

Lancet 1991 Jan 12;337(8733):70-3

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Phase II trial of whole-cell pertussis vaccine vs an acellular vaccine containing agglutinogens.

Miller E, Ashworth LA, Robinson A, Waight PA, Irons LI.

Public Health Laboratory Service, Communicable Disease Surveillance Centre, Colindale, London, UK.

An acellular pertussis vaccine containing agglutinogens 2 and 3, pertussis toxin, and filamentous haemagglutinin was developed by the Centre for Applied Microbiology and Research in the UK. 188 infants were entered into a randomised blind trial and received either the acellular or a whole-cell vaccine, combined with diphtheria and tetanus toxoids, in a 3, 5, and 8-10 month schedule. Local reactions were similar in the two groups but significantly fewer infants had systemic symptoms after the acellular vaccine. Mean log-antibody titres to the agglutinogen and toxin components were higher with the acellular than with the whole-cell vaccine. Persistence of antibodies one year after the third dose was also better in the acellular group.

Publication Types:

• Clinical Trial
• Randomized Controlled Trial

PMID: 1670725 [PubMed - indexed for MEDLINE]

http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=PubMed&list_uids=1830374&dopt=Abstract

 

Nephron 1991;58(1):47-51

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Complete seroconversion by low-dose intradermal injection of recombinant hepatitis B vaccine in hemodialysis patients.

Ono K, Kashiwagi S.

Ono Geka Clinic, Kyushu University, Fukuoka, Japan.

The present study was undertaken to find out if the seroconversion rate of hemodialysis (HD) patients was enhanced by the intradermal (i.d.) inoculation of recombinant hepatitis B (HB) vaccine. Thirty-five HBs-Ag, HBs-Ab and HBc-Ag, HBc-Ab negative HD patients were divided into three groups: 14 patients in group I received 5 micrograms HBs Ag i.d. every 2 weeks, 13 patients in group II were given 2.5 micrograms HBs vaccine i.d. every 2 weeks, 5 times, then every week. The remaining 8 patients in group III were immunised with 10 micrograms HBs Ag every 4 weeks 5 times intramuscularly (i.m.), then 5 micrograms i.d., every 2 weeks until complete seroconversion. Antibody response to i.m. injection was poor and only 37.5% of patients developed anti-HBs at a titer of 10 mIU/ml or more at 16 weeks after the start of immunisation. However, this poor response was improved by i.d. injection. The time of seroconversion was significantly earlier and the rate of response was higher in group I. The poor response in group II was markedly improved by doubling the inoculation rate. Overall, 100% of seroconversion was finally obtained by multiple i.d. immunisation. However, the anti-HBs titers were lower in all patients and declined in some patients after the immunisation was stopped. The last seroconverted patient in each group lost protective antibody levels at the 39th week. These patients became antibody positive again at the 52nd week with a booster dose. We feel that the i.d. route remains a useful and cheaper method of obtaining prophylaxis against HBs in high-risk HD patients but it would seem to be prudent to monitor these patients serially to assess the persistence of anti-HBs in the serum.

PMID: 1830374 [PubMed - indexed for MEDLINE]

http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=PubMed&list_uids=2139280&dopt=Abstract

 

Vaccine 1990 Mar;8 Suppl:S129-33; discussion S134-8

Related Articles,

WHO strategy for the global elimination of new cases of hepatitis B.

Ghendon Y.

World Health Organization, Geneva, Switzerland.

Hepatitis B infection and its sequelae remain major public health problems internationally despite the existence of sensitive tests to screen blood and blood products for hepatitis B surface antigen (HBsAg) and immunogenic vaccines. Since the human hepatitis B virus has no known animal reservoir, a systematic vaccination programme against hepatitis B, including vaccination of all newborns and young children within the framework of the WHO Expanded Programme on Immunization, as well as protection of high-risk individuals, together with the testing of all blood and blood products for HBsAg, could eliminate hepatitis B virus infection and its sequelae. However, for the successful realization of this programme, many important and difficult problems need to be solved, especially those related to vaccination strategy, determination of the duration of immunity, investigation of the mechanisms of perinatal and horizontal virus transmission, and improvement of the immunogenicity of hepatitis B vaccine. The problem of the hepatitis B carrier is also paramount as the eradication of hepatitis B can be achieved only after the 300 million carriers of the disease in the world today are either cured or dead.

PMID: 2139280 [PubMed - indexed for MEDLINE]

http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=PubMed&list_uids=2179836&dopt=Abstract

 

Pediatr Infect Dis J 1990 Feb;9(2):101-10

Related Articles,

Duration of live measles vaccine-induced immunity.

Markowitz LE, Preblud SR, Fine PE, Orenstein WA.

Division of Immunization, Centers for Disease Control, Atlanta, GA 30333.

Publication Types:

• Review
• Review, Tutorial

From the article:  Similar to immunity after natural measles infection, live measles vaccine-induced immunity has been thought to be lifelong.  Vaccinees who subsequently develop measles have been considered primary vaccine failures, defined as the failure of the initial vaccination to elicit an appropriate immune response.  Primary vaccine failures are believed to be caused by (1) interference by maternal antibody when vaccination occurs at a young age, (2) technical problems, such as improper vaccine storage or administration, or (2) other unknown reasons.  Transmission of measles among older children in the United States, most of whom have been appropriately vaccinated, has raised the question of whether waning vaccine-induced immunity may also be responsible for some vaccine failures.  Current vaccination policy as well as mathematical models assume that vaccine-induced immunity is life-long.  If waning vaccine-induced immunity does occur, changes in measles vaccination strategies might be necessary.  The purpose of this paper is to review information concerning the duration and quality of measles vaccine-induced immunity.

Discussion: Several types of studies have been applied to evaluate the duration and quality of measles vaccine-induced immunity.  The few reports of measles disease in persons who had seroconverted after vaccination document that secondary vaccine failure can occur.  In addition two studies provide data on the potential magnitude of the risk of secondary vaccine failure.  However, most data suggest that waning immunity is uncommon.

Many questions concerning the duration of vaccine-induced immunity remain to be answered, including what percentage of cases reported in previously vaccinated persons in the United States is caused by primary or secondary vaccine failure, whether different measles vaccine strains produce immunity which is more or less "durable", whether reexposure to wild measles virus is important for maintenance of vaccine-induced immunity and whether it is possible to identify individuals at risk for waning immunity.

The consequences of waning measles vaccine-induced immunity may be minor for individuals if secondary vaccine failure is associated with mild disease.  However, waning vaccine-induced immunity could be of greater consequence to a population.  Although persons with subclinical reinfection have not been shown to transmit virus, it is not known whether this is true for persons with secondary vaccine failure.  If these individuals are able to transmit disease to other susceptibles, waning immunity, even in a small percentage of persons, may impede realization of the goal of measles elimination.  Revaccination may be successful in decreasing the number of persons who become susceptible due to waning immunity.  However, it is not known whether revaccination of such persons will result in sustained immunity. 

Questions concerning duration of vaccine-induced immunity and secondary vaccine failure were raised at the time of vaccine licensure and discussed 10 to 15 years later when outbreaks occurred in vaccinated children.  Now, 26 years after licensure, many of the same issues remain unresolved.  Although waning immunity has been documented to occur in a small proportion of vaccinees, the epidemiologic significance of this is still unclear.

         

          
PMID: 2179836 [PubMed - indexed for MEDLINE]

http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=PubMed&list_uids=2239007&dopt=Abstract

 

Zh Mikrobiol Epidemiol Immunobiol 1990 Aug;(8):66-70

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[The results of multiyear observations on the duration of the maintenance of immunity in those vaccinated and revaccinated against and recovered from measles]

[Article in Russian]

Sliusar' LI, Sokhin AA, Radomskaia FS, Degtiareva GV, Panasenko LI, Litvinova TP, Komarevskaia RV, Bol'shinskaia ZhI.

The results of 5-year observations on the duration of immunity to measles virus in persons vaccinated and revaccinated against measles, as well as in persons having had this infection, are presented. The intensity of immunity was determined in the same persons with the use of the passive hemagglutination test. The study revealed differences in the formation, intensity and duration of postvaccinal immunity. A significant decrease in the concentration of antibodies over the period of 5 years was established in 50.0-52.3% of vaccines. Revaccination with live measles vaccine is an effective measure for enhancing immunity to measles virus in persons with initial antibody titers less than 1:10-1:20, but revaccination made in a single injection is not sufficient for the stable maintenance of measles morbidity at the sporadic level. Postinfectious immunity is characterized by stability and has no tendency towards decrease. Persons having had measles have no need in additional measures irrespective of the time elapsed after the disease.

PMID: 2239007 [PubMed - indexed for MEDLINE]

http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=PubMed&list_uids=2194379&dopt=Abstract

 

Vaccine 1990 Jun;8(3):205-8

Related Articles,

Yeast-derived hepatitis B vaccine in dental students. A three-year follow-up study.

Zanetti AR, Tanzi E, Pozzi A, Romano L, Bergamini F.

Institute of Virology, University of Milan, Italy.

Sixty health adults (56 dental students and four post-graduates of the Dental Faculty in Milan; mean age 26.4 years, range 22-42 years) were vaccinated with a recombinant DNA vaccine (Engerix B, Smith Kline and French; 20 micrograms given i.m. at time 0, 1 and 6 months). One month after the third injection, 98.3% (59/60) vaccinees showed anti-HBs at levels higher than 10 mIU ml-1 (geometric mean titre 734.8 mIU ml-1). One year after the beginning of vaccination (i.e. 6 months after the third injection of vaccine), 46 vaccinees showed anti-HBs titre higher than 100 mIU ml-1 (24 between 100 and 1000 mIU ml-1 and 22 higher than 1000 mIU ml-1) and 14 vaccinees had anti-HBs below 100 mIU ml-1 (12 between 10 and 99 mIU ml-1 and 2 below 10 mIU ml-1). Since duration of antibody is directly related to the height of the initial response, the 14 vaccinees with lower anti-HBs titres were given a fourth dose of vaccine. All boosted vaccinees showed a vigorous anti-HBs response and the post-booster anti-HBs GMT increased to 1570 mIU ml-1 compared with 47.8 mIU ml-1 attained before the boosting injection. At three years from the beginning of vaccination, all vaccinees who showed anti-HBs titres higher than 100 mIU ml-1 after the primary vaccination and all but one of the boosted vaccinees were still anti-HBs positive.(ABSTRACT TRUNCATED AT 250 WORDS)

PMID: 2194379 [PubMed - indexed for MEDLINE]

http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=PubMed&list_uids=2278542&dopt=Abstract

 

JAMA 1990 May 9;263(18):2467-71

Related Articles,

Comment in:

• JAMA. 1990 Nov 7;264(17):2211-2.

Mild measles and secondary vaccine failure during a sustained outbreak in a highly vaccinated population.

Edmonson MB, Addiss DG, McPherson JT, Berg JL, Circo SR, Davis JP.

Department of Pediatrics, University of Wisconsin, Madison 53792.

A prolonged school-based outbreak of measles provided an opportunity to study "vaccine-modified" mild measles and secondary vaccine failure. Thirty-six (97%) of 37 unvaccinated patients had rash illnesses that met the Centers for Disease Control clinical case definition of measles, but 29 (15%) of 198 vaccinated patients did not, primarily because of low-grade or absent fever. Of 122 patients with seroconfirmed measles, 10 patients (all previously vaccinated) had no detectable measles-specific IgM and significantly milder illness than either vaccinated or unvaccinated patients with IgM-positive serum. Of 108 vaccinated patients with seroconfirmed measles, 17 patients (16%) had IgM-negative serology or rash illnesses that failed to meet the clinical case definition; their mean age (13 years), age at the time of vaccination, and time since vaccination did not differ from those of other vaccinated patients. The occurrence of secondary vaccine failure and vaccine-modified measles does not appear to be a major impediment to measles control in the United States but may lead to underreporting of measles cases and result in overestimation of vaccine efficacy in highly vaccinated populations.

PMID: 2278542 [PubMed - indexed for MEDLINE]

AN: 90230400

http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=PubMed&list_uids=2523251&dopt=Abstract

 

Bull World Health Organ 1989;67(1):65-70

Related Articles,

The hepatitis B immunization programme in Singapore.

Goh KT, Doraisingham S, Tan KL, Oon CJ, Ho ML, Chen AJ, Chan SH.

A voluntary immunization programme to prevent perinatal transmission of hepatitis B virus (HBV) infection in Singapore was implemented on 1 October 1985 as an integral component of the national childhood immunization programme. Up to April 1988, a total of 68,845 mothers who attended government maternal and child health clinics were screened for the disease. Of these, 2432 (3.5%) were positive for hepatitis B surface antigen (HBsAg) and 904 (1.3%) for hepatitis B e antigen (HBeAg). Virtually all the babies born to carrier mothers completed the full immunization schedule; and in addition, those of HBeAg-positive mothers were given a dose of hepatitis B immunoglobulin at birth. The hepatitis B immunization programme was extended on 1 September 1987 to cover all newborns. About 90% of the 15,943 babies delivered in government institutions from September 1987 to April 1988 were immunized at birth, with the subsequent doses being administered at maternal and child health clinics at 4-6 weeks and 5 months later. More than 85% of the children given the full course of plasma-derived and yeast-derived hepatitis B vaccine from birth continued to have protective antibody to HBV two years after immunization. The programme is being closely monitored to assess the duration of immunity and the need for booster doses, while seronegative adults are also being encouraged to be vaccinated.

PMID: 2523251 [PubMed - indexed for MEDLINE]

Somewhere between 0 and 14% did not continue to have protective antibodies even 2 years later. - SM

http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=PubMed&list_uids=2526418&dopt=Abstract

 

: Vaccine 1989 Apr;7(2):102-3

Related Articles,

Duration of immunity to hepatitis B vaccination in institutionalized mentally retarded patients.

Torre D, Broggini M, Botta V, Sampietro C.

Division of Infectious Diseases Regional Hospital and Foundation E. and S. Macchi, Varese, Italy.

Susceptible individuals of an institution for the mentally retarded (20 residents and six staff members) were vaccinated with Hevac B Pasteur (5 micrograms, months 0, 1, 2, 14). There were protective levels of anti-HBs in 75% of residents and 100% of staff members after 15 months from the first dose of the vaccine. After a 4-year follow-up period, there were persistent and protective levels of anti-HBs in 80% of residents, compared with 66% in staff members. In addition, no clinical hepatitis B infections were observed during this period.

PMID: 2526418 [PubMed - indexed for MEDLINE]

http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=PubMed&list_uids=2528297&dopt=Abstract

 

Am J Med 1989 Sep 4;87(3A):36S-40S

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Factors influencing the immune response to hepatitis B vaccine, booster dose guidelines, and vaccine protocol recommendations.

Hollinger FB.

Department of Virology, Baylor College of Medicine, Houston, Texas 77030.

The clinical course and immunodiagnosis of hepatitis B infection is discussed. Immunization is necessary to prevent the clinical disease, the development of carriers, and the transmission of the hepatitis B virus to susceptible persons. Host factors that can curtail the immune response include increasing age, obesity, smoking cigarettes, and having a medical condition that compromises the immune system. Increasing the dose of vaccine, administering the inoculations intramuscularly, and giving the vaccine more frequently can enhance the immune response. The duration of immunity following vaccination has not yet been defined, but booster dose guidelines for selected groups are provided. Finally, recommendations for developing and implementing hepatitis B immunization protocols are presented.

Publication Types:

• Review
• Review, Tutorial

PMID: 2528297 [PubMed - indexed for MEDLINE]

http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=PubMed&list_uids=2929807&dopt=Abstract

 

Am J Public Health 1989 Apr;79(4):475-8

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The role of secondary vaccine failures in measles outbreaks.

Mathias RG, Meekison WG, Arcand TA, Schechter MT.

Department of Health Care and Epidemiology, University of British Columbia, Vancouver.

An outbreak of measles in 1985-86 in a community where measles vaccine trials had been carried out from 1974-76 allowed the assessment of the role of secondary vaccine failures in previously immunized children. A total of 188 children from the vaccine trial were followed. Of these, 175 seroconverted initially while 13 (6 per cent) required re-immunization (primary failure). A total of 13 cases of measles, eight of which were laboratory and/or physician-confirmed, were reported in this cohort. Of these, nine cases occurred in the 175 subjects who had hemagglutination inhibition test (HI) and neutralizing antibody responses following the initial immunization. These nine cases represent secondary vaccine failures. An additional four cases occurred in the 13 subjects with primary vaccine failure. We conclude that secondary vaccine failures occur and that while primary failures account for most cases, secondary vaccine failures contribute to the occurrence of measles cases in an epidemic. A booster dose of measles vaccine may be necessary to reduce susceptibility to a sufficiently low level to allow the goal of measles elimination to be achieved.

PMID: 2929807 [PubMed - indexed for MEDLINE]

http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=PubMed&list_uids=2529345&dopt=Abstract

 

J Fla Med Assoc 1989 Apr;76(4):399-402

Related Articles,

Deltoid versus buttock as preferred site of injection for hepatitis B vaccine.

Hellgren TE.

Several factors concerning effectiveness of the hepatitis B virus (HBV) vaccination have been discovered: site of injection, indications for revaccination, testing for immunity, persistence of HBV antibody following vaccination, and age of recipient. The site may be important in provoking an appropriate antibody response. The deltoid is recommended rather than the gluteal. It is suggested that recipients of gluteal vaccinations receive revaccination in the deltoid. Revaccination is also recommended five years after the original series due to possible loss of antibody response. This is especially important to those with continued exposure to HBV such as medical personnel. However, caution is suggested as undetectable antibody appears to be an unreliable predictor of susceptibility to infection. It is also recommended that testing for immunity after vaccination be conducted only in those in whom a suboptimal response is expected, i.e., gluteal injection recipients and immunocompromised patients. Age of the recipient appears to be a major confounder influencing the duration of vaccine-induced immunity. The physician's consideration of these factors when administering the HBV vaccine should increase the overall effectiveness of immunization.

Publication Types:

• Review
• Review, Tutorial

PMID: 2529345 [PubMed - indexed for MEDLINE]

http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=PubMed&list_uids=2963570&dopt=Abstract

 

Ann Intern Med 1988 Feb;108(2):185-9

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Duration of immunity after hepatitis B vaccination: efficacy of low-dose booster vaccine.

Horowitz MM, Ershler WB, McKinney WP, Battiola RJ.

Department of Medicine, Medical College of Wisconsin, Milwaukee.

Although the efficacy of hepatitis vaccine is well documented, the duration of immunity of healthy adults after vaccination is unknown. We studied 245 hospital employees 3 years after primary vaccination with hepatitis B vaccine to determine the prevalence of immunity indicated by levels of antibody to hepatitis B surface antigen of 10 mIU/mL or greater; and to compare the immunogenicity of low-dose intradermal vaccine with standard-dose intramuscular vaccine in persons found to be seronegative. Thirty-eight percent of employees studied had antibody levels less than 10 mIU/mL. Low levels were associated with smoking, older age, and higher body-mass index. Seventy-eight percent of persons with low antibody levels responded to a single booster vaccine. Two micrograms of intradermal vaccine was as effective as 20 micrograms of intramuscular vaccine in inducing an antibody response; however, intradermal vaccine was associated with more local reactions (42% compared with 17%). Many healthy adults will need periodic boosters of hepatitis B vaccine to maintain production of antibody to hepatitis B surface antigen; low-dose intradermal booster schedules may be feasible.

PMID: 2963570 [PubMed - indexed for MEDLINE]

http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=PubMed&list_uids=3660859&dopt=Abstract

 

Yale J Biol Med 1987 Jul-Aug;60(4):333-9

Related Articles,

Hepatitis B vaccine: prospects for duration of immunity.

Krugman S, Davidson M.

Department of Pediatrics, NYU Medical Center, New York 10016.

The duration of hepatitis B vaccine-induced immunity was studied in a group of 54 seronegative health professionals who received plasma-derived hepatitis B vaccine (Merck's Heptavax) in 1978 and 1979. Five to seven years later, 52 vaccinees received a booster dose of yeast recombinant hepatitis B vaccine (Merck's Recombivax). Of 54 vaccinees, 47 (87 percent) had a favorable anti-HBs response (greater than 10 S/N RIA units) and 7 (13 percent) had low (2.1-10 S/N) or undetectable levels (less than 2.1 S/N) one year after primary immunization. After five to seven years, the anti-HBs values had declined to undetectable levels in 25 percent and to low levels in 23 percent. A booster dose of vaccine induced an anamnestic response in 90 percent of vaccinees by two weeks. The results of this study indicate that persons who respond favorably to primary immunization may be protected for at least seven years.

PMID: 3660859 [PubMed - indexed for MEDLINE]

http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=PubMed&list_uids=3021273&dopt=Abstract

 

Br Med J (Clin Res Ed) 1986 Nov 1;293(6555):1153-5

Related Articles,

Prevalence of antibody to poliovirus in England and Wales 1984-6.

White PM, Green J.

Serum from 995 subjects aged 6 months to 99 years was screened at a dilution of 1/8 for neutralising antibodies to poliovirus. Of these samples, 975 (98%) contained antibody to at least one serotype, and 763 (77%) contained antibody to all three, an improvement since previous studies. Children aged 8 to 15, however, had a low prevalence of antibody to poliovirus type 3, with only four (40%) of those aged 12 protected. This finding is possibly due to the waning of antibodies induced by the type 3 component of oral poliovirus vaccine and emphasises the continued importance of a booster dose of vaccine for those leaving school.

PMID: 3021273 [PubMed - indexed for MEDLINE]

http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=PubMed&list_uids=4001723&dopt=Abstract

 

: Rev Infect Dis 1985 Mar-Apr;7 Suppl 1:S157-63

Related Articles, Books, LinkOut

Challenge with rubella virus after loss of detectable vaccine-induced antibody.

Schiff GM, Young BC, Stefanovic' GM, Stamler EF, Knowlton DR, Grundy BJ, Dorsett PH.

Studies were conducted of experimental challenge with rubella virus in vaccinees whose possession of vaccine-induced antibody after vaccination had been documented and whose antibody level had become undetectable or very low over time. The challenge virus was the Howell strain, which had been shown to produce typical clinical and laboratory features of rubella in susceptible persons. The challenge of the vaccinees resulted in local viral replication in all but one; in viremia, a primary immunologic response, and a secondary antibody response in some; and usually in illness without a rash or in subclinical infection. The results emphasize the importance of continuing careful clinical and laboratory surveillance of vaccinees for determining the persistence of vaccine-induced immunity and of considering methods for identifying and revaccinating the minority of vaccinees who lose such immunity.

PMID: 4001723 [PubMed - indexed for MEDLINE]

http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=PubMed&list_uids=4055805&dopt=Abstract

J Biol Stand 1985 Oct;13(4):283-93

Related Articles,

http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=PubMed&list_uids=6693863&dopt=Abstract

: J Med Virol 1984;13(1):93-103

Related Articles,

The use of IgM tests for analysis of the causes of measles vaccine failures: experience gained in an epidemic in Hungary in 1980 and 1981.

Nagy G, Kosa S, Takatsy S, Koller M.

Following a period of 6 years of low measles incidence, an epidemic occurred in Hungary with more than 11,000 reported cases between September 1980 and August 1981. About 60% of the cases had a documented history of previous measles vaccination. Serum samples obtained from 7815 patients were examined for measles antibody by haemagglutination inhibition (HI). In addition to conventional antibody titration, most of the sera or their IgM fraction obtained by a simple ion exchange chromatography were tested for the presence of measles-specific IgM antibodies by 2-mercaptoethanol (2-ME) treatment, and in 300 patients also by the fluorescent antibody (FA) technique. Laboratory results confirmed the diagnosis of measles in 5356 patients and supported it in 685 cases. Primary antibody response was found in 96.1% of unvaccinated and in 77.4% of previously vaccinated patients. The percentage of secondary antibody responses increased with increasing time from vaccination only in patients vaccinated before their first birthday, whereas in those who were immunized when over 12 months old, the distribution of primary and secondary antibody responses was independent from the time that had elapsed since vaccination. Therefore, secondary vaccine failure due to waning immunity account for only 6.2% of previously vaccinated patients, whereas in 93.8% of patients, including the majority of those with secondary antibody response, a primary failure of vaccination due to unsuccessful immunization was incriminated.

PMID: 6693863 [PubMed - indexed for MEDLINE]

AN: 84113582

This abstract was put here because although most vaccine failures were considered to be "primary", secondary vaccine failures did occur. - SM

http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=PubMed&list_uids=6241767&dopt=Abstract

 

Vaccine 1983 Dec;1(1):10-2

Related Articles,

Immunogenicity of HBV vaccine in healthy Chinese children.

Hwang LY, Beasley RP, Stevens CE, Szmuness W.

The immunogenic response of healthy Chinese children to three different doses of hepatitis B virus (HBV) vaccine was compared. One hundred susceptible children received two doses of 10, 20 or 40 micrograms a month apart. A month following the first dose 33% of all the children had antibodies. The response rate rose to 78% a month later and 99% four months later. Ninety percent of the 100 children still had antibody at 12 months after vaccination was initiated. The response rate, antibody levels and persistence of antibody were directly related to the dose of vaccine and inversely to the age of children. No adverse reactions were observed.

Publication Types:

• Clinical Trial
• Randomized Controlled Trial

PMID: 6241767 [PubMed - indexed for MEDLINE]

 

Obviously, after 12 months 10% did not. - SM

http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=PubMed&list_uids=6879006&dopt=Abstract

 

Rev Infect Dis 1983 May-Jun;5(3):506-10

Related Articles,

Measles vaccine in the People's Republic of China.

Xiang JZ, Chen ZH.

The strains of measles virus and the method used in the production of further attenuated live-virus vaccine in the People's Republic of China were studied. Observation of clinical reactions and serologic responses to immunization with Shanghai-191 measles vaccine, which is produced on a large scale with a locally isolated viral strain, revealed that this vaccine is adequately safe and immunogenic. Epidemiologic data showed a significant decrease in measles-associated morbidity after the introduction of mass vaccination in 1965. The duration of immunity induced by Shanghai-191 measles vaccine was studied for eight years in a region in which interference due to natural measles infection had been minimized by mass vaccination of children. Although immunity appeared to persist for at least eight years, the results suggested that primary vaccination does not confer lifelong immunity. Reactions and antibody responses to this vaccine were compared with those to two vaccines from abroad, the Schwarz and Leningrad-16 strains. The hemagglutination-inhibiting (HAI) antibody titer induced by Shanghai-191 vaccine was higher than that induced by Leningrad-16 vaccine and lower than that induced by Schwarz vaccine; however, these differences were not significant. Preliminary studies on the preparation of measles vaccine in human diploid cells have yielded promising results.

PMID: 6879006 [PubMed - indexed for MEDLINE]

http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=PubMed&list_uids=230111&dopt=Abstract

 

Dev Biol Stand 1979;43:207-13

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Poliovirus antibodies in age groups: an assessment of obligatory vaccination in Belgium.

Lamy ME, Cornu C, Desmyter J.

Since 1967, compulsory oral vaccination before 2 years of age has been nearly the only form of poliovaccination practiced in Belgium, and there have been almost no cases of polio. In recent sera from 2,225 Belgians, 2 year olds lacked demonstrable seroneutralizing antibody, in 31% for type 1, in 8% for type 2, and in 21% for type 3. The lack of antibodies grew as the children reached 11--12 years, at which age 65% lacked antibody for type 1, 15% for type 2, and 54% for type 3; only 19% had antibodies against all types. It is argued that this decline of antibodies is not due to insufficient vaccination in former years, but is a strong example of the waning of vaccine-acquired serum antibody. Antibody rates went up after age 12. The highest rates of types 1 and 3 antibodies were seen at age 20--59. There was some decrease of antibody after 60 years. Mean antibody titers paralleled positivity rates. Results of two laboratories studying different populations with different standard techniques were similar. The data support revaccination at school entrance.

PMID: 230111 [PubMed - indexed for MEDLINE]

http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=PubMed&list_uids=688165&dopt=Abstract

 

: Can J Public Health 1978 Jul-Aug;69(4):325-33

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The measles epidemic in Calgary, 1974-1975: the duration of protection conferred by vaccine.

O'Neil AE.

 

From the article: Individual immunity to measles, derived from live vaccine, wanes with time.

PMID: 688165 [PubMed - indexed for MEDLINE]

http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=PubMed&list_uids=645653&dopt=Abstract

 

Am J Dis Child 1978 Apr;132(4):371-3

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The changing epidemiology of pertussis in young infants. The role of adults as reservoirs of infection.

Nelson JD.

We reviewed 400 bacteriologically confirmed cases of pertussis in infants and children during the past 18 years. Several changes in the epidemiology have occurred in the most recent six-year period. The incidence of whooping cough in children has decreased by at least 50%, but the proportion of cases occurring in infants younger than 12 weeks of age has doubled to 30% of all cases. Formerly most young infants acquired their illness from siblings or other children, but in the recent period adults in the household were the most common source of infection to neonates and young infants. This observation plus the increasingly high level of immunization in preschool and school-aged children suggest that young adults with waning immunity and mild illness are a major reservoir for transmission of pertussis to infants too young to be immunized.

PMID: 645653 [PubMed - indexed for MEDLINE]

http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=PubMed&list_uids=830888&dopt=Abstract

: J Pediatr 1977 Jan;90(1):17-20

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A measles outbreak among adolescents.

Weiner LB, Corwin RM, Nieburg PI, Feldman HA.

In a May, 1975, outbreak, 147 adolescents, ages 12 to 19 years, were identified as having measles by a physician or school nurse. One junior high school, with an enrollment of 1,122, contributed 131 of the cases. Of the 147 students, 54 were seen by physicians who also supplied their immunization records; 19 of 54 (35%) had received live measles virus vaccine without measles immune globulin, after age one year. The remaining 35 received: killed virus vaccine only (1), K + L (4), L + MIG (4), L at less than 1 year of age (4), L + ? MIG (4), immune serum globulin only, for exposure (6), no vaccine but history of measles previously (9); history uncertain (3). Hemagglutination-inhibition antibody titers were consistent with the diagnosis of acute measles in 11 children. No index case was identified and no secondary cases occured within the families of the 54 cases. This measles outbreak among seemingly immunized adolescents raises a serious question as to the duration of such protection.

PMID: 830888 [PubMed - indexed for MEDLINE]

http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=PubMed&list_uids=1126572&dopt=Abstract

 

Dev Biol Stand 1975;28:273-84

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Duration of circulating and secretory antibody and cell-mediated immunity following immunization.

Waldman RH, Ganguly R.

An important consideration in evaluating vaccines is the duration of immunity. The only really important measure of this immunity is the protection against infections and/or illness at various time intervals, following natural or artificial challenge. There are few data of this sort, more commonly immunity is estimated by measuring serum antibody, in many instances an erroneous measure. Serum antibody levels to respiratory viruses fall only slightly 6 months following infection or immunization. It is difficult to assess the duration of antibody for much longer than this, because of problems with intercurrent infection. With respiratory bacterial infections, e.g. pneumococcal pneumonia, parenterally-induced immunity probably lasts for only several months. Secretory antibody induced by inactivated viral vaccines, seems to persist for about a year, after having reached a peak level at about 4-6 weeks following immunization. Work with the live attenuated polio virus vaccine indicates longer lasting immunity, with detectable antibody persisting for up to 34 months. Restimulation with the inactivated polio virus vaccine produced no evidence of a secondary response (memory). Following booster immunization with influenza very little evidence of memory is seen. Cell-mediated immunity (CMI): in guinea pigs BCG sensitization can be demonstrated for at least 2-9 months. In humans, intracutaneous BCG immunization leads to positive tuberculin reaction in 6-10 weeks, and skin sensitivity lasts an average of about 4 years. There is contradicting data as to the duration of protection against infection following BCG immunization. Local and systemic CMI have been shown to exist independently of each other in experimental animals and man.

PMID: 1126572 [PubMed - indexed for MEDLINE]

http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=PubMed&list_uids=5362859&dopt=Abstract

 

: Am J Epidemiol 1969 Dec;90(6):514-8

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Persistence of measles antibody in the absence of circulating natural virus five years after immunization of an isolated virgin population with Edmonston B vaccine.

Brown P, Gajdusek DC, Tsai T.

 

From the abstract:  In the absence of circulating natural measles virus in an isolated Pacific atoll community after immunization of 136 immunologically virgin individuals from 1 to 24 years of age with Edmonston B strain live attenuated measles vaccine, serum levels of HI antibody remained stable between 1 and 2 1/2 years after immunization, but decline 2 to 3-fold by 5 years after immunization.  Sera having the highest antibody titers at 1 year showed the greatest decline, with a resultant narrowing of the titer range at 5 years.  Individuals with even undetectable HI antibody levels at 5 years, nevertheless showed neutralizing antibody at a serum dilution of at least 1:2, and thus presumably remain immune from infection.

PMID: 5362859 [PubMed - indexed for MEDLINE]