Nonresponsiveness to Hepatitis B Vaccine in Health Care Workers

Craven, Donald E.; Awdeh, Zuheir L.; Kunches, Laureen M.; Yunis, Edmond J.; Dienstag, Jules L.; Werner, Barbara G.; Polk, B. Frank; Syndman, D R; Platt, Richard; Crumpacker, Clyde S.

doi:10.7326/0003-4819-105-3-356

Cited by 206 publications

(107 citation statements)

References 25 publications

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“…Usually, one would expect patients with autoimmune diseases to be high responders instead of low responders. Our results differ from Craven et al [5], Cooksley et al [4], and Walker et at. [27] with regard to DR-7, which they found elevated.…”

Section: Discussioncontrasting

confidence: 99%

“…In this study, A-10, B-12, CW-5, DR-3, and DR-5 were found to be increased in histocompatibility testing, whereas DR-2 was decreased. With regard to DR-3, this is in agreement with Craven et al [5]. Paradoxically, an increased frequency of HLA-DR-3 was also seen in patients with autoimmune chronic active hepatitis [15].…”

Section: Discussionsupporting

confidence: 89%

“…Only 9 persons (36%) remained protected (>10 IU/1 anti-HBs) 12 months after the fourth inoculation. Similar findings among poor responders were also reported by Craven and coworkers using a different vaccine preparation [5]. On the other hand, among normal responders only 8.7% fell to unprotective levels over 12months [11].…”

Section: Discussionsupporting

confidence: 87%

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Non-responsiveness to hepatitis-B vaccination: Revaccination and immunogenetic typing

Krämer¹,

Herth²,

Keyserlingk

et al. 1988

Klin Wochenschr

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Summary. The variation in immune responses to standard inoculation of the hepatitis-B virus vaccine suggest that host factors influence response in ways that are not presently understood. We studied 25 low/nonresponding health care workers (anti-HBs titer < 50 IU/1) after the third inoculation of an experimental hepatitis-B vaccine to determine their immune status (through lymphocyte phenotypes) and HLA type. After application of a fourth inoculation, the seroconverting subjects showed only low anti-HBs levels; three male subjects remained anti-HBs negative. Twelve months after the fourth inoculation only 9 of 25 subjects (36%) maintained anti-HBs titer >10 IU/1. Almost all subjects had normal B-cell and CD-4 and CD-8 counts and ratios. Relative to other European populations HLA-A-10 (P<0.05), B-12 ( P < 0.025), CW-5 (P<0.05), DR-3 (P<0.025), and DR-5 (P<0.025) were increased, whereas DR-2 (P<0.05) was decreased. However, after correction of the P-values for the number of HLA antigens determined, these differences were no longer significant. Furthermore, these HLA types were n o t the same as those reported in other studies (except for DR-3). We suggest that larger sample sizes or even not yet available immunogenetic markers wilt be required to prove a n " immunogenetic background" in low/nonresponders, if it exists.

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Section: Discussioncontrasting

confidence: 99%

Section: Discussionsupporting

confidence: 89%

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Non-responsiveness to hepatitis-B vaccination: Revaccination and immunogenetic typing

Krämer¹,

Herth²,

Keyserlingk

et al. 1988

Klin Wochenschr

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“…Individuals responding to vaccination with the induction of a high anti-HBsAg titer showed a strong T cell response non-responsiveness (HBsAg titer < 10 kU/L) to vaccination are associated with certain human leukocyte antigen (HLA)-class Ⅱ alleles. DRB1*0301, DRB1*0701, and DQB1*0201 [5,8,9] were shown to have a higher prevalence in non-responders, whereas other antigens (DRB1*0101, *1301, *1501, and DPB1*0401) seem to mediate strong immune responses [9][10][11][12] . Higher age, obesity, male gender, smoking, and chronic dialysis are risk factors for a non-/ low-responsiveness [8,9,[13][14][15] .…”

Section: Resultsmentioning

confidence: 99%

“…Hepatitis B vaccinations prevent HBV infections as well as its complications in most of the vaccines [3,4] . However, 5% to 10% fail to produce protective anti-HBsAg titers after three vaccinations irrespective of the source of the antigen, which is a problem not only for health care workers, and represents a major medical as well as economic challenge [5][6][7] . Low-(HBsAg titer 10-99 kU/L) or Abstract AIM: To evaluate, whether humoral hepatitis-B-vaccine non-responders also fail to mount a T cell response and to compare these results to normal vaccines.…”

mentioning

confidence: 99%

T cell responses to hepatitis B surface antigen are detectable in non-vaccinated individuals

Weihrauch¹,

Bergwelt‐Baildon²,

Kandic³

et al. 2008

WJG

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CONCLUSION:Our data suggest that there is no general immune deficiency in non-/low-responders. Thus, we hypothesize that the induction of anti-HBsAg responses by vaccination is significantly dependent on the pre-existing T cell repertoire against the specific antigen rather than the presence of a general T cell defect. INTRODUCTIONWorldwide, hepatitis B virus (HBV) infections are a growing problem with a high prevalence of over 8% hepatitis B surface antigen (HBsAg) positive individuals in Africa, South America, parts of Eastern Europe, South Asia, and Canada [1] . It is estimated that approximately 350 million people are chronic carriers of HBV with 1-1.5 million dying from liver cirrhosis and primary liver cancer [2] . Nowadays, protective repeated vaccinations with recombinant HBsAg are not only recommended to all health care workers and travellers, but have recently been included in the childhood and adolescence immunization schedule. Hepatitis B vaccinations prevent HBV infections as well as its complications in most of the vaccines [3,4] . However, 5% to 10% fail to produce protective anti-HBsAg titers after three vaccinations irrespective of the source of the antigen, which is a problem not only for health care workers, and represents a major medical as well as economic challenge [5][6][7] . Low-(HBsAg titer 10-99 kU/L) or Abstract AIM: To evaluate, whether humoral hepatitis-B-vaccine non-responders also fail to mount a T cell response and to compare these results to normal vaccines. RAPID COMMUNICATION T cell responses to hepatitis B surface antigen are detectable in non-vaccinated individuals

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Lack of Response to Recombinant Hepatitis B Vaccine in Nonresponders to the Plasma Vaccine

Weissman

Tsuchiyose²,

Tong³

et al. 1988

JAMA

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Yeast recombinant hepatitis B vaccine was administered to 25 nonresponders to the plasma-derived hepatitis B vaccine. After three 10-micrograms doses, nine subjects (36%) produced levels of antibodies to hepatitis B surface antigen (anti-HBs) of less than 2.1 sample ratio units (SRU) (nonresponders), and five (20%) developed anti-HBs of 2.1 to 9.9 SRU (hyporesponders); anti-HBs levels of 10 SRU or greater were detected at least once in 11 vaccinees (44%), but by the sixth and 12th months after the last vaccination, only three and one of these "responders," respectively, still maintained anti-HBs values of 10 SRU or greater. In these 25 subjects HLA subtyping showed a high prevalence of DR7, B8, and the combinations of DR3 and DR7 and DR4 and DR7. Our findings indicate that the yeast recombinant hepatitis B vaccine was not effective in eliciting a sustained anti-HBs response in nonresponders to the plasma hepatitis B vaccine.

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Nonresponsiveness to Hepatitis B Vaccine in Health Care Workers

Cited by 206 publications

References 25 publications

Non-responsiveness to hepatitis-B vaccination: Revaccination and immunogenetic typing

Non-responsiveness to hepatitis-B vaccination: Revaccination and immunogenetic typing

T cell responses to hepatitis B surface antigen are detectable in non-vaccinated individuals

Lack of Response to Recombinant Hepatitis B Vaccine in Nonresponders to the Plasma Vaccine

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