HIV Clinical Trial
Official title:
Long Term Serological Response and Memory Cells Role After Different Pneumococcal Vaccine Strategies in HIV Adults
Streptococcus pneumoniae is a cause of high morbidity and mortality in HIV-positive subjects, representing the leading etiological agent of severe bacterial pneumonia. International guidelines recommend that HIV positive patients aged >=19 years, who are 13-valent conjugate vaccine (PCV13) naïve, should receive a single dose of PCV13. Pneumococcal polysaccharide vaccine 23-valent (PPV23) should be given >=8 weeks after indicated dose of PCV13, and a second dose of PPV23 should be given 5 years later. For those who previously received PPV23, PCV13 should be administered >=1 year after the last PPV23 dose. HIV infection affects humoral immunity both through reduced T-cell help and changes in the B-cell compartment. Neither amount of circulating memory B cells nor their functions are restored by antiretroviral therapy: this may affect antibody mediated immunity, even in well-treated HIV patients. In asplenic childrens a single dose of PCV13 seems sufficient to restore the pool of anti-pneumococcal polysaccharides IgG memory B cells. In adults, it has been reported that a single dose of 7-valent pneumococcal conjugate vaccine induces significant increases in serotype-specific memory B-cell populations, conversely, immunization with PPV23 seems to decrease memory B-cell frequency. However, data on immunological response after PCV13 in HIV positive adults are still scanty and the optimal pneumococcal prophylaxis strategy needs further investigation. Number of PCV13 doses is actually demanded to clinical judgment for each patient; also current Italian indications recommend at least one dose, but till 3 doses seem to be suggested for immunocompromised patients. Present study aims to investigate short and long term immunological response after different standard vaccine schedule and to evaluate pneumococcal nasopharyngeal colonization in vaccinated patients.
The study will be divided in 3 main aims; in the first, the long term immunological response
to PCV13 and PPV23 in HIV+ adults will be evaluated. In a previous clinical trial (PRIN 2009
study, Clinicaltrials: NCT02123433) a cohort of HIV positive adults had been vaccinated
either with 2 doses of PCV13 8 weeks apart or 1 dose of PPV23 (last enrollment: December
2012). Immunoglobulins G (IgGs) against 12 common pneumococcal serotypes included in PCV13
and PPV23 were quantified by ELISA at baseline (BL), 8, 24 and 48 weeks: analysis are still
ongoing; preliminary data revealed that both vaccines were safe and well tolerated and
showed similar immunogenicity. The present study aims to evaluate persistence of long term
(>= 3 years) serological and memory B cells response in those previous vaccinated groups. In
this phase, population will be screened for inclusion and exclusion criteria to entire study
conduction. Once obtained informed consent, patients will be enrolled. Together with the
collection of blood samples for routine purposes, an additional blood sample will be taken
so to run immunological tests (ELISA, ELISpot). It is important to underline that no
invasive procedures are needed for the study, apart from routine clinical practice: blood
specimens will be obtained as part of routine investigations, blood will be hence taken for
CD4+ cell count, viraemia analysis and anti-HIV drug monitoring; enrolled patients will
agree just to donate a blood sample for research purposes. Blood samples will be collected
from all previously PCV13 or PPV23 vaccinated HIV+ subjects and serum antibodies and B cells
isotypes will be analyzed at baseline (BL), that is >= 3 years after a previous PCV13 or
PPV23 vaccination.
The second objective of this study aims to evaluate short and long term immunological
response with different combined vaccine strategies in HIV+ adults. Participants will be
recruited if they'll have needed to receive antipneumococcal vaccines (primary or booster)
according to clinical standard indications.
Elicited immunological response (serum antibodies and B cells isotypes) will be explored at
BL, 8, 24, 48 and 96 weeks after additional different received pneumococcal vaccine
strategies. At BL, after collecting blood samples as previously described for Aim1, every
patient will be assigned to a specific Group on the basis of the received vaccine schedule,
prescribed by clinicians according to individual clinical indications. Short- (30 minutes),
medium- (<=5 days) and long-term adverse reactions will be reported, by clinical evaluation
within 30 minute post-vaccine, phone call at day 5 and anamnestic data collection during
follow up 8, 24, 48 and 96 weeks.
Blood samples will be analyzed at 8, 24, 48 and 96 weeks to evaluate serum antibodies and B
cells isotypes.
Finally, the third aim of the study will lead an epidemiological and microbiological survey
in vaccinated HIV+ adults. At BL, 8, 24, 48 and 96 weeks all clinical-anamnestic data will
be updated, together with blood sample analysis to title IgG towards each vaccinal
pneumococcal polysaccharides and to evaluate B cells isotypes and nasopharyngeal swab for S.
pneumoniae culture, in vitro chemosusceptibility tests, serotyping, clonal analysis by
Multilocus Locus Sequence Typing (MLST).
Carriage will be defined as S. pneumoniae isolation from one or more of the nasal swabs, in
absence of any clinical signs or symptoms; a 12 months clinical follow up will be performed
in colonized patients. All patients developing infections will be followed until resolution.
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Observational Model: Case-Only, Time Perspective: Prospective
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