Comparative study of IgA V H 3 gene usage in healthy TST − and TST + population exposed to tuberculosis: deep sequencing analysis
The acquired immune response against tuberculosis is commonly associated with T‐cell responses with little known about the role of B cells or antibodies. There have been suggestions that B cells and humoral immunity can modulate the immune response to Mycobacterium tuberculosis . However, the mechan...
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Veröffentlicht in: | Immunology 2015-02, Vol.144 (2), p.302-311 |
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Format: | Artikel |
Sprache: | eng |
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Zusammenfassung: | The acquired immune response against tuberculosis is commonly associated with T‐cell responses with little known about the role of B cells or antibodies. There have been suggestions that B cells and humoral immunity can modulate the immune response to
Mycobacterium tuberculosis
. However, the mechanisms involving B‐cell responses in
M. tuberculosis
are not fully understood, in particular the antibody gene preferences. We hypothesized that a preferential use of V genes can be seen associated with resistance to infection mainly in the IgA isotype, which is of prominent importance for infection by pathogens via the mucosal route. We studied healthy individuals with long‐term exposure to tuberculosis, infected (
TST
+
) and uninfected
TST
−
) with
M. tuberculosis
. From a total of 22 V genes analysed, the
TST
−
population preferred the
V
H
3‐23 and V
κ
1 genes. The
V
H
3‐23 genes were subsequently subjected to 454 amplicon sequencing. The
TST
−
population showed a higher frequency of the D3‐10 segment compared with the D3‐22 segment for the
TST
+
population. The J segment usage pattern was similar for both populations with J4 segment being used the most. A preferential pairing of J4 segments to D3‐3 was seen for the
TST
−
population. The antibodyome difference between both populations suggests a preference for antibodies with
V
H
3‐23, D3‐3,
J
H
4 gene usage by the
TST
−
population that could be associated with resistance to infection with
M. tuberculosis
. |
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ISSN: | 0019-2805 1365-2567 |
DOI: | 10.1111/imm.12372 |