Bifidobacterium bifidum 791 (commercially available as B. bifidum BIM B-733D) cell-surface biopolymers (BPs) interact selectively with human serum thyroid peroxidase (TPO) and thyroglobulin (Tg) autoantibodies (anti TPO and anti Tg, respectively). BPanti-TPO and BPanti-Tg were isolated from the soluble fraction of B. bifidum BIM B-733D by affinity chromatography with anti-TPO or anti-Tg, respectively. Homogeneity of affinity eluates (AEanti-TPO and AEanti-Tg) was tested by size exclusion chromatography. For each AE, the elution profiles generated on the basis of absorbance at 280 nm do not conform to ELISA data for functional activity characteristic of BPs. Moreover, high functional activity was detected in chromatographic fractions that had significantly different molecular weights and no absorbance at 280 nm, which suggests a non-protein (carbohydrate) nature of BPanti-TPO and BPanti-Tg. The semi-preparative size exclusion chromatography of AEanti-TPO and AEanti-Tg with detection by refractometer gave 5,000-7,000 Da fractions containing substances that interact selectively with either anti TPO (BPanti-TPO) or anti-Tg (BPanti-Tg) according to ELISA data. Analysis by two-dimensional NMR spectroscopy including a 1H, 13C-heteronuclear single-quantum coherence experiment indicated that both substances are linear α-1,6-glucans. For the first time, an immunological similarity (molecular mimicry) of glycopolymers of B. bifidum BIM B-733D and human thyroid proteins, TPO and Tg, was shown. On the whole, our data point to a possible role of bifidobacteria in the pathogenesis of autoimmune thyroid diseases (ATD). The main requirements for triggering/acceleration or prevention/abrogation of ATD by bifidobacteria through molecular mimicry mechanism are hypothesised to be (1) genetic predisposition to ATD and (2) intestinal epithelium penetration by α-1,6-glucan.

Autoantibodies, molecular mimicry, Bifidobacterium, α-1, 6-glucan

NCBI PubMed ID: 24311320
Publication DOI: 10.3920/BM2013.0015
Journal NLM ID: 101507616
Publisher: Wageningen: Wageningen Academic Publishers
Correspondence: epkiselevayandex.ru
Institutions: The Institute of Bioorganic Chemistry, National Academy of Sciences of Belaru, Acad. Kuprevicha 5/2, 220141 Minsk, Republic of Belarus.
Methods: 13C NMR, 1H NMR, NMR-2D, ELISA, serological methods
 

• Compound ID: 219
  

  -6)-a-D-Glcp-(1-

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  Structure type: homopolymer
  Trivial name: glucan, α-D-glucan, dextran, α-1,6-glucan, α-(1,6)-glucan, dextran, α-(1,6)-glucan, α-1,6 dextran, β-1,3-D-glucan, polysaccharide IOP
  Compound class: EPS, O-polysaccharide, cell wall polysaccharide, glucan, polysaccharide
  Reference(s) to other database(s): GTC:G69605LY, GlycomeDB:2461
  
   
  
  Bifidobacterium bifidum BIM B-733D
  CSDB ID 29235 (all data & tools)

Role of microorganisms in induction of/protection from autoimmune diseases is proven though molecular mechanisms and bacterial/viral/yeast biopolymers responsible for these effects are in the research stage. Autoantobodies (AAbs) to thyroid peroxidase (anti-TPO) and thyroglobulin (anti-Tg) as well as AAbs to transglutaminase 2 (anti-TG2) and antibodies to gliadins (anti-gliadins) are serological markers of autoimmune thyroid disease and celiac disease, respectively, and players in pathogenesis of these autoimmune diseases. In current study, biopolymer of Bifidobacterium bifidum BIM B-733D that interacts selectively with anti-gliadins (Bb-Ganti-gliadins) was isolated by affinity chromatography with anti-gliadins, purified by size exclusion chromatography on TSK 40 gel and identified by NMR as linear α-(1→6)-d-glucan with molecular mass about 5000?Da. It was proven that compounds Bb-Ganti-gliadins and Bb-Ganti-TPO/Bb-Ganti-Tg isolated early from the same strain [Kiseleva, E. P. et al., Benef Microbes.2013, 4, 375 -391] are the same substance designated GBb. Its unique immunochemical property is the ability to interact selectively with anti-TPO, anti-Tg, anti-TG2 and anti-gliadins in presence of no less than 10-fold excess of total immunoglobulins of class G (tIgG), as it was proven by ELISA. Synthesis of GBb-bovine serum albumin (GBb-BSA) conjugate is an example of increasing the reliability and reproducibility of ELISA results by mediated immobilization of a polysaccharide covalently attached to a well-adsorbed protein. Taking into account that there are population of bispecific anti-gliadins (anti-gliadins and anti-TG2 simultaneously) we regard our data as first argument in favor of hypothesis that GBb differentiates between human AAbs per se and other human Ig (e.g. antibodies to antigens of infectious agents) due to its binding with a yet unidentified site which is present in the molecules of all AAbs (independently on their specificity) and absent in other human Igs.

Autoantibodies, ELISA, Bifidobacteria, Autoimmune thyroid disease, Celiac disease, Linear α-(1>6)-d-glucan

NCBI PubMed ID: 29422338
Publication DOI: 10.1016/j.carres.2017.12.008
Journal NLM ID: 0043535
Publisher: Elsevier
Correspondence: epkiselevayandex.ru
Institutions: N.D. Zelinsky Institute of Organic Chemistry, Russian Academy of Sciences, Moscow, Russia, Institute of Bioorganic chemistry, National Academy of Sciences of Belarus, Minsk, Belarus, Institute of Microbiology, National Academy of Sciences of Belarus, Minsk, Belarus
Methods: 1H NMR, ELISA, serological methods, SEC, conjugation
 

• Compound ID: 13045
  

  -6)-a-D-Glcp-(1-

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  Structure type: homopolymer ; 5000
  Reference(s) to other database(s): GTC:G69605LY
  
   
  
  Bifidobacterium bifidum BIM B-733D
  CSDB ID 12923 (all data & tools)