Own). These data suggest that complex formation of GM1-like and GD1a-like LOSs could induce the production of anti-GM1b antibodies in such patients.Induction of anti-GM1b antibodies in miceSensitization of immune-naive mice with C. jejuni (GC105) bearing GM1-like and GD1a-like LOSs induced the production of high titers (OD >1.0) of anti-GM1b antibodies in 4 of 13 mice, as well as anti-GM1 antibodies in 10 mice and anti-GD1a antibodies in 9 mice. In contrast, immunization with C. jejuni (NCTC11168) bearing GM1-like and GM2-like LOSs did not induce the production of anti-GM1b antibodies in any of the 8 mice tested, and resulted in the induction of anti-GM1 antibodies in 7 mice and anti-GD1a antibodies in 5 mice.Cross-reactive antibodies to cM1/D1a with GM1bAnti-cM1/D1a IgG antibodies were found in 20 of the 119 patients with neuropathy and its related conditions from whom C. jejuni had been isolated, whereas no anti-cM1/D1a antibodies were detected in the sera from 105 healthy subjects and 83 patients with other neurological disorders such as amyotrophic lateral sclerosis and myasthenia gravis. Five of the 20 patients carried anti-cM1/D1a IgG antibodies (1:500 to 1:16,000), but neither anti-GM1 nor anti-GD1a IgG antibodies (Table 1). All the 5 patients had GBS, but not ICG-001 site Miller Fisher syndrome. Surprisingly, all of the 5 patients carrying anti-cM1/D1a antibodies had high titers of anti-GM1b IgG antibodies (1:16,000 to 1:128,000). Fig 2A demonstrates that IgG antibodies from Patient 4 in Table 1 reacted with GM1b and cM1/D1a, but with neither GM1 nor GD1a. Anti-cM1/D1a IgG antibodies from the patients were dose-dependently absorbed by GM1b, as well as by cM1/D1a, but by neither GM1 nor GD1a, indicating that anti-cM1/D1a antibodies cross-react with GM1b. Fig 2B shows representative results using serum from a patient with GBS after C. jejuni enteritis (S6325). Anti-GM1b antibodies also were absorbed by cM1/D1a, as well as by GM1b, but by neither GM1 nor GD1a.PLOS ONE | DOI:10.1371/journal.pone.0124004 April 13,5/Campylobacter LOS Complex in GBSFig 2. Complex of GM1 and GD1a (cM1/GD1a). (A) Immunostaining with IgG antibodies from Patient 4. Bovine brain ganglioside mixture (lane 1), authentic GM1b (lane 2) and a mixture of GM1 and GD1a (lane 3) were spotted on a thin-layer chromatogram plate and developed with a solvent. After the development of the plate, a mixture of GM1 and GD1a was spotted and not further resolved (lane 4). The patient’s IgG strongly bound to GM1b (asterisk) with the development, and to the mixture of GM1 and GD1a that was not separated (arrow). In contrast, the binding nearly Actinomycin IV dose disappeared after separation of GM1 and GD1a with the development (arrow head). (B) Cross-reactivity of the antibodies to cM1/D1a with GM1b. IgG anti-cM1/D1a antibodies of serum (S6325) from a patient with GBS subsequent to C. jejuni enteritis were dose-dependently absorbed by GM1b, as well as by cM1/D1a, whereas the antibodies were absorbed by neither GM1 nor GD1a. doi:10.1371/journal.pone.0124004.gAnti-GM1b antibodies and C. jejuni LOSsBased on the ganglioside-mimicking pattern of C. jejuni LOSs, the 119 neuropathic patients were classified into three groups; (i) both GM1 and GD1a mimics, (ii) GM1 mimic alone, and (iii) neither GM1 nor GD1a mimic (Table 2). The first group of patients more often had IgG antibodies to GM1 and GD1a, as well as to cM1/D1a, than the others, and each difference was statistically significant. The autoantibody response was.Own). These data suggest that complex formation of GM1-like and GD1a-like LOSs could induce the production of anti-GM1b antibodies in such patients.Induction of anti-GM1b antibodies in miceSensitization of immune-naive mice with C. jejuni (GC105) bearing GM1-like and GD1a-like LOSs induced the production of high titers (OD >1.0) of anti-GM1b antibodies in 4 of 13 mice, as well as anti-GM1 antibodies in 10 mice and anti-GD1a antibodies in 9 mice. In contrast, immunization with C. jejuni (NCTC11168) bearing GM1-like and GM2-like LOSs did not induce the production of anti-GM1b antibodies in any of the 8 mice tested, and resulted in the induction of anti-GM1 antibodies in 7 mice and anti-GD1a antibodies in 5 mice.Cross-reactive antibodies to cM1/D1a with GM1bAnti-cM1/D1a IgG antibodies were found in 20 of the 119 patients with neuropathy and its related conditions from whom C. jejuni had been isolated, whereas no anti-cM1/D1a antibodies were detected in the sera from 105 healthy subjects and 83 patients with other neurological disorders such as amyotrophic lateral sclerosis and myasthenia gravis. Five of the 20 patients carried anti-cM1/D1a IgG antibodies (1:500 to 1:16,000), but neither anti-GM1 nor anti-GD1a IgG antibodies (Table 1). All the 5 patients had GBS, but not Miller Fisher syndrome. Surprisingly, all of the 5 patients carrying anti-cM1/D1a antibodies had high titers of anti-GM1b IgG antibodies (1:16,000 to 1:128,000). Fig 2A demonstrates that IgG antibodies from Patient 4 in Table 1 reacted with GM1b and cM1/D1a, but with neither GM1 nor GD1a. Anti-cM1/D1a IgG antibodies from the patients were dose-dependently absorbed by GM1b, as well as by cM1/D1a, but by neither GM1 nor GD1a, indicating that anti-cM1/D1a antibodies cross-react with GM1b. Fig 2B shows representative results using serum from a patient with GBS after C. jejuni enteritis (S6325). Anti-GM1b antibodies also were absorbed by cM1/D1a, as well as by GM1b, but by neither GM1 nor GD1a.PLOS ONE | DOI:10.1371/journal.pone.0124004 April 13,5/Campylobacter LOS Complex in GBSFig 2. Complex of GM1 and GD1a (cM1/GD1a). (A) Immunostaining with IgG antibodies from Patient 4. Bovine brain ganglioside mixture (lane 1), authentic GM1b (lane 2) and a mixture of GM1 and GD1a (lane 3) were spotted on a thin-layer chromatogram plate and developed with a solvent. After the development of the plate, a mixture of GM1 and GD1a was spotted and not further resolved (lane 4). The patient’s IgG strongly bound to GM1b (asterisk) with the development, and to the mixture of GM1 and GD1a that was not separated (arrow). In contrast, the binding nearly disappeared after separation of GM1 and GD1a with the development (arrow head). (B) Cross-reactivity of the antibodies to cM1/D1a with GM1b. IgG anti-cM1/D1a antibodies of serum (S6325) from a patient with GBS subsequent to C. jejuni enteritis were dose-dependently absorbed by GM1b, as well as by cM1/D1a, whereas the antibodies were absorbed by neither GM1 nor GD1a. doi:10.1371/journal.pone.0124004.gAnti-GM1b antibodies and C. jejuni LOSsBased on the ganglioside-mimicking pattern of C. jejuni LOSs, the 119 neuropathic patients were classified into three groups; (i) both GM1 and GD1a mimics, (ii) GM1 mimic alone, and (iii) neither GM1 nor GD1a mimic (Table 2). The first group of patients more often had IgG antibodies to GM1 and GD1a, as well as to cM1/D1a, than the others, and each difference was statistically significant. The autoantibody response was.
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