大島 信子

Four kinds of avian-derived H5N1 influenza virus, A/Vietnam/1194/2004 (Clade 1), A/Indonesia/5/2005 (Clade 2.1), A/Qinghai/1A/2005 (Clade 2.2), and A/Anhui/1/2005 (Clade 2.3), have been stocked in Japan for use as pre-pandemic vaccines. When a pandemic occurs, these viruses would be used as vaccines in the hope of inducing immunity against the pandemic virus. We analyzed the specificity of antibodies (Abs) produced by B lymphocytes present in the blood after immunization with these vaccines. Eighteen volunteers took part in this project. After libraries of Ab-encoding sequences were constructed using blood from subjects vaccinated with these viruses, a large number of clones that encoded Abs that bound to the virus particles used as vaccines were isolated. These clones were classified into two groups according to the hemagglutination inhibition (HI) activity of the encoded Abs. While two-thirds of the clones were HI positive, the encoded Abs exhibited only restricted strain specificity. On the other hand, half of the HI-negative clones encoded Abs that bound not only to the H5N1 virus but also to the H1N1 virus; with a few exceptions, these Abs appeared to be encoded by memory B cells present before vaccination. The HI-negative clones included those encoding broadly cross-reactive Abs, some of which were encoded by non-VH1-69 germline genes. However, although this work shows that various kinds of anti-H5N1 Abs are encoded by volunteers vaccinated with pre-pandemic vaccines, broad cross-reactivity was seen only in a minority of clones, raising concern regarding the utility of these H5N1 vaccine viruses for the prevention of H5N1 pandemics.

The relative activity of niacin-related compounds to nicotinic acid was tested as the niacin nutriture in Lactobacillus plantarum ATCC 8014, the strain for the measurement of niacin in foods. As the results, this microorganism could use nicotinuric acid as equimolar as nicotinic acid. The relative niacin activities of N'-methylnicotinamide, pyridine 3-aldehyde, and nicotinamide N-oxide to nicotinic acid were 1/20, 1/30 and 1/40 in molar basis, respectively. While pyridine 3-methanol, nicotinic acid N-oxide, 3-acetylpyridine, β-picoline, N^1-methylnicotinamide, N^1-methylnicotinic acid, 6-hydroxynicotinic acid, 6-aminonicotinamide, quinolinic acid, and cinchomeronic acid did not show niacin activity.