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1 en rendered obsolete by the recombinant OspA Lyme disease vaccine.
2 suggests that DbpA may not be suitable as a Lyme disease vaccine.
3 implicate DBP as a new candidate for a human Lyme disease vaccine.
4 n important consideration in the design of a Lyme disease vaccine.
5 e successfully developed a second-generation Lyme disease vaccine.
6 es a basis for rational design of OspA-based Lyme disease vaccines.
7 articipants enrolled in a phase III trial of Lyme disease vaccine; 118 participants had erythema migr
8 ken to examine the cost-effectiveness of the Lyme disease vaccine and the factors that influence its
10 ol groups: 1) inflammatory arthritis but not Lyme disease vaccine (arthritis controls), 2) Lyme disea
14 yme disease vaccine (arthritis controls), 2) Lyme disease vaccine but not inflammatory arthritis (vac
16 m inflammatory arthritis had developed after Lyme disease vaccine (cases) were compared with 3 contro
17 effectiveness and cost-effectiveness of the Lyme disease vaccine in populations at various levels of
23 ified mRNA (mRNA-LNP) platform to generate a Lyme disease vaccine like the successful clinical vaccin
24 arthritis (vaccine controls), and 3) neither Lyme disease vaccine nor inflammatory arthritis (normal
25 r surface protein (Osp) A has been used as a Lyme disease vaccine that blocks transmission: OspA anti
26 highlighting use of BBI39 proteins as novel Lyme disease vaccines that can target pathogens in the h