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1 r protection and support advancement of this attenuated vaccine.
2 eltawzy, was created and evaluated as a live attenuated vaccine.
3 lly serve as a positive-marker modified live-attenuated vaccine.
4 ed vaccine as compared with those given live attenuated vaccine.
5 for rational design of a genetically stable attenuated vaccine.
6 ccine and 36% (95% CI, 0 to 59) for the live attenuated vaccine.
7 that the M2KO virus has potential as a live attenuated vaccine.
8 ants (median age, 11 weeks) administered the attenuated vaccine.
9 hat can be used in the development of a live attenuated vaccine.
10 9% (95% CI, -113 to 33; P=0.55) for the live attenuated vaccine.
11 ed for the inactivated vaccines and the live attenuated vaccine.
12 at it may serve as the starting point for an attenuated vaccine.
13 formation to take steps toward developing an attenuated vaccine.
14 a safe and potentially more efficacious live attenuated vaccine.
15 pism of a virus is a new approach for a live attenuated vaccine.
16 o and supports targeting the SH gene in live attenuated vaccines.
17 s are good candidates for the design of live attenuated vaccines.
18 ILTV vaccines are less efficacious than live attenuated vaccines.
19 y attenuate hMPV for the development of live attenuated vaccines.
20 aramyxoviruses for rationally designing live attenuated vaccines.
21 hich combines the advantages of DNA and live attenuated vaccines.
22 t can be mutated to generate successful live attenuated vaccines.
23 culture has hindered the development of live-attenuated vaccines.
24 ines but not in children who received highly attenuated vaccines.
25 ontribute to virulence, and could be used as attenuated vaccines.
26 serve as a model for the rational design of attenuated vaccines.
27 tic deletion to produce whole parasite-based attenuated vaccines.
28 that induced by live virus and possibly live attenuated vaccines.
29 ors, and may differ for inactivated and live attenuated vaccines.
30 with vhs deleted have been proposed as live-attenuated vaccines.
31 f non-toxigenic C. difficile strains as live attenuated vaccines.
32 r approach for prevention is the use of live attenuated vaccines.
33 inactivated vaccines and cold-adapted, live attenuated vaccines.
34 or development of classical swine fever live attenuated vaccines.
35 e pathogenesis of HAV and the development of attenuated vaccines.
36 poor or diminished efficacy compared to live attenuated vaccines.
37 iviral discovery and development of new live attenuated vaccines.
38 erstand virus biology and develop novel live attenuated vaccines.
39 d activity is a strategy for generating live-attenuated vaccines.
40 imals (DIVA tests) for established killed or attenuated vaccines.
41 ay be more informative on the safety of live-attenuated vaccines.
42 on as safe, immunogenic, and protective live-attenuated vaccines.
43 r receipt of dose 1 among recipients of live attenuated vaccine (3.8%) than among recipients of inact
47 tential strategy to develop a neurovirulence-attenuated vaccine against chickenpox and herpes zoster
49 most promising candidates for a genetically attenuated vaccine against malaria (5) , as a unique and
50 ned F. novicida mutant (DeltaiglC) as a live attenuated vaccine against subsequent intranasal challen
52 e possibilities for developing improved live attenuated vaccines against arteriviruses and other viru
53 ons for development of both subunit and live-attenuated vaccines against ETEC and other enteric patho
54 ral infection and strategies to develop live attenuated vaccines against flaviviral species.IMPORTANC
55 eficient chlamydial strains function as live attenuated vaccines against genital and ocular infection
58 imilar approach may guide the design of live-attenuated vaccines against Lassa and other arenaviral h
59 dy may aid in the design of efficacious live attenuated vaccines against PEDV, as well as other CoVs
60 the polymerase could be used to design live attenuated vaccines against serious pathogens within the
61 erapeutics and the development of killed and attenuated vaccines against this important emerging path
63 ) and Card9(-/-) mice immunized with a live, attenuated vaccine also fail to acquire protective immun
67 lity control of new lots of the current live-attenuated vaccine and provide insight for the rational
69 the development of rationally-designed live-attenuated vaccines and antivirals for control of outbre
70 ebo-controlled trial of inactivated and live attenuated vaccines and compared titers in subjects with
71 s display characteristics desirable for live attenuated vaccines and hold potential as vaccine candid
72 r mucosal application in humans, use of live-attenuated vaccines and microbial vectors, and productio
74 association between revaccination with live attenuated vaccines and off-target infections are needed
75 uperseded by a final report, studies of live-attenuated vaccine, and studies of prepandemic seasonal
76 responses similar to those elicited by live-attenuated vaccines, and its flexibility permits the fas
77 ebo-controlled trial of inactivated and live attenuated vaccines, and we evaluated the laboratory end
87 ge to lentiviral vaccine immunity, even when attenuated vaccines are used that, to date, achieve the
88 ay serve as a novel approach to develop live attenuated vaccines as well as antiviral drugs for pneum
90 y can lead to the development of novel, live attenuated vaccines, as well as antiviral drugs for pneu
91 irway selectively recruited airway Tregs and attenuated vaccine-augmented disease, reducing weight lo
93 rulence factors, we hypothesized that a live-attenuated vaccine based on PA14 might elicit a broader
95 deration should be taken when designing live attenuated vaccines based on deletions of nonstructural
96 venue for the development of arenavirus live attenuated vaccines based on rearrangement of their vira
97 ed drastically following the introduction of attenuated vaccines, but progress toward the eradication
98 A single inoculation of the RVF MP-12 live attenuated vaccine by the aerosol or intranasal route ma
99 The fact that uncontrolled replication of an attenuated vaccine can lead to regaining of its virulenc
101 f the p27 gene could be considered as a live attenuated vaccine candidate against visceral leishmania
103 is not available, and the more advanced live attenuated vaccine candidate in clinical trials requires
104 was then assessed for its efficacy as a live attenuated vaccine candidate in mice after challenge wit
109 ike HEp-2 cells, in which wild-type and live-attenuated vaccine candidate viruses grow equally well,
112 In our research, we developed novel live attenuated vaccine candidates against chikungunya virus
113 y of a CD-based approach for developing live-attenuated vaccine candidates against human-pathogenic a
114 viruses might have a great potential as live attenuated vaccine candidates against SIV infections of
115 onal development of safe and protective live attenuated vaccine candidates based on genome reorganiza
117 f the virus, many of which were developed as attenuated vaccine candidates by serial passage in fibro
118 and provides an approach for generating live-attenuated vaccine candidates for emerging coronaviruses
120 information for the rational design of live attenuated vaccine candidates for other viral hemorrhagi
121 tion as a target for rational design of live attenuated vaccine candidates for RSV and perhaps other
122 be assembled and have been developed as live attenuated vaccine candidates for several flaviviruses.
123 o-recover RV strains such as low-replicating attenuated vaccine candidates or low-cell culture passag
124 ential for further development as novel live attenuated vaccine candidates that may rapidly control d
125 s strategy may be useful for generating live attenuated vaccine candidates that prevent disease and f
126 fely attenuate FMDV and further develop live attenuated vaccine candidates to control such a feared l
127 genicity, justifying their inclusion in live attenuated vaccine candidates to protect against the cur
128 deISGylase activity for development of live attenuated vaccine candidates, and ISG15 as a novel biot
129 testing the potential of the three forms as attenuated vaccine candidates, strain 4295 was inoculate
138 nogenicity and protective efficacy of a live attenuated vaccine consisting of a recombinant severe ac
139 xed viral populations and indicate that live-attenuated vaccines containing virulent virus may be saf
142 o the development of safe and effective live attenuated vaccines directed against VEEV and other rela
143 o the development of safe and effective live attenuated vaccines directed against VEEV and perhaps ot
144 e of virulent revertant viruses in some live-attenuated vaccines, disease from vaccination is rare.
145 hus far, the goal of developing a safe, live attenuated vaccine effective after a single dose has rem
147 Isolation frequency was lowest among live attenuated vaccine failures, a reflection of lower speci
150 reviously reported that an experimental live attenuated vaccine for equine infectious anemia virus (E
155 d an opportunity to design a successful live-attenuated vaccine for SARS-CoV and opens avenues for tr
156 herefore, NU14 DeltawaaL is a candidate live-attenuated vaccine for the treatment and prevention of a
157 , indicating the potential of TCRV as a live-attenuated vaccine for the treatment of Argentine hemorr
161 as a novel target to rationally design live attenuated vaccines for aMPV and perhaps other paramyxov
162 ding may also enable the development of live attenuated vaccines for both RSV and other members of th
163 approach to produce safe and effective live-attenuated vaccines for DENV and other insect-borne viru
165 the development of safe and efficacious live attenuated vaccines for hMPV and other human paramyxovir
166 as a novel target to rationally design live attenuated vaccines for hMPV and perhaps other paramyxov
170 also facilitate the development of new live attenuated vaccines for VSV, and perhaps other NNS RNA v
171 ccine constructs use the E protein in a live attenuated vaccine format, utilizing a backbone derived
173 CoVs), and the inactivation of nsp16 in live attenuated vaccines has been attempted for several betac
177 ed in various animal lentivirus models, live attenuated vaccines have proven to be the most effective
179 can be restored by immunization with highly attenuated vaccines.IMPORTANCE Chronic viral infections
184 Because concerns exist about the use of live-attenuated vaccines in immunocompromised individuals, a
187 vanted inactivated vaccine, but not the live-attenuated vaccine, induced a substantial serum IgG anti
188 ed to further define the nature of the live, attenuated vaccine-induced immunity against Coccidioides
190 ogy, including human host-pathogen and live, attenuated vaccine interactions; host and cell type rest
191 ancestral immunogens, because the Env of the attenuated vaccine is a direct ancestor to the variant p
192 e vaccine than the previously developed live attenuated vaccine is needed for combating Francisella t
193 ptive immune response generated to this live attenuated vaccine is regulated by both the presence of
195 reassortant (ML29) is a LASV candidate live-attenuated vaccine (LAV) that has shown promising result
196 dmonston-Zagreb has long been used as a live-attenuated vaccine (LAV) to protect against measles, not
203 regulated immune system, and/or exposure to attenuated vaccines may enhance trained immunity to limi
204 unity in individuals unable to receive live, attenuated vaccines may have employment implications.
207 Boosting T cell-mediated immunity by live attenuated vaccine Mycobacterium bovis bacillus Calmette
208 s included a chimeric H8/1, intranasal, live-attenuated vaccine on day 1 followed by a non-adjuvanted
209 V and to explore its potential use as a live-attenuated vaccine or a vaccine vector for the treatment
210 of TCRV and also its potential use as a live-attenuated vaccine or a vaccine vector for the treatment
212 nd safety concerns regarding the use of live attenuated vaccines or potent adjuvants in this populati
213 enaviruses, for their implementation as live-attenuated vaccines or vaccine vectors.IMPORTANCE To dat
215 pening the possibility for its use as a live-attenuated vaccine platform for ZIKV and other clinicall
216 report the development of a recombinant live-attenuated vaccine platform strain that retains the pote
221 valent rotavirus vaccine (RV5), a live, oral attenuated vaccine, prevented 98% of severe rotavirus di
224 nza A (H3N2), 90% of placebo and 87% of live attenuated vaccine recipients but only 23% of inactivate
228 f the risks and benefits indicates that live attenuated vaccine should be a highly effective, safe va
231 s of JUNV have been documented, and a highly attenuated vaccine strain (Candid #1) was generated and
232 igen polymerase) deletion mutant of Ft. live attenuated vaccine strain (Ft.LVS), designated Ft.LVS::D
234 llei Deltaasd mutant may be a promising live attenuated vaccine strain and a biosafe strain for consi
235 some success in animal models, including an attenuated vaccine strain based on an isolate from La Re
236 otection against plague, we developed a live-attenuated vaccine strain by deleting the Braun lipoprot
238 on, DeltaP(rfaH178), was introduced into the attenuated vaccine strain chi9241 (DeltapabA DeltapabB D
239 the highly pathogenic Brescia strain and the attenuated vaccine strain CS were constructed and evalua
241 ptomic analysis of the M. gallisepticum live attenuated vaccine strain F and the virulent strain R(lo
244 virulent Mycobacterium tuberculosis with the attenuated vaccine strain Mycobacterium bovis bacillus C
245 rensis organisms were comparable to the live attenuated vaccine strain of Francisella tularensis subs
247 ity of the glycoprotein of the Candid#1 live-attenuated vaccine strain of JUNV in MACV replication an
248 c-resistance markers in a single recombinant attenuated vaccine strain of Salmonella enterica serotyp
250 (cryo-EM), we determined the structure of an attenuated vaccine strain, TC-83, of VEEV to 4.4 A resol
253 reverse genetics, a set of experimental live attenuated vaccine strains based on recombinant H5N1 inf
259 strains of Salmonella may be useful as live attenuated vaccine strains or as vehicles for heterologo
268 DENV or vaccination with tetravalent dengue attenuated vaccines (TDLAV) recognize ZIKV-derived pepti
269 ed influenza in the group that received live attenuated vaccine than in the group that received inact
270 stration of dose 1 was more common with live attenuated vaccine than with inactivated vaccine, primar
272 ribe the first genetically engineered, live, attenuated vaccine that protects both BALB/c and C57BL/6
273 has resulted in the development of two live, attenuated vaccines that are now licensed in many countr
274 might be deleted for the development of live attenuated vaccines that would be safer to use in situat
275 didates demonstrate the potential for a live attenuated vaccine to protect against disease caused by
277 nstitutes of Health (NIH) has developed live attenuated vaccines to each of the 4 serotypes of dengue
278 Yersinia species have been utilized as live attenuated vaccines to prime protective immunity against
280 nant Sendai virus (rSeV) was used as a live, attenuated vaccine vector for intranasal inoculation and
281 ting the feasibility of using TCRV as a live-attenuated vaccine vector for the treatment of JUNV and
282 of heterologous flavivirus species as a live attenuated vaccine vector is not likely to generate opti
284 othesized that persistent replication of the attenuated vaccine virus modulates inflammatory response
287 ains unclear whether the replication of live attenuated vaccine viruses will be similarly enhanced wh
290 ve (95% CI, 47 to 70; P<0.001), and the live attenuated vaccine was not observed to be effective (vac
291 stalk and catalytic domains of NA as a live attenuated vaccine was shown to confer a strong IAV-spec
293 16-2017 A(H1N1)pdm09 strain used in the live attenuated vaccine was unchanged from 2015-2016, the Adv
296 and human infections, new candidate H5 live attenuated vaccines were developed by using two differen
297 ion were higher among the recipients of live attenuated vaccine who were 6 to 11 months of age (6.1%)
298 fer a general approach to the development of attenuated vaccines with well-defined antigenicities and
299 ine and 29% (95% CI, -14 to 55) for the live attenuated vaccine, with a relative efficacy of 60% (95%
300 A single intranasal administration of live attenuated vaccine without adjuvant was sufficient to in