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1 4.4%) and 64 099 (25.6%) not vaccinated with rotavirus vaccine.
2 hort of infants who received the pentavalent rotavirus vaccine.
3 within 7 days of getting their first dose of rotavirus vaccine.
4 ompared with infants who did not receive the rotavirus vaccine.
5 ccine, whereas one was related to monovalent rotavirus vaccine.
6 ntries that were among the early adopters of rotavirus vaccine.
7 0-March 31, 2001), only 2 stories focused on rotavirus vaccine.
8 ation-sudden condemnation" pattern seen with rotavirus vaccine.
9 evolution may undermine the effectiveness of rotavirus vaccines.
10 strain-specific effectiveness of RV1 and RV5 rotavirus vaccines.
11 ountries and evaluating additional candidate rotavirus vaccines.
12 widely marketed, licensed, live virus, oral rotavirus vaccines.
13 e for monitoring the postlicensure safety of rotavirus vaccines.
14 can infants prior to the introduction of new rotavirus vaccines.
15 cape mutants noted since the introduction of rotavirus vaccines.
16 llance is essential to assess the success of rotavirus vaccines.
17 protection provided by live attenuated oral rotavirus vaccines.
18 use model for active protection studies with rotavirus vaccines.
19 nt and the variety of approaches to creating rotavirus vaccines.
20 or the development of the next generation of rotavirus vaccines.
21 potentially could be prevented by the use of rotavirus vaccines.
22 e design and testing of parenteral candidate rotavirus vaccines.
23 infants who received 1 of several live oral rotavirus vaccines.
26 e significantly less likely to have received rotavirus vaccine (33/44 [73%] unvaccinated) compared wi
28 ssociation between IS and the first licensed rotavirus vaccine, a reassortant-tetravalent, rhesus-bas
31 declined from 54.8% (95% CI, 48.3%-61.5%) in rotavirus vaccine age-ineligible children to 20.0% (95%
32 ective association exists between receipt of rotavirus vaccine and being hospitalized or visiting the
33 een the tetravalent rhesus-human reassortant rotavirus vaccine and intussusception has increased the
34 Plasma IgA levels specific for antigens in rotavirus vaccine and oral polio vaccine containing poli
35 an association between vaccination with the rotavirus vaccine and the development of intussusception
36 ed implementation of existing interventions (rotavirus vaccine and zinc) are needed to prevent diseas
37 re data has identified a causal link between rotavirus vaccines and intussusception in some settings.
38 We review clinical trial data for available rotavirus vaccines and summarize postlicensure data on e
41 versity in Europe before the introduction of rotavirus vaccines, and the network will provide a robus
44 ory and clinical studies, safe and effective rotavirus vaccines are approaching regulatory approval.
52 vaccine in an African setting, especially as rotavirus vaccines are introduced into an increasing num
54 ine was associated with intussusception, new rotavirus vaccines are monitored postlicensure for any s
58 nd immunogenicity of the P2-VP8-P[8] subunit rotavirus vaccine at different doses in South African to
60 ues to recommend that all US infants receive rotavirus vaccine based on the age and precaution/contra
62 lable on the safety of the second-generation rotavirus vaccines both in the United States and interna
63 itis have declined since the introduction of rotavirus vaccines, but the burden of norovirus-associat
65 A quadrivalent precursor to the pentavalent rotavirus vaccine candidate RotaTeq was evaluated in a 3
69 rhesus macaques in vaccine trials with human rotavirus vaccine candidates is the major objective of f
70 rtant implications for the development of G9 rotavirus vaccine candidates, as the strain with the bro
72 %) one dose, and 136 (25%) no doses of human rotavirus vaccine, compared with 1434 rotavirus-negative
84 end of 2013, the majority of countries using rotavirus vaccine during the review period were low-mort
85 of US children, we observed that RV5 and RV1 rotavirus vaccines each provided a lasting and broadly h
86 l study at 6 public sector sites to estimate rotavirus vaccine effectiveness (VE) in age-eligible chi
89 ion of rotavirus strains and strain-specific rotavirus vaccine effectiveness after vaccine introducti
91 gnificant correlation between IgA titers and rotavirus vaccine efficacy and hypothesize that a critic
92 e used regional rotavirus disease burden and rotavirus vaccine efficacy data, global natural intussus
94 on cases and mortality potentially caused by rotavirus vaccine for each of the 14 countries and compa
95 nd tolerability of a monovalent human-bovine rotavirus vaccine for severe rotavirus gastroenteritis i
100 ction of children who are age-ineligible for rotavirus vaccine has also been observed in some high an
115 The pentavalent human-bovine reassortant rotavirus vaccine (HBRV) is directed against each of the
117 mmended schedule for receipt of 2-dose human rotavirus vaccine (HRV) coincides with receipt of the fi
118 bella vaccine (MR) and a third dose of human rotavirus vaccine (HRV; MR + HRV), compared with MR give
119 tiveness of a two-dose schedule of the human rotavirus vaccine (HRV; Rotarix) given early at 6 and 10
120 have received at least one dose of the human rotavirus vaccine (ie, those born after June 14, 2009) a
121 strategies should be evaluated for improving rotavirus vaccine immunogenicity in high burden countrie
122 MA) to identify observational evaluations of rotavirus vaccine impact among children <5 years of age
123 Our findings might implicate challenges for rotavirus vaccine implementation in a European populatio
124 rotavirus in Rwanda fell substantially after rotavirus vaccine implementation, including among older
125 pilot introduction of the Rotarix live, oral rotavirus vaccine in all public health facilities in Lus
126 g and establishes the public health value of rotavirus vaccine in an African setting, especially as r
129 is unique project, which is developing a new rotavirus vaccine in India with the use of Indian strain
130 he vaccine effectiveness of monovalent human rotavirus vaccine in preventing admission to hospital fo
131 vaccine effectiveness of 1 or more doses of rotavirus vaccine in preventing rotavirus gastroenteriti
132 Together with the demonstrated impact of rotavirus vaccine in reducing population hospitalization
133 tions raise concerns regarding the safety of rotavirus vaccine in severely immunocompromised patients
136 recast model was used to predict adoption of rotavirus vaccine in the poorest countries in the world.
139 round the performance of orally administered rotavirus vaccines in developing countries, vaccine impl
141 roduction Plan to close the gap of access to rotavirus vaccines in industrialized and developing coun
142 level of protection detected for the current rotavirus vaccines in low-income versus high-income sett
144 ctiveness of RV5 (RotaTeq) and RV1 (Rotarix) rotavirus vaccines in preventing rotavirus gastroenterit
145 lso allow assessment of the effectiveness of rotavirus vaccines in programmatic use and the need for
148 he study period, 207,955 doses of monovalent rotavirus vaccine (including 115,908 first doses and 92,
149 acy stems from studies of previous candidate rotavirus vaccines, including bovine and rhesus rotaviru
150 clinical trials for the current and previous rotavirus vaccines indicate that, as countries begin to
151 unization Hotline during the period in which rotavirus vaccine information was captured (July 1-Decem
152 umented an intussusception risk with current rotavirus vaccines, international data indicate a possib
153 countries in sub-Saharan Africa to introduce rotavirus vaccine into its national immunization program
154 in the Newly Independent States to introduce rotavirus vaccine into its national immunization program
155 ome African country to introduce pentavalent rotavirus vaccine into its routine national immunisation
156 esburg, before and after the introduction of rotavirus vaccine into South Africa's national immunizat
158 recommendation that all countries introduce rotavirus vaccine into their national immunization progr
159 Accelerated development and introduction of rotavirus vaccines into global immunisation programmes h
163 us vaccine introduction (2009-2011) and post-rotavirus vaccine introduction (2013-2014) periods were
164 ur new estimates can be used to advocate for rotavirus vaccine introduction and to monitor the effect
165 rus vaccination are important for supporting rotavirus vaccine introduction in Africa, where limited
168 ill allow measurement of the rapid impact of rotavirus vaccine introduction on the heavy burden of ro
169 e basis of a $9.18 (53 LE) single-dose cost, rotavirus vaccine introduction would cost the Ministry o
172 hospitalizations, temporally associated with rotavirus vaccine introduction, was observed in children
184 Live pentavalent human-bovine reassortant rotavirus vaccine is recommended in the United States fo
188 involved in the development of a multivalent rotavirus vaccine, it is important to identify the serot
191 ation formulation, zinc supplementation, and rotavirus vaccines-make now the time to revitalise effor
197 14 Latin American countries currently using rotavirus vaccine must now weigh the health benefits ver
198 of human rotaviruses for change suggest that rotavirus vaccines must provide good heterotypic protect
201 re low-mortality countries and the impact of rotavirus vaccine on global estimates of rotavirus morta
202 strain replacement after the introduction of rotavirus vaccines, particularly in developing countries
205 In 2003, the GAVI Alliance launched the Rotavirus Vaccine Program and the Accelerated Developmen
208 ound direct and herd immunity impacts of the rotavirus vaccine program in young children in the Repub
211 ether monovalent (RV1) and pentavalent (RV5) rotavirus vaccines provide adequate protection against d
214 he combined vaccine regimens with individual rotavirus vaccine regimens, we included in the experimen
215 global natural intussusception and regional rotavirus vaccine-related risk estimates, and country-sp
217 Rotarix (GlaxoSmithKline), a newly licensed rotavirus vaccine requiring 2 doses, may have the potent
218 n and immune activation were correlated with rotavirus vaccine responses in 68 human immunodeficiency
219 ors aimed to estimate the effectiveness of a rotavirus vaccine (rhesus rotavirus vaccine-tetravalent
221 an immunological correlate of protection for rotavirus vaccines (Rotarix [RV1] and RotaTeq [RV5]) wou
224 after vaccination with the live tetravalent rotavirus vaccine RotaShield resulted in voluntary withd
225 temporal association between a first dose of rotavirus vaccine (Rotashield) and infant intussusceptio
226 sure surveillance determined that a previous rotavirus vaccine, RotaShield, caused intussusception in
228 after vaccination with the second-generation rotavirus vaccines RotaTeq (RV5, a pentavalent vaccine)
229 vaccine effectiveness (VE) of a pentavalent rotavirus vaccine (RotaTeq) against rotavirus diarrhea.
230 amples collected during clinical trials of a rotavirus vaccine (RotaTeq) and identified a serotype in
231 live, pentavalent, human-bovine reassortant rotavirus vaccine (RotaTeq; Merck) in developed countrie
232 ing the tetravalent rhesus-human reassortant rotavirus vaccine (RRV-TV) were reported to the Vaccine
233 ine, a reassortant-tetravalent, rhesus-based rotavirus vaccine (RRV-TV), led to the withdrawal of the
234 live oral vaccine, tetravalent, rhesus-based rotavirus vaccine (RRV-TV), which was incorporated into
235 a surveillance to evaluate monovalent G1P[8] rotavirus vaccine (RV1) efficacy and understand variable
240 irst African nations to introduce monovalent rotavirus vaccine (RV1) into its childhood immunization
243 sessed the association of the new monovalent rotavirus vaccine (RV1) with intussusception after routi
245 tion (IS) associated with currently licensed rotavirus vaccines (RV1 [Rotarix; GSK] and RV5 [RotaTeq;
252 (WHO) recommended that the efficacy of "new" rotavirus vaccines should be demonstrated in diverse geo
254 es in Asia and Africa have demonstrated that rotavirus vaccines significantly reduce severe diarrhea
256 Monitoring Services of America databases for rotavirus vaccine stories from the first US clinical tri
257 stlicensure surveillance of a newly licensed rotavirus vaccine suggested an increased risk of intussu
258 effectiveness of a rotavirus vaccine (rhesus rotavirus vaccine-tetravalent (RRV-TV)) to prevent rotav
261 of an increased risk of intussusception with rotavirus vaccine, the 14 Latin American countries curre
262 financial challenges face the global use of rotavirus vaccines, these vaccines-and new candidates in
265 e modeled the cost-effectiveness of adding a rotavirus vaccine to the Peruvian immunization program u
266 Among 181 Pakistani infants in a G1P[8] rotavirus vaccine trial who were seronegative at baselin
270 ry 2001 through March 2006, a period without rotavirus vaccine use, by a search of discharge, billing
271 ctiveness estimates and absolute benefits of rotavirus vaccines vary through the years following vacc
273 he administration of two doses of monovalent rotavirus vaccine was estimated to be 5.3 per 100,000 in
278 f children born after 28 February 2006 (when rotavirus vaccine was licensed in the United States) and
281 tavirus disease before the introduction of a rotavirus vaccine, we aimed to update the estimated numb
282 udy of more than 200,000 doses of monovalent rotavirus vaccine, we observed a significant increase in
289 Four strains were related to pentavalent rotavirus vaccine, whereas one was related to monovalent
292 sception among children receiving monovalent rotavirus vaccine with historical background rates.
293 ne among households whose child had received rotavirus vaccine with those whose child did not receive
294 population for scenarios with and without a rotavirus vaccine with use of data on health outcomes of
296 ata for the protective efficacy of the 2 new rotavirus vaccines, with emphasis on issues particularly
297 f 9.5 million infants in these 14 countries, rotavirus vaccine would annually prevent 144 746 (90% co
298 dule versus an unrestricted schedule whereby rotavirus vaccine would be administered with DTP vaccine
300 overage and timing, a 90% efficacious 3-dose rotavirus vaccine would prevent 70% of deaths due to rot
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