Your search keyword '"Jorba, Jaume"' showing total 6 results

1. Vaccine-derived poliovirus serotype 2 outbreaks and response in the Democratic Republic of the Congo, 2017–2021.

Author

Alleman, Mary M., Jorba, Jaume, Riziki, Yogolelo, Henderson, Elizabeth, Mwehu, Anicet, Seakamela, Lerato, Howard, Wayne, Kadiobo Mbule, Albert, Nsamba, Renee Ntumbannji, Djawe, Kpandja, Yapi, Moïse Désiré, Mengouo, Marcellin Nimpa, Gumede, Nicksy, Ndoutabe, Modjirom, Kfutwah, Anfumbom K.W., Senouci, Kamel, and Burns, Cara C.

Subjects

*POLIOVIRUS, *ACUTE flaccid paralysis, *ORAL vaccines, *HERD immunity, *VACCINATION coverage, *POLIOMYELITIS vaccines

Abstract

Vaccine-derived polioviruses (VDPVs) can emerge from Sabin strain poliovirus serotypes 1, 2, and 3 contained in oral poliovirus vaccine (OPV) after prolonged person-to-person transmission where population vaccination immunity against polioviruses is suboptimal. VDPVs can cause paralysis indistinguishable from wild polioviruses and outbreaks when community circulation ensues. VDPV serotype 2 outbreaks (cVDPV2) have been documented in The Democratic Republic of the Congo (DRC) since 2005. The nine cVDPV2 outbreaks detected during 2005–2012 were geographically-limited and resulted in 73 paralysis cases. No outbreaks were detected during 2013–2016. During January 1, 2017–December 31, 2021, 19 cVDPV2 outbreaks were detected in DRC. Seventeen of the 19 (including two first detected in Angola) resulted in 235 paralysis cases notified in 84 health zones in 18 of DRC's 26 provinces; no notified paralysis cases were associated with the remaining two outbreaks. The DRC-KAS-3 cVDPV2 outbreak that circulated during 2019–2021, and resulted in 101 paralysis cases in 10 provinces, was the largest recorded in DRC during the reporting period in terms of numbers of paralysis cases and geographic expanse. The 15 outbreaks occurring during 2017–early 2021 were successfully controlled with numerous supplemental immunization activities (SIAs) using monovalent OPV Sabin-strain serotype 2 (mOPV2); however, suboptimal mOPV2 vaccination coverage appears to have seeded the cVDPV2 emergences detected during semester 2, 2018 through 2021. Use of the novel OPV serotype 2 (nOPV2), designed to have greater genetic stability than mOPV2, should help DRC's efforts in controlling the more recent cVDPV2 outbreaks with a much lower risk of further seeding VDPV2 emergence. Improving nOPV2 SIA coverage should decrease the number of SIAs needed to interrupt transmission. DRC needs the support of polio eradication and Essential Immunization (EI) partners to accelerate the country's ongoing initiatives for EI strengthening, introduction of a second dose of inactivated poliovirus vaccine (IPV) to increase protection against paralysis, and improving nOPV2 SIA coverage. [ABSTRACT FROM AUTHOR]

Published

2023

2. Does the introduction of new resuscitation guidelines increase survival after cardiac arrest?

Author

Dotras, Jaume Fontanals, Mendaña, Marta Magaldi, Caravaca, Montserrat Fontanals, Felip, Montserrat Tió, and Jorba, Jaume Fontanals

Published

2013

3. Genetic and epidemiological description of an outbreak of circulating vaccine-derived polio-virus type 2 (cVDPV2) in Angola, 2019–2020.

Author

Morais, Alda, Morais, Joana, Felix, Miguel, Neto, Zoraima, Madaleno, Valódia, Umar, Abubakar Sadiq, Panda, Nirakar, Lemma, Fekadu, Chivale, José Alexandre Lifande, Cavalcante, Danielle Graça, Davlantes, Elizabeth, Ghiselli, Margherita, Espinosa, Catherine, Whiteman, Ari, Iber, Jane, Henderson, Elizabeth, Bullard, Kelley, Jorba, Jaume, Burns, Cara C., and Diop, Ousmane

Subjects

*COVID-19, *POLIO, *VIRAL transmission, *COVID-19 pandemic, *SEWAGE, *POLIOVIRUS, *IMMUNIZATION

Abstract

After six years without any detection of poliomyelitis cases, Angola reported a case of circulating vaccine-derived poliovirus type 2 (cVDPV2) with paralysis onset date of 27 March 2019. Ultimately, 141 cVDPV2 polio cases were reported in all 18 provinces in 2019–2020, with particularly large hotspots in the south-central provinces of Luanda, Cuanza Sul, and Huambo. Most cases were reported from August to December 2019, with a peak of 15 cases in October 2019. These cases were classified into five distinct genetic emergences (emergence groups) and have ties with cases identified in 2017–2018 in the Democratic Republic of Congo. From June 2019 to July 2020, the Angola Ministry of Health and partners conducted 30 supplementary immunization activity (SIA) rounds as part of 10 campaign groups, using monovalent OPV type 2 (mOPV2). There were Sabin 2 vaccine strain detections in the environmental (sewage) samples taken after mOPV2 SIAs in each province. Following the initial response, additional cVDPV2 polio cases occurred in other provinces. However, the national surveillance system did not detect any new cVDPV2 polio cases after 9 February 2020. While reporting subpar indicator performance in epidemiological surveillance, the laboratory and environmental data as of May 2021 strongly suggest that Angola successfully interrupted transmission of cVDPV2 early in 2020. Additionally, the COVID-19 pandemic did not allow a formal Outbreak Response Assessment (OBRA). Improving the sensitivity of the surveillance system and the completeness of AFP case investigations will be vital to promptly detect and interrupt viral transmission if a new case or sewage isolate are identified in Angola or central Africa. [ABSTRACT FROM AUTHOR]

Published

2023

4. Assessing country compliance with circulating vaccine-derived poliovirus type 2 outbreak response standard operating procedures: April 2016 to December 2020.

Author

Darwar, Roopa, Biya, Oladayo, Greene, Sharon A., Jorba, Jaume, Al Safadi, Mohammad, Franka, Richard, Wiesen, Eric, Durry, Elias, and Pallansch, Mark A.

Subjects

*POLIOVIRUS, *STANDARD operating procedure, *VACCINE approval, *ORAL vaccines, *SECONDARY analysis, *POLIO

Abstract

• Successful outbreak response requires timely supplemental immunization activities. • There are numerous sources of delayed response beyond the vaccine approval process. • Several countries met multiple target indicators for successful outbreak response. Trivalent oral poliovirus vaccine (tOPV) was globally replaced with bivalent oral poliovirus vaccine (bOPV) in April 2016 ("the switch"). Many outbreaks of paralytic poliomyelitis associated with type 2 circulating vaccine-derived poliovirus (cVDPV2) have been reported since this time. The Global Polio Eradication Initiative (GPEI) developed standard operating procedures (SOPs) to guide countries experiencing cVDPV2 outbreaks to implement timely and effective outbreak response (OBR). To assess the possible role of compliance with SOPs in successfully stopping cVDPV2 outbreaks, we analyzed data on critical timelines in the OBR process. Data were collected on all cVDPV2 outbreaks detected for the period April 1, 2016 and December 31, 2020 and all outbreak responses to those outbreaks between April 1, 2016 and December 31, 2021. We conducted secondary data analysis using the GPEI Polio Information System database, records from the U.S. Centers for Disease Control and Prevention Polio Laboratory, and meeting minutes of the monovalent OPV2 (mOPV2) Advisory Group. Date of notification of circulating virus was defined as Day 0 for this analysis. Extracted process variables were compared with indicators in the GPEI SOP version 3.1. One hundred and eleven cVDPV2 outbreaks resulting from 67 distinct cVDPV2 emergences were reported during April 1, 2016-December 31, 2020, affecting 34 countries across four World Health Organization Regions. Out of 65 OBRs with the first large-scale campaign (R1) conducted after Day 0, only 12 (18.5%) R1s were conducted by the target of 28 days after Day 0. Of the 89 OBRs with the second large-scale campaign (R2) conducted after Day 0, 30 (33.7%) R2s were conducted by the target of 56 days after Day 0. Twenty-three (31.9%) of the 72 outbreaks with isolates dated after Day 0 were stopped within the 120-day target. Since "the switch", delays in OBR implementation were evident in many countries, which may be related to the persistence of cVDPV2 outbreaks >120 days. To achieve timely and effective response, countries should follow GPEI OBR guidelines. [ABSTRACT FROM AUTHOR]

Published

2023

5. Neutralization capacity of highly divergent type 2 vaccine-derived polioviruses from immunodeficient patients.

Author

McDonald, Sharla L., Weldon, William C., Wei, Ling, Chen, Qi, Shaw, Jing, Zhao, Kun, Jorba, Jaume, Kew, Olen M., Pallansch, Mark A., Burns, Cara C., and Steven Oberste, M.

Subjects

*POLIO, *COMBINED vaccines, *ORAL vaccines, *POLIOMYELITIS vaccines, *VIRAL vaccines, DEVELOPING countries

Abstract

The use of the oral poliovirus vaccine (OPV) in developing countries has reduced the incidence of poliomyelitis by >99% since 1988 and is the primary tool for global polio eradication. Spontaneous reversions of the vaccine virus to a neurovirulent form can impede this effort. In persons with primary B-cell immunodeficiencies, exposure to OPV can result in chronic infection, mutation, and excretion of immunodeficiency-associated vaccine-derived polioviruses, (iVDPVs). These iVDPVs may have the potential for transmission in a susceptible population and cause paralysis. The extent to which sera from OPV recipients are able to neutralize iVDPVs with varying degrees of antigenic site substitutions is investigated here. We tested sera from a population immunized with a combination vaccine schedule (both OPV and inactivated polio vaccine) against a panel of iVDPVs and found that increases in amino acid substitution in the P1 capsid protein resulted in a decrease in the neutralizing capacity of the sera. This study underscores the importance of maintaining high vaccine coverage in areas of OPV use as well as active surveillance of those known to be immunocompromised. [ABSTRACT FROM AUTHOR]

Published

2020

6. Isolation of recombinant type 2 vaccine-derived poliovirus (VDPV) from a Nigerian child

Author

Adu, Festus, Iber, Jane, Bukbuk, David, Gumede, Nicksy, Yang, Su-Ju, Jorba, Jaume, Campagnoli, Ray, Sule, Waidi Folorunso, Yang, Chen-Fu, Burns, Cara, Pallansch, Mark, Harry, Tekena, and Kew, Olen

Subjects

*IMMUNIZATION of children, *PREVENTIVE medicine, *ENTEROVIRUSES, *PARALYSIS

Abstract

Abstract: A type 2 vaccine-derived poliovirus (VDPV), differing from Sabin 2 at 2.5% (22/903) of VP1 nucleotide (nt) positions, was isolated from an incompletely immunized 21-month-old Nigerian child who developed acute flaccid paralysis in 2002. Sequences upstream of nt position 620 (within the 5′-untranslated region [5′-UTR]) and downstream of nt position 5840 (in the 3Cpro region) were derived from species C enteroviruses unrelated to the oral poliovirus vaccine (OPV) strains. The two substitutions associated with the attenuated phenotype had either recombined out (A481 →G in the 5′-UTR) or reverted (Ile143 →Thr in VP1). The VDPV isolate had lost the temperature sensitive phenotype of Sabin 2 and it was antigenically distinct from the parental OPV strain, having amino acid substitutions in or near neutralizing antigenic sites 1 and 3. The date of the initiating OPV dose, calculated from the number of synonymous substitutions in the capsid region, was estimated to be ∼16 to 18 months before onset of paralysis, a finding inconsistent with the most recent mass OPV campaign (conducted 12 days before onset of paralysis) as being the source of infection. Although no related type 2 VDPVs were detected in Nigeria or elsewhere, the VDPV was found in an area where conditions favor VDPV emergence and spread. [Copyright &y& Elsevier]

Published

2007