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Research Project
Molecular epidemiology, drug resistance and pathogenesis of HIV and TB in Angola: the Angolan PErinatal HIV Cohort (APEHC)
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Authors
Publications
Determinants of highly active antiretroviral therapy duration in HIV-1-infected children and adolescents in Madrid, Spain, from 1996 to 2012
Publication . Palladino, Claudia; Briz, Verónica; Bellón, José María; Climent, Francisco J.; De Ory, Santiago J.; Mellado, María José; Navarro, María Luisa; Ramos, José T.; Taveira, Nuno; De José, María Isabel; Munõz-Fernandes, María Ángeles; CoRISpeS-Madrid Cohort Working Group
"Objectives: To investigate the duration of sequential HAART regimens and predictors of first-line regimen discontinuation
among HIV-1 vertically infected children and adolescents.
Design: Multicentre survey of antiretroviral-naı¨ve patients enrolled in the HIV-Paediatric Cohor,t CoRISpeS-Madrid Cohort,
Spain.
Methods: Patients with a follow-up of $1 month spent on HAART, with available baseline CD4 count and HIV-viral load (VL)
were included. Time spent on sequential HAART regimens was estimated and multivariable regression was used to identify
predictors of time to first-line regimen discontinuation.
Results: 104 patients were followed for a median 8 years after starting HAART among 1996–2012; baseline %CD4 was 21.5
(12.3–34.0)and viral load was 5.1 (4.6–5.6) log10 copies/mL. Patients received a mean of 1.9 regimens. Median time on firstline
HAART (n = 104) was 64.5 months; second HAART (n = 56) 69.8 months; and third HAART (n = 21) 66.5 months. Eleven
(11%) patients were lost to follow-up while on first-line HAART and 54% discontinued (cumulative incidence of 16% and
38% by 1 and 3-year, respectively). The main predictor of first-line regimen discontinuation was suboptimal adherence to
antiretrovirals (AHR: 2.60; 95% CI: 1.44–4.70).
Conclusions: Adherence to therapy was the main determinant of the duration of the first-line HAART regimen in children. It
is important to identify patients at high risk for non-adherence, such as very young children and adolescents, in provide
special care and support to those patients."
HIV-1 Diversity, Transmission Dynamics and Primary Drug Resistance in Angola
Publication . Bártolo, Inês; Zakovic, Susana; Martin, Francisco; Palladino, Claudia; Carvalho, Patrícia; Camacho, Ricardo; Thamm, Sven; Clemente, Sofia; Taveira, Nuno
"Objectives: To assess HIV-1 diversity, transmission dynamics and prevalence of
transmitted drug resistance (TDR) in Angola, five years after ART scale-up.
Methods: Population sequencing of the pol gene was performed on 139 plasma
samples collected in 2009 from drug-naive HIV-1 infected individuals living in
Luanda. HIV-1 subtypes were determined using phylogenetic analysis. Drug
resistance mutations were identified using the Calibrated Population Resistance
Tool (CPR). Transmission networks were determined using phylogenetic analysis
of all Angolan sequences present in the databases. Evolutionary trends were
determined by comparison with a similar survey performed in 2001.
Results: 47.1% of the viruses were pure subtypes (all except B), 47.1% were
recombinants and 5.8% were untypable. The prevalence of subtype A decreased
significantly from 2001 to 2009 (40.0% to 10.8%, P50.0019) while the prevalence
of unique recombinant forms (URFs) increased.2-fold (40.0% to 83.1%,
P,0.0001). The most frequent URFs comprised untypable sequences with
subtypes H (U/H, n57, 10.8%), A (U/A, n56, 9.2%) and G (G/U, n54, 6.2%). Newly
identified U/H recombinants formed a highly supported monophyletic cluster
suggesting a local and common origin. TDR mutation K103N was found in one
(0.7%) patient (1.6% in 2001). Out of the 364 sequences sampled for transmission
network analysis, 130 (35.7%) were part of a transmission network. Forty eight
transmission clusters were identified; the majority (56.3%) comprised sequences
sampled in 2008–2010 in Luanda which is consistent with a locally fuelled
epidemic. Very low genetic distance was found in 27 transmission pairs sampled in
the same year, suggesting recent transmission events.
Conclusions: Transmission of drug resistant strains was still negligible in Luanda
in 2009, five years after the scale-up of ART. The dominance of small and recent
transmission clusters and the emergence of new URFs are consistent with a rising
HIV-1 epidemics mainly driven by heterosexual transmission."
Donor-Recipient identification in para- and poly-phyletic trees under alternative HIV-1 transmission hypotheses using approximate Bayesian computation
Publication . Romero-Severson, Ethan O.; Bulla, Ingo; Hengartner, Nick; Bártolo, Inês; Abecasis, Ana; Azevedo-Pereira, José M.; Taveira, Nuno; Leitner, Thomas
Diversity of the founding population of Human Immunodeficiency Virus Type 1 (HIV-1) transmissions raises many important biological, clinical, and epidemiological issues. In up to 40% of sexual infections, there is clear evidence for multiple founding variants, which can influence the efficacy of putative prevention methods, and the reconstruction of epidemiologic histories. To infer who-infected-whom, and to compute the probability of alternative transmission scenarios while explicitly taking phylogenetic uncertainty into account, we created an approximate Bayesian computation (ABC) method based on a set of statistics measuring phylogenetic topology, branch lengths, and genetic diversity. We applied our method to a suspected heterosexual transmission case involving three individuals, showing a complex monophyletic-paraphyletic-polyphyletic phylogenetic topology. We detected that seven phylogenetic lineages had been transmitted between two of the individuals based on the available samples, implying that many more unsampled lineages had also been transmitted. Testing whether the lineages had been transmitted at one time or over some length of time suggested that an ongoing superinfection process over several years was most likely. While one individual was found unlinked to the other two, surprisingly, when evaluating two competing epidemiological priors, the donor of the two that did infect each other was not identified by the host root-label, and was also not the primary suspect in that transmission. This highlights that it is important to take epidemiological information into account when analyzing support for one transmission hypothesis over another, as results may be nonintuitive and sensitive to details about sampling dates relative to possible infection dates. Our study provides a formal inference framework to include information on infection and sampling times, and to investigate ancestral node-label states, transmission direction, transmitted genetic diversity, and frequency of transmission.
Genetic diversity, transmission dynamics and drug resistance of Mycobacterium tuberculosis in Angola
Publication . Perdigão, João; Clemente, Sofia; Ramos, Jorge; Masakidi, Pedro; Machado, Diana; Silva, Carla; Couto, Isabel; Viveiros, Miguel; Taveira, Nuno; Portugal, Isabel
"Tuberculosis (TB) poses a serious public health problem in Angola. No surveillance data on drug resistance is available and nothing is known regarding the genetic diversity and population structure of circulating Mycobacterium tuberculosis strains. Here, we have genotyped and evaluated drug susceptibility of 89 Mycobacterium tuberculosis clinical isolates from Luanda. Thirty-three different spoligotype profiles corresponding to 24 different Shared International Types (SIT) and 9 orphan profiles were detected. SIT 20 (LAM1) was the most prevalent (n = 16, 18.2%) followed by SIT 42 (LAM9; n = 15, 17.1%). Overall, the M. tuberculosis population structure in this sample was dominated by LAM (64.8%) and T (33.0%) strains. Twenty-four-loci MIRU-VNTR analysis revealed that a total of 13 isolates were grouped in 5 distinct clusters. Drug susceptibility data showed that 22 (24.7%) of the 89 clinical isolates were resistant to one or more antibacillary drugs of which 4 (4.5%) were multidrug resistant. In conclusion, this study demonstrates a high predominance of LAM strains circulating in the Luanda setting and the presence of recent transmission events. The rate and the emergence dynamics of drug resistant TB found in this sample are significant and highlight the need of further studies specifically focused on MDR-TB transmission."
Development of synthetic light-chain antibodies as novel and potent HIV fusion inhibitors
Publication . Cunha-Santos, Catarina; Figueira, Tiago N.; Borrego, Pedro; Oliveira, Soraia S.; Rocha, Cheila; Couto, Andreia; Cantante, Cátia; Santos- Costa, Quirina; Azevedo-Pereira, José M.; Fontes, Carlos M. G. A.; Taveira, Nuno; Aires-Da-Silva, Frederico; Castanho, Miguel A. R. B.; Veiga, Ana Salomé; Gonçalves, João
"Objective: To develop a novel and potent fusion inhibitor of HIV infection based on a rational strategy for synthetic antibody library construction.
Design: The reduced molecular weight of single-domain antibodies (sdAbs) allows targeting of cryptic epitopes, the most conserved and critical ones in the context of HIV entry. Heavy-chain sdAbs from camelids are particularly suited for this type of epitope recognition because of the presence of long and flexible antigen-binding regions [complementary-determining regions (CDRs)]."
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Funders
Funding agency
Fundação para a Ciência e a Tecnologia
Funding programme
3599-PPCDT
Funding Award Number
PTDC/SAU-EPI/122400/2010