Showing total 22 results

1. Development and evaluation of serological screening based on one dried plasma spot for HIV, syphilis, and HCV.

Author

Ma, Jie-qiong, Ren, Ya-nan, Wen, Shi-yuan, Dong, Ao-bo, Xing, Wen-ge, and Jiang, Yan

Subjects

HIV, TREPONEMA pallidum, MEDICAL screening, SYPHILIS, HEPATITIS C virus, BLOOD volume, DIAGNOSIS of HIV infections

Abstract

Background: In the effort to prevent and control HIV/AIDS, China has established a national sentinel surveillance system. However, some sentinel sites face limitations in environmental resources and accessibility, prompting the exploration of alternative sample strategies. Dried plasma spots (DPS) samples are viewed as promising alternatives to traditional plasma samples due to their advantages, including sample stability, easy storage, and convenient transport. This study aims to develop a method for screening HIV, Treponema pallidum (TP), and Hepatitis C Virus (HCV) using DPS samples and assess their performance. Methods: Based on existing commercial assay kits, a detection method was established through the optimization of experimental parameters, including the amount of plasma on filter paper, the volume of elution solution applied to dried plasma spots, the size of dried plasma spots, elution solution volume, elution solution components, elution temperature, and elution time. A series of laboratory evaluation panels were constructed for laboratory assessments, including the laboratory basic panel, laboratory interference panel, and laboratory precision panel. Additionally, clinical samples were used for evaluation. Results: Optimal conditions for DPS sample extraction were: plasma volume, 100 µL; DPS size, whole spot; eluent volume, 500 µL; eluent, PBS with 1‰ Tween20; elution time, 2 h; elution temperature, room temperature. A total of 619 paired plasma/DPS samples were tested by both methods. The DPS-based ELISA method exhibited 100% sensitivity/specificity for HIV, 98.6%/100% for TP, and 99.6%/100% for HCV. Kappa values between the plasma samples and DPS samples were 100% for HIV, 99% for TP, and 100% for HCV. The DPS-based ELISA method failed to detect 1 HCV mono-infected sample and TP in 1 HIV/HCV/TP co-infected sample. For the HIV/HCV/TP co-infected sample, the S/CO in the plasma sample was 2.143 and in the DPS sample was 0.5. For HCV, the S/CO (sample OD/cut-off) was 3.049 in the plasma sample and 0.878 in the DPS sample. Conclusions: A single DPS, following one-time standardized processing, can be used to detect HIV, HCV, and TP. Researching and establishing laboratory testing methods better suited for China's sentinel surveillance have significant practical applications in improving HIV testing in resource-constrained environments. [ABSTRACT FROM AUTHOR]

Published

2023

2. Impact of subtype C-specific amino acid variants on HIV-1 Tat-TAR interaction: insights from molecular modelling and dynamics.

Author

Gotora, Piwai T., Brown, Keaghan, Martin, Darius R., van der Sluis, Rencia, Cloete, Ruben, and Williams, Monray E.

Subjects

AMINO acids, MOLECULAR dynamics, TAT protein, HIV, MOLECULAR docking

Abstract

Background: HIV-1 produces Tat, a crucial protein for transcription, viral replication, and CNS neurotoxicity. Tat interacts with TAR, enhancing HIV reverse transcription. Subtype C Tat variants (C31S, R57S, Q63E) are associated with reduced transactivation and neurovirulence compared to subtype B. However, their precise impact on Tat-TAR binding is unclear. This study investigates how these substitutions affect Tat-TAR interaction. Methods: We utilized molecular modelling techniques, including MODELLER, to produce precise three-dimensional structures of HIV-1 Tat protein variants. We utilized Tat subtype B as the reference or wild type, and generated Tat variants to mirror those amino acid variants found in Tat subtype C. Subtype C-specific amino acid substitutions were selected based on their role in the neuropathogenesis of HIV-1. Subsequently, we conducted molecular docking of each Tat protein variant to TAR using HDOCK, followed by molecular dynamic simulations. Results: Molecular docking results indicated that Tat subtype B (TatWt) showed the highest affinity for the TAR element (-262.07), followed by TatC31S (-261.61), TatQ63E (-256.43), TatC31S/R57S/Q63E (-238.92), and TatR57S (-222.24). However, binding free energy analysis showed higher affinities for single variants TatQ63E (-349.2 ± 10.4 kcal/mol) and TatR57S (-290.0 ± 9.6 kcal/mol) compared to TatWt (-247.9 ± 27.7 kcal/mol), while TatC31S and TatC31S/R57SQ/63E showed lower values. Interactions over the protein trajectory were also higher for TatQ63E and TatR57S compared to TatWt, TatC31S, and TatC31S/R57SQ/63E, suggesting that modifying amino acids within the Arginine/Glutamine-rich region notably affects TAR interaction. Single amino acid mutations TatR57S and TatQ63E had a significant impact, while TatC31S had minimal effect. Introducing single amino acid variants from TatWt to a more representative Tat subtype C (TatC31S/R57SQ/63E) resulted in lower predicted binding affinity, consistent with previous findings. Conclusions: These identified amino acid positions likely contribute significantly to Tat-TAR interaction and the differential pathogenesis and neuropathogenesis observed between subtype B and subtype C. Additional experimental investigations should prioritize exploring the influence of these amino acid signatures on TAR binding to gain a comprehensive understanding of their impact on viral transactivation, potentially identifying them as therapeutic targets. [ABSTRACT FROM AUTHOR]

Published

2024

3. Development of a highly sensitive and specific intact proviral DNA assay for HIV-1 subtype B and C.

Author

Buchholtz, N. V. E. J., Nühn, M. M., de Jong, T. C. M., Stienstra, T. A. T., Reddy, K., Ndung'u, T., Ndhlovu, Z. M., Fisher, K., Palmer, S., Wensing, A. M. J., Symons, J., and Nijhuis, M.

Subjects

HIV, DNA, DNA primers, ANTIRETROVIRAL agents, TENOFOVIR, DETECTION limit, SENSITIVITY & specificity (Statistics)

Abstract

Introduction: HIV reservoir quantification is essential for evaluation of HIV curative strategies and may provide valuable insights about reservoir dynamics during antiretroviral therapy. The Intact Proviral DNA Assay (IPDA) provides the unique opportunity to quantify the intact and defective reservoir. The current IPDA is optimized for HIV-1 subtype B, the dominant subtype in resource-rich settings. However, subtype C is dominant in Sub-Saharan Africa, jointly accounting for around 60% of the pandemic. We developed an assay capable of quantifying intact and defective proviral HIV-1 DNA of subtype B and C. Methods: Primer and probe sequences were strategically positioned at conserved regions in psi and env and adapted to subtype B&C. In silico analysis of 752 subtype B and 697 subtype C near-full length genome sequences (nFGS) was performed to predict the specificity and sensitivity. Gblocks were used to determine the limit of blank (LoB), limit of detection (LoD), and different annealing temperatures were tested to address impact of sequence variability. Results: The in silico analysis showed that the HIV-1 B&C IPDA correctly identified 100% of the intact subtype B, and 86% of the subtype C sequences. In contrast, the original IPDA identified 86% and 12% of these subtype B and C sequences as intact. Furthermore, the HIV-1 B&C IPDA correctly identified hypermutated (87% and 88%) and other defective sequences (73% and 66%) for subtype B and C with comparable specificity as the original IPDA for subtype B (59% and 63%). Subtype B cis-acting sequences were more frequently identified as intact by the HIV-1 B&C IPDA compared to the original IPDA (39% and 2%). The LoB for intact proviral DNA copies was 0, and the LoD for intact proviral DNA copies was 6 (> 95% certainty) at 60 °C. Quantification of 2–6 copies can be performed with > 80% certainty. Lowering the annealing temperature to 55 °C slightly lowered the specificity but prevented exclusion of samples with single mutations in the primer/probe region. Conclusions: We developed a robust and sensitive assay for the quantification of intact and defective HIV-1 subtype B and C proviral DNA, making this a suitable tool to monitor the impact of (large-scale) curative interventions. [ABSTRACT FROM AUTHOR]

Published

2024

4. A bibliometric analysis of m6A methylation in viral infection from 2000 to 2022.

Author

Tao, Xing, Wang, Gang, Wei, Wudi, Su, Jinming, Chen, Xiu, Shi, Minjuan, Liao, Yinlu, Qin, Tongxue, Wu, Yuting, Lu, Beibei, Liang, Hao, Ye, Li, and Jiang, Junjun

Subjects

BIBLIOMETRICS, VIRUS diseases, TYPE I interferons, METHYLATION, HIV

Abstract

Background: N6-methyladenosine (m6A) methylation has become an active research area in viral infection, while little bibliometric analysis has been performed. In this study, we aim to visualize hotspots and trends using bibliometric analysis to provide a comprehensive and objective overview of the current research dynamics in this field. Methods: The data related to m6A methylation in viral infection were obtained through the Web of Science Core Collection form 2000 to 2022. To reduce bias, the literature search was conducted on December 1, 2022. Bibliometric and visual analyzes were performed using CiteSpace and Bibliometrix package. After screening, 319 qualified records were retrieved. Results: These publications mainly came from 28 countries led by China and the United States (the US), with the US ranking highest in terms of total link strength.The most common keywords were m6A, COVID-19, epitranscriptomics, METTL3, hepatitis B virus, innate immunity and human immunodeficiency virus 1. The thematic map showed that METTL3, plant viruses, cancer progression and type I interferon (IFN-I) reflected a good development trend and might become a research hotspot in the future, while post-transcriptional modification, as an emerging or declining theme, might not develop well. Conclusions: In conclusion, m6A methylation in viral infection is an increasingly important topic in articles. METTL3, plant viruses, cancer progression and IFN-I may still be research hotspots and trends in the future. [ABSTRACT FROM AUTHOR]

Published

2024

5. Learning from cerebrospinal fluid drug-resistant HIV escape-associated encephalitis: a case report.

Author

Kang, Jing, Wang, Ziqiu, Zhou, Ying, Wang, Wen, and Wen, Ying

Subjects

CEREBROSPINAL fluid examination, CEREBROSPINAL fluid, HIV, HIV infections, ENCEPHALITIS, MAGNETIC resonance imaging

Abstract

Background: In the era of antiretroviral therapy (ART), central nervous system (CNS) complications in patients with human immunodeficiency virus (HIV) infection are sometimes associated with cerebrospinal fluid (CSF) viral escape. Here, we reported a case of persistent CNS viral escape with recurrent symptomatic encephalitis, which had ultimate stabilization achieved by a combination of ART adjustment and corticosteroids. Case presentation: A 27-year-old man with HIV infection complained of recurrent headaches during the last year. His magnetic resonance imaging (MRI) presented diffused bilateral white matter lesions, and laboratory tests confirmed elevated CSF protein level, lymphocytic pleocytosis, and detectable CSF HIV RNA (774 copies/mL). Plasma HIV RNA was well suppressed with tenofovir, lamivudine, and lopinavir/ritonavir. Prednisone 60 mg once daily was initiated to reduce intracranial inflammation, followed by a good clinical response, with CSF HIV RNA still detectable (31.1 copies/mL). During the gradual tapering of prednisone, his headache relapsed, and booming viral loads were detected in both CSF (4580 copies/mL) and plasma (340 copies/mL) with consistent drug-resistant mutations. Thereupon, prednisone was resumed and the ART regimen was switched to zidovudine, lamivudine, and dolutegravir according to drug resistance tests. Persistent clinical recovery of symptoms, neuroimaging, and laboratory abnormalities were observed in the follow-up visits. Conclusion: CSF and plasma HIV RNA and further drug resistance tests should be monitored in HIV-infected patients with neurologic symptoms, as opportunistic infections or tumors can be ruled out. ART optimization using a sensitive regimen may be crucial for addressing CSF viral escape and the related encephalitis. [ABSTRACT FROM AUTHOR]

Published

2023

6. HIV-1 drug resistance and genetic transmission network among newly diagnosed people living with HIV/AIDS in Ningbo, China between 2018 and 2021.

Author

Hong, Hang, Tang, Chunlan, Liu, Yuhui, Jiang, Haibo, Fang, Ting, and Xu, Guozhang

Subjects

DRUG resistance, HIV-positive persons, AIDS, HIV, HIV infection transmission, MOLECULAR epidemiology

Abstract

Background: As the HIV epidemic continues to grow, transmitted drug resistance(TDR) and determining relationship of HIV transmission are major barriers to reduce the risk of HIV transmissions.This study aimed to examine the molecular epidemiology and TDR and evaluated the transmission pattern among newly diagnosed people living with HIV/AIDS(PLWHA) in Ningbo city, which could contribute to the development of targeted precision interventions. Methods: Consecutive cross-sectional surveys were conducted in Ningbo City between January 2018 and December 2021. The HIV-1 pol gene region was amplified and sequenced for drug resistance and genetic transmission network analysis. TDR was determined using the Stanford University HIV Drug Resistance Database. Genetic transmission network was visualized using Cytoscape with the genetic distance threshold of 0.013. Results: A total of 1006 sequences were sequenced successfully, of which 61 (6.1%) showed evidence of TDR. The most common mutations were K103N (2.3%), E138A/G/Q (1.7%) and V179D/E (1.2%). 12 HIV-1 genotypes were identified, with CRF07_BC being the major genotype (43.3%, 332/767), followed by CRF01_AE (33.7%, 339/1006). 444 (44.1%) pol sequences formed 856 links within 120 transmission clusters in the network. An increasing trend in clustering rate between 2018 and 2021(χ2 = 9.546, P = 0.023) was observed. The odds of older age (≥ 60 years:OR = 2.038, 95%CI = 1.072 ~ 3.872, compared to < 25 years), HIV-1 genotypes (CRF07_BC: OR = 2.147, 95%CI = 1.582 ~ 2.914; CRF55_01B:OR = 2.217, 95%CI = 1.201 ~ 4.091, compared to CRF01_AE) were significantly related to clustering. Compared with CRF01_AE, CRF07_BC were prone to form larger clusters. The largest cluster with CRF07_BC was increased from 15 cases in 2018 to 83 cases in 2021. Conclusions: This study revealed distribution of HIV-1 genotypes, and genetic transmission network were diverse and complex in Ningbo city. The prevalence of TDR was moderate, and NVP and EFV were high-level NNRTI resistance. Individuals aged ≥ 60 years old were more easily detected in the networks and CRF07_BC were prone to form rapid growth and larger clusters. These date suggested that surveillance and comprehensive intervention should be designed for key rapid growth clusters to reduce the potential risk factors of HIV-1 transmission. [ABSTRACT FROM AUTHOR]

Published

2023

7. Relation between interleukin-6 concentrations and oxidative status of HIV infected patients with /or at risk of Kaposi disease in Yaounde.

Author

Voufo, Roger Ahouga, Kouotou, Armand Emmanuel, Tatah, Nchinda Jones, TeTo, Georges, Gueguim, Cédric, Ngondé, Chantal Marie Essome, Njiguet Tepa, Armand Gabin, Gabin, Arnaud, Amazia, Falmata, Yembeau, Natacha Lena, Kouanfack, Charles, and Anatole, Pieme Constant

Subjects

XERODERMA pigmentosum, HIV, INTERLEUKIN-6, OXIDANT status, HIV status, OXIDATIVE stress

Abstract

Objective: To investigate the relation between interleukin-6 concentration and oxidative status of HIV infected patients with or at risk of Kaposi's disease in Yaoundé. Methods: We conducted a two-months cross-sectional study on 87 consenting HIV infected patients followed at the Day Hospital of the Yaoundé Central Hospital. Serum/plasma obtained after centrifugation of blood collected in dry/EDTA tubes was used for the determination of Human Herpes Virus-8 antigen (HHV-8) and Interleukin-6 (IL-6) by the ELISA technique, and that of oxidative stress markers: Malondialdehyde (MDA) reduced Glutathione (GSH) and total antioxidant capacity by spectrophotometry. Results: Subjects belonging to the [40–50[year-old age group were mainly represented in our study population with 43.7%. The average age was 44.6 ± 10.4 years with extremes ranging from 26 to 72 years. The sex ratio was 0.24. Our population was mainly represented by people infected with HIV type I (90.8%) and 3.4% had developed clinical signs of Kaposi's disease. The prevalence of the HHV-8 antigen was 57.5%. Immune and oxidative parameters did not vary with age, sex and therapeutic line. We noted a significant increase in IL-6 concentrations in patients positive to the HHV-8 antigen for IL-6 concentrations < 37 (P = 0.005; CI= [0.40; 0.59]. MDA and GSH concentrations increased significantly with the HHV-8 infection (P < 0.0001; CI= [0.40; 0.59] and P < 0.0001; CI= [13.30;21.45], respectively). Total antioxidant capacity (FRAP) decreased significantly with HHV-8 infection (P = 0.004; CI= [-69.18; -13.78]). We noted a significant increase in MDA concentrations in patients taking their ARVs irregularly, (P < 0.0001). Conclusion: Our study showed a weak positive correlation between IL-6 and MDA, a strong negative correlation between FRAP and MDA and a strong positive correlation between MDA and GSH highlighting the association of these few markers of oxidative stress and Il-6 to the risk of Kaposi's disease. [ABSTRACT FROM AUTHOR]

Published

2023

8. SARSCoV-2 antibody prevalence and titers in persons living with HIV cared for at a large tertiary reference center in Mexico City

Author

Soto-Nava, Maribel, Dávila-Conn, Vanessa, Venancio-Rocha, Juan P., García-Esparza, Pedro, Tapia-Trejo, Daniela, Hernández-Juan, Ramón, Zarza-Sánchez, Eduardo, Murakami-Ogasawara, Akio, and Ávila-Ríos, Santiago

Published

2023

9. In-house ELISA protocols for capsid p24 detection of diverse HIV isolates

Author

Molina, Mariano A., Vink, Monique, Berkhout, Ben, and Herrera-Carrillo, Elena

Published

2023

10. Trends in HIV-1 pretreatment drug resistance and HIV-1 variant dynamics among antiretroviral therapy-naive Ethiopians from 2003 to 2018: a pooled sequence analysis

Author

Kiros, Mulugeta, Biset, Sirak, Gebremariam, Birhane, Yalew, Gebrehiwet Tesfay, Abegaz, Woldaregay Erku, and Geteneh, Alene

Published

2023

11. Transient plasma viral rebound after SARS-CoV-2 vaccination in an exceptional HIV-1 elite controller woman

Author

Di Girolamo, L., Ferrara, M., Trevisan, G., Longo, B. M., Allice, T., Burdino, E., Alladio, F., Fantino, S., Di Perri, G., Calcagno, A., and Bonora, S.

Published

2023

12. Epstein-Barr virus variation in people living with human immunodeficiency virus in southeastern China

Author

Wan, Zhikai, Chen, Ying, Hui, Jiangjin, Guo, Yongzheng, Peng, Xiaorong, Wang, Mengyan, Hu, Caiqin, Xie, Yirui, Su, Junwei, Huang, Ying, Xu, Xiaoke, Xu, Yan, and Zhu, Biao

Published

2023

13. Switch from a ritonavir to a cobicistat containing antiretroviral regimen and impact on tacrolimus levels in a kidney transplant recipient

Author

Erba, Andrea, Marzolini, Catia, Rentsch, Katharina, Stoeckle, Marcel, Battegay, Manuel, Mayr, Michael, and Weisser, Maja

Published

2023

14. A Δ42PD1 fusion-expressing DNA vaccine elicits enhanced adaptive immune response to HIV-1: the key role of TLR4.

Author

Cheng, Lin, Tang, Xian, He, Yun, Ju, Bin, and Wang, Hui

Subjects

DNA vaccines, TOLL-like receptors, IMMUNE response, HIV, CHIMERIC proteins

Abstract

Since its discovery in the 1990s, the DNA vaccine has been of great interest because of its ability to elicit both humoral and cellular immune responses while showing relative advantages regarding producibility, stability and storage. However, when applied to human subjects, inadequate immunogenicity remains as the greatest challenge for the practical use of DNA vaccines. In this study, we generated a DNA vaccine Δ42PD1-P24 encoding a fusion protein comprised of the HIV-1 Gag p24 antigen and the extracellular domain of murine Δ42PD1, a novel endogenous Toll-like receptor 4 (TLR4) agonist. Using a mouse model, we found that Δ42PD1-P24 DNA vaccine elicited a higher antibody response and an increased number of IFN-γ-producing CD4 and CD8 T cells. Moreover, mice with Δ42PD1-P24 DNA vaccination were protected from a subcutaneous challenge with murine mesothelioma cells expressing the HIV-1 p24 antigen. Importantly, the Δ42PD1-mediated enhancement of immune responses was not observed in TLR4 knockout mice. Collectively, these data demonstrate that the immunogenicity and efficacy of DNA vaccines could be improved by the fusion of the extracellular domain of Δ42PD1 to target the immunogen to dendritic cells. [ABSTRACT FROM AUTHOR]

Published

2022

15. Transmission networks of hepatitis C virus among HIV/HCV-coinfected patients in Guangdong, China.

Author

Deng, Xizi, Liang, Zhiwei, Cai, Weiping, Li, Feng, Li, Junbin, Hu, Fengyu, and Lan, Yun

Subjects

HEPATITIS C virus, HIV, LOGISTIC regression analysis, MARRIED people, MARITAL status, IMMUNOLOGICAL deficiency syndromes, HIV infection transmission

Abstract

Background: Coinfection with hepatitis C virus (HCV) is common in human immunodeficiency virus (HIV)/acquired immunodeficiency syndrome (AIDS) patients due to shared routes of transmission. We aimed to investigate the characteristics of HCV subgenotypes among HIV/HCV-coinfected patients in Guangdong and explore the molecular transmission networks and related risk factors for HCV strains. Methods: Plasma samples were obtained from 356 HIV/HCV-coinfected patients for HCV NS5B region sequencing. A neighbor-joining phylogenetic tree was constructed to affirm HCV subgenotypes. The transmission networks based on maximum likelihood phylogenetic tree were determined by Cluster Picker, and visualized using Cytoscape 3.2.1. Results: A total of 302 HCV NS5B sequences were successfully amplified and sequenced from the 356 plasma samples. A neighbor-joining phylogenetic tree based on the 302 NS5B sequences revealed the profile of HCV subgenotypes circulating among HIV/HCV coinfection patients in Guangdong. Two predominant strains were found to be 6a (58.28%, 176/302) and 1b (18.54%, 56/302), followed by 3a (10.93%, 33/302), 3b (6.95%, 21/302), 1a (3.64%, 11/302), 2a (0.99%, 3/302) and 6n (0.66%, 2/302). A molecular transmission network of five major HCV genotypes was constructed, with a clustering rate of 44.04%. The clustering rates of subgenotypes 1a, 3a, 3b, 1b, and 6a were 18.18% (2/11), 42.42%, 52.38%, 48.21%, and 44.89%, respectively. Multivariate logistic regression analysis showed no significant effects from sex, age, transmission route, geographical region, baseline CD4 + T cell count or subgenotype (P > 0.05), except marital status. Married or cohabiting people (compared with unmarried people) had more difficulty forming transmission networks. Conclusions: In summary, this study, based on HCV NS5B subgenotypes, revealed the HCV subtype diversity and distribution among HIV/HCV-coinfected patients in Guangdong. Marital status inclined to be the factor influencing HCV transmission networks formation. [ABSTRACT FROM AUTHOR]

Published

2022

16. Genetic characterization of varicella-zoster and HIV-1 viruses from the cerebrospinal fluid of a co-infected encephalitic patient, Ghana

Author

El-Duah, Philip, Sylverken, Augustina Angelina, Owusu, Michael, Amoako, Yaw Ampem, Yeboah, Richmond, Gorman, Richmond, Nyarko-Afriyie, Emmanuella, Schneider, Julia, Jones, Terry C., Bonney, Joseph, Adade, Titus, Yeboah, Eric Smart, Binger, Tabea, Corman, Victor Max, Drosten, Christian, and Phillips, Richard Odame

Published

2022

17. Clinical and molecular aspects of human pegiviruses in the interaction host and infectious agent

Author

Samadi, Mehdi, Salimi, Vahid, Haghshenas, Mohammad Reza, Miri, Seyed Mohammad, Mohebbi, Seyed Reza, and Ghaemi, Amir

Published

2022

18. Analysis of HIV quasispecies and virological outcome of an HIV D+/R+ kidney–liver transplantation

Author

Rozera, Gabriella, Visco-Comandini, Ubaldo, Giombini, Emanuela, Santini, Francesco, Forbici, Federica, Berno, Giulia, Gruber, Cesare, De Paolis, Paolo, Colonnelli, Roberto, D’Offizi, Gianpiero, Ettorre, Giuseppe Maria, Grossi, Paolo, Capobianchi, Maria Rosaria, Ippolito, Giuseppe, and Abbate, Isabella

Published

2022

19. Prevalence of HIV and hepatitis B virus among pregnant women in Luanda (Angola): geospatial distribution and its association with socio-demographic and clinical-obstetric determinants

Author

Vueba, Amélia Nkutxi, Almendra, Ricardo, Santana, Paula, Faria, Clarissa, and do Céu Sousa, Maria

Published

2021

20. HPyV6 and HPyV7 in urine from immunocompromised patients

Author

Prezioso, Carla, Van Ghelue, Marijke, Moens, Ugo, and Pietropaolo, Valeria

Published

2021

21. Prevalence and characteristics of hepatitis B and D virus infections among HIV-positive individuals in Southwestern Nigeria

Author

Opaleye, Oluyinka Oladele, Akanbi, Olusola Anuoluwapo, Osundare, Folakemi Abiodun, Wang, Bo, Adesina, Olufisayo, Oluremi, Adeolu Sunday, Sunday, Sola Thomas, Akindele, Abiodun Akeem, Klink, Patrycja, and Bock, C. Thomas

Published

2021

22. Combination gene therapy for HIV using a conditional suicidal gene with CCR5 knockout

Author

Mehmetoglu-Gurbuz, Tugba, Yeh, Rose, Garg, Himanshu, and Joshi, Anjali

Published

2021