SARS-CoV-2 B.1.617.2 Delta variant replication and immune evasion

Mlčochová, Petra; Kemp, Steven; Papa, Guido; Meng, Bo; Ferreira, Isabella; Datir, Rawlings P.; Collier, Dami; Albecka, Anna; Singh, Sujeet Kumar; Pandey, Rajesh; Brown, Jonathan C.; Zhou, Jie; Goonawardane, Niluka; Mishra, Swapnil; Whittaker, Charles; Mellan, Thomas A.; Marwal, Robin; Datta, Meena; Sengupta, Shantanu; Ponnusamy, Kalaiarasan; Radhakrishnan, Venkatraman; Abdullahi, Adam; Charles, Oscar; Chattopadhyay, Partha; Devi, Priti; Peacock, Thomas P.; Wattal, Chand; Goel, Neeraj; Satwik, Ambrish; Vaishya, Raju; Agarwal, Meenakshi; Chauhan, Himanshu; Dikid, Tanzin; Gogia, Hema; Lall, Hemlata; Verma, Kaptan; Dhar, Mahesh Shanker; Singh, Manoj Kumar; Soni, Namita; Meena, Namonarayan; Madan, Preeti; Singh, Priyanka; Sharma, Ramesh; Sharma, Rajeev; Kabra, Sandhya; Kumar, Sattender; Kumari, Swati; Sharma, Uma; Chaudhary, Urmila; Sivasubbu, Sridhar; Scaria, Vinod; Oberoi, Jaspal Kaur; Raveendran, Reena; Datta, Sandip K.; Das, Saumitra; Maitra, Arindam; Chinnaswamy, Sreedhar; Biswas, Nidhan K.; Parida, Ajay; Raghav, Sunil K.; Prasad, Punit; Sarin, Apurva; Mayor, Satyajit; Ramakrishnan, Uma; Palakodeti, Dasaradhi; Seshasayee, Aswin Sai Narain; Thangaraj, Kumarasamy; Bashyam, Murali D.; Dalal, Ashwin; Bhat, Manoj Kumar; Shouche, Yogesh S.; Pillai, Ajay D.; Abraham, Priya; Potdar, Varsha; Cherian, Sarah; Desai, Anita; Pattabiraman, Chitra; Manjunatha, M. V.; Mani, R; Udupi, Gautam Arunachal; Nandicoori, Vinay Kumar; Tallapaka, Karthik Bharadwaj; Sowpati, Divya Tej; Kawabata, Ryoko; Morizako, Nanami; Sadamasu, Kenji; Asakura, Hiroyuki; Nagashima, Mami; Yoshimura, Kazuhisa; Ito, Jumpei; Kimura, Izumi; Uriu, Keiya; Kosugi, Yusuke; Suganami, Mai; Oide, Akiko; Yokoyama, Miyabishara; Chiba, Mika; Saito, Akatsuki; Butlertanaka, Erika P.; Tanaka, Yuri; Ikeda, Terumasa; Motozono, Chihiro; Nasser, Hesham; Shimizu, Ryo; Yuan, Yue; Kitazato, Kazuko; Hasebe, Haruyo; Nakagawa, So; Wu, Jiaqi; Takahashi, Miyoko; Fukuhara, Takasuke; Shimizu, Kenta; Tsushima, Kana; Kubo, Haruko; Shirakawa, Kotaro; Kazuma, Yasuhiro; Nomura, Ryosuke; Horisawa, Yoshihito; Takaori‐Kondo, Akifumi; Tokunaga, Kenzo; Ozono, Seiya; Baker, Stephen; Dougan, Gordon; Hess, Christoph; Kingston, Nathalie; Lehner, Paul J.; Lyons, Paul; Matheson, Nicholas J; Owehand, Willem H.; Saunders, Caroline; Summers, Charlotte; Thaventhiran, James; Toshner, Mark; Weekes, Michael P.; Maxwell, Patrick H.; Shaw, Ashley; Bucke, Ashlea; Calder, Jo; Canna, Laura; Domingo, Jason; Elmer, Anne; Fuller, Stewart; Harris, Julie; Hewitt, Sarah; Kennet, Jane; Jose, Sherly; Kourampa, Jenny; Meadows, Anne; O’Brien, Criona; Price, Jane; Publico, Cherry; Rastall, Rebecca; Ribeiro, Carla M. S.; Rowlands, Jane; Ruffolo, Valentina; Tordesillas, Hugo; Bullman, Ben; Dunmore, Benjamin J.; Graf, Stefan Ting; Hodgson, Josh; Huang, Christopher L.‐H.; Hunter, Kelvin; Jones, Emma; Legchenko, Ekaterina; Matara, Cecilia; Martin, Jennifer; Mescia, Federica; O’Donnell, Ciara; Pointon, Linda; Pond, Nicole; Shih, Joy; Sutcliffe, Rachel; Tilly, Tobias; Treacy, Carmen; Tong, Zhen; Wood, Jennifer; Wylot, Marta; Bergamaschi, Laura; Betancourt, Ariana; Bower, Georgie; Cossetti, Chiara; De, Aloka; Epping, Madeline; Fawke, Stuart; Gleadall, Nick; Grenfell, Richard; Hinch, Andrew; Huhn, Oisín; Jackson, Sarah E.; Jarvis, Isobel; Krishna, Ben; Lewis, Daniel; Marsden, Joe; Nice, Francesca; Okecha, Georgina; Omarjee, Ommar; Perera, Marianne; Potts, Martin; Richoz, Nathan; Romashova, Veronika; Yarkoni, Natalia Savinykh; Sharma, Rahul; Stefanucci, Luca; Stephens, Jonathan; Strezlecki, Mateusz; Turner, Lori; Bie, Eckart M. D. D. De; Bunclark, Katherine; Josipovic, Masa; Mackay, Michael; Rossi, Sabrina; Selvan, Mayurun; Spencer, Sarah; Yong, Cissy; Allison, John; Butcher, Helen; Caputo, Daniela; Clapham-Riley, Debbie; Dewhurst, Eleanor; Furlong, Anita; Graves, Barbara; Gray, Jennifer; Ivers, Tasmin; Kasanicki, Mary; Gresley, Emma Le; Linger, Rachel; Meloy, Sarah; Muldoon, Francesca; Ovington, Nigel; Papadia, Sofia; Phelan, Isabel; Stark, Hannah; Stirrups, Kathleen; Townsend, Paul; Walker, Neil; Webster, Jennifer; Scholtes, Ingrid; Hein, Sabine; King, Rebecca; Mavousian, Antranik; Lee, Joo Hyeon; Bassi, Jessica; Silacci-Fegni, Chiara; Saliba, Christian; Pinto, Dora; Irie, Takashi; Yoshida, Isao; Hamilton, William L.; Sato, Kei; Bhatt, Samir; Flaxman, Seth; James, Leo C.; Corti, Davide; Piccoli, Luca; Barclay, Wendy S.; Rakshit, Partha; Agrawal, Anurag; Rk, Gupta

doi:10.1038/s41586-021-03944-y

Cited by 1,091 publications

(891 citation statements)

References 41 publications

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“…Moreover, studies with pseudoviruses and the authentic SARS-CoV-2-containing variant substitutions suggested that the neutralizing ability of the antibodies in sera raised after CoroVaxG.3 vaccination is only slightly reduced but overall largely preserved against the B.1.1.7, P.1 and B.1.617.2 lineages that are VOC-prevalent in Latin America [64]. This mild reduction in neutralization by a single dose of CoroVax.G3 vaccine-raised sera against the VOC is in the same range as that observed for sera of patients who received mRNA or adenoviral vector vaccines [65][66][67]; interestingly, one dose of the Pfizer or the Astra Zeneca vaccines induced almost undetectable levels of neutralizing antibodies against Delta [68].…”

Section: Discussionsupporting

confidence: 55%

A Single Dose of a Hybrid hAdV5-Based Anti-COVID-19 Vaccine Induces a Long-Lasting Immune Response and Broad Coverage against VOC

et al. 2021

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Most approved vaccines against COVID-19 have to be administered in a prime/boost regimen. We engineered a novel vaccine based on a chimeric human adenovirus 5 (hAdV5) vector. The vaccine (named CoroVaxG.3) is based on three pillars: (i) high expression of Spike to enhance its immunodominance by using a potent promoter and an mRNA stabilizer; (ii) enhanced infection of muscle and dendritic cells by replacing the fiber knob domain of hAdV5 by hAdV3; (iii) use of Spike stabilized in a prefusion conformation. The transduction with CoroVaxG.3-expressing Spike (D614G) dramatically enhanced the Spike expression in human muscle cells, monocytes and dendritic cells compared to CoroVaxG.5 that expressed the native fiber knob domain. A single dose of CoroVaxG.3 induced a potent humoral immunity with a balanced Th1/Th2 ratio and potent T-cell immunity, both lasting for at least 5 months. Sera from CoroVaxG.3-vaccinated mice was able to neutralize pseudoviruses expressing B.1 (wild type D614G), B.1.117 (alpha), P.1 (gamma) and B.1.617.2 (delta) Spikes, as well as an authentic P.1 SARS-CoV-2 isolate. Neutralizing antibodies did not wane even after 5 months, making this kind of vaccine a likely candidate to enter clinical trials.

show abstract

Section: Discussionsupporting

confidence: 55%

A Single Dose of a Hybrid hAdV5-Based Anti-COVID-19 Vaccine Induces a Long-Lasting Immune Response and Broad Coverage against VOC

et al. 2021

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“…* sublineages) variant. Delta was shown to spread faster than Alpha [1][2][3] and may be associated with higher virulence [4][5][6] and lower vaccine effectiveness [6,7] against symptomatic disease, especially with incomplete vaccination.…”

mentioning

confidence: 99%

Characterisation of vaccine breakthrough infections of SARS-CoV-2 Delta and Alpha variants and within-host viral load dynamics in the community, France, June to July 2021

Blanquart

Abad²,

Ambroise³

et al. 2021

Eurosurveillance

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We compared PCR results from SARS-CoV-2-positive patients tested in the community in France from 14 June to 30 July 2021. In asymptomatic individuals, Cq values were significantly higher in fully vaccinated than non-fully vaccinated individuals (effect size: 1.7; 95% CI: 1–2.3; p < 10−6). In symptomatic individuals and controlling for time since symptoms, the difference vanished (p = 0.26). Infections with the Delta variant had lower Cq values at symptom onset than with Alpha (effect size: −3.32; 95% CI: −4.38 to −2.25; p < 10−6).

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“…The coatings would need only periodic re-application depending on the amount of wear, for example 6-12 monthly, and would be widely available in the future. Such interventions are increasingly critical in conditions where viral variants with increased transmissibility are the new norm 14,[17][18][19] .…”

Section: Discussionmentioning

confidence: 99%

Rapid inactivation of SARS-CoV-2 by titanium dioxide surface coating

Micochova¹,

Chadha²,

Hesseloj³

et al. 2021

Wellcome Open Res

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Background: Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) transmission occurs via airborne droplets and surface contamination. Titanium dioxide (TiO2) coating of surfaces is a promising infection control measure, though to date has not been tested against SARS-CoV-2. Methods: Virus stability was evaluated on TiO2- and TiO2–Ag (Ti:Ag atomic ratio 1:0.04)-coated 45 x 45 mm ceramic tiles. After coating the tiles were stored for 2–4 months before use. We tested the stability of both SARS-CoV-2 Spike pseudotyped virions based on a lentiviral system, as well as fully infectious SARS-CoV-2 virus. For the former, tile surfaces were inoculated with SARS-CoV-2 spike pseudotyped HIV-1 luciferase virus. At intervals virus was recovered from surfaces and target cells infected. For live virus, after illuminating tiles for 0–300 min virus was recovered from surfaces followed by infection of Vero E6 cells. % of infected cells was determined by flow cytometry detecting SARS-CoV-2 nucleocapsid protein 24 h post-infection. Results: After 1 h illumination the pseudotyped viral titre was decreased by four orders of magnitude. There was no significant difference between the TiO2 and TiO2–Ag coatings. Light alone had no significant effect on viral viability. For live SARS-CoV-2, virus was already significantly inactivated on the TiO2 surfaces after 20 min illumination. After 5 h no detectable active virus remained. Significantly, SARS-CoV-2 on the untreated surface was still fully infectious at 5 h post-addition of virus. Overall, tiles coated with TiO2 120 days previously were able to inactivate SARS-CoV-2 under ambient indoor lighting with 87% reduction in titres at 1h and complete loss by 5h exposure. Conclusions: In the context of emerging viral variants with increased transmissibility, TiO2 coatings could be an important tool in containing SARS-CoV-2, particularly in health care facilities where nosocomial infection rates are high.

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SARS-CoV-2 B.1.617.2 Delta variant replication and immune evasion

Cited by 1,091 publications

References 41 publications

A Single Dose of a Hybrid hAdV5-Based Anti-COVID-19 Vaccine Induces a Long-Lasting Immune Response and Broad Coverage against VOC

A Single Dose of a Hybrid hAdV5-Based Anti-COVID-19 Vaccine Induces a Long-Lasting Immune Response and Broad Coverage against VOC

Characterisation of vaccine breakthrough infections of SARS-CoV-2 Delta and Alpha variants and within-host viral load dynamics in the community, France, June to July 2021

Rapid inactivation of SARS-CoV-2 by titanium dioxide surface coating

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