Your search keyword '"Abebe, Yonas"' showing total 4 results

1. In vitro production of infectious Plasmodium falciparumsporozoites

Author

Eappen, Abraham G., Li, Tao, Marquette, Meghan, Chakravarty, Sumana, KC, Natasha, Zanghi, Gigliola, Hoffman, Benjamin U., Hettiarachchi, Hashani, Patil, Asha, Abebe, Yonas, Tran, Christiane, Yossef, Alemtaye A., McWilliams, Ian, Morrison, Robert D., Rathakrishnan, Ayyappan, Inbar, Ehud, Aly, Ahmed S. I., De La Vega, Patricia, Belmonte, Maria, Sedegah, Martha, Wai, Tint, Campo, Joseph J., King, Harley, Kappe, Stefan H. I., Li, MingLin, Billingsley, Peter F., Sim, B. Kim Lee, and Hoffman, Stephen L.

Abstract

An effective vaccine is needed for the prevention and elimination of malaria. The only immunogens that have been shown to have a protective efficacy of more than 90% against human malaria are Plasmodium falciparum(Pf) sporozoites (PfSPZ) manufactured in mosquitoes (mPfSPZ)1–7. The ability to produce PfSPZ in vitro (iPfSPZ) without mosquitoes would substantially enhance the production of PfSPZ vaccines and mosquito-stage malaria research, but this ability is lacking. Here we report the production of hundreds of millions of iPfSPZ. iPfSPZ invaded human hepatocytes in culture and developed to mature liver-stage schizonts expressing P. falciparummerozoite surface protein 1 (PfMSP1) in numbers comparable to mPfSPZ. When injected into FRGhuHep mice containing humanized livers, iPfSPZ invaded the human hepatocytes and developed to PfMSP1-expressing late liver stage parasites at 45% the quantity of cryopreserved mPfSPZ. Human blood from FRGhuHep mice infected with iPfSPZ produced asexual and sexual erythrocytic-stage parasites in culture, and gametocytes developed to PfSPZ when fed to mosquitoes, completing the P. falciparumlife cycle from infectious gametocyte to infectious gametocyte without mosquitoes or primates.

Published

2022

2. Anti-merozoite antibodies induce natural killer cell effector function and are associated with immunity against malaria

Author

Odera, Dennis O., Tuju, James, Mwai, Kennedy, Nkumama, Irene N., Fürle, Kristin, Chege, Timothy, Kimathi, Rinter, Diehl, Stefan, Musasia, Fauzia K., Rosenkranz, Micha, Njuguna, Patricia, Hamaluba, Mainga, Kapulu, Melissa C., Frank, Roland, Osier, Faith H. A., Abdi, Abdirahman I., Chi, Primus Che, de Laurent, Zaydah, Jao, Irene, Kamuya, Dorcas, Kamuyu, Gathoni, Makale, Johnstone, Murungi, Linda, Musyoki, Jennifer, Muthui, Michelle, Mwacharo, Jedidah, Kariuki, Silvia, Mwanga, Daniel, Mwongeli, Joyce, Ndungu, Francis, Njue, Maureen, Nyangweso, George, Kimani, Domitila, Ngoi, Joyce M., Musembi, Janet, Ngoto, Omar, Otieno, Edward, Ooko, Michael, Shangala, Jimmy, Wambua, Juliana, Mohammed, Khadija Said, Omuoyo, Donwilliams, Mosobo, Moses, Kibinge, Nelson, Kinyanjui, Sam, Bejon, Philip, Lowe, Brett, Marsh, Kevin, Marsh, Vicki, Abebe, Yonas, Billingsley, Peter F., Sim, Betty Kim Lee, Hoffman, Stephen L., James, Eric R., Richie, Thomas L., Audi, Agnes, Olewe, Fredrick, Oloo, James, Ongecha, John, Ongas, Martin O., Koskei, Nelly, Bull, Peter C., Hodgson, Susanne H., Kivisi, Cheryl, Imwong, Mallika, Murphy, Sean C., Ogutu, Bernhards, Tarning, Joel, Winterberg, Markus, and Williams, Thomas N.

Abstract

Natural killer (NK) cells are potent immune effectors that can be activated via antibody-mediated Fc receptor engagement. Using multiparameter flow cytometry, we found that NK cells degranulate and release IFN-γ upon stimulation with antibody-opsonized Plasmodium falciparummerozoites. Antibody-dependent NK (Ab-NK) activity was largely strain transcending and enhanced invasion inhibition into erythrocytes. Ab-NK was associated with the successful control of parasitemia after experimental malaria challenge in African adults. In an independent cohort study in children, Ab-NK increased with age, was boosted by concurrent P. falciparuminfections, and was associated with a lower risk of clinical episodes of malaria. Nine of the 14 vaccine candidates tested induced Ab-NK, including some less well-characterized antigens: P41, P113, MSP11, RHOPH3, and Pf_11363200. These data highlight an important role of Ab-NK activity in immunity against malaria and provide a potential mechanism for evaluating vaccine candidates.

Published

2023

3. A randomized controlled trial showing safety and efficacy of a whole sporozoite vaccine against endemic malaria

Author

Sirima, Sodiomon B., Ouédraogo, Alphonse, Tiono, Alfred B., Kaboré, Jean M., Bougouma, Edith C., Ouattara, Maurice S., Kargougou, Désiré, Diarra, Amidou, Henry, Noelie, Ouédraogo, Issa N., Billingsley, Peter F., Manoj, Anita, Abebe, Yonas, KC, Natasha, Ruben, Adam, Richie, Thomas L., James, Eric R., Joshi, Sudhaunshu, Shrestha, Biraj, Strauss, Kathy, Lyke, Kirsten E., Plowe, Christopher V., Potter, Gail E., Cox, Catherine, Jones, Walter, Sim, B. Kim Lee, Hoffman, Stephen L., and Laurens, Matthew B.

Abstract

A highly effective malaria vaccine remains elusive despite decades of research. Plasmodium falciparumsporozoite vaccine (PfSPZ Vaccine), a metabolically active, nonreplicating, whole parasite vaccine demonstrated safety and vaccine efficacy (VE) against endemic P. falciparumfor 6 months in Malian adults receiving a five-dose regimen. Safety, immunogenicity, and VE of a three-dose regimen were assessed in adults in Balonghin, Burkina Faso in a two-component study: an open-label dose escalation trial with 32 participants followed by a double-blind, randomized, placebo-controlled trial (RCT) with 80 participants randomized to receive three doses of 2.7 × 106PfSPZ (N= 39) or normal saline (N= 41) just before malaria season. To clear parasitemia, artesunate monotherapy was administered before first and last vaccinations. Thick blood smear microscopy was performed on samples collected during illness and every 4 weeks for 72 weeks after last vaccinations, including two 6-month malaria transmission seasons. Safety outcomes were assessed in all 80 participants who received at least one dose and VE for 79 participants who received three vaccinations. Myalgia was the only symptom that differed between groups. VE (1 − risk ratio; primary VE endpoint) was 38% at 6 months (P= 0.017) and 15% at 18 months (0.078). VE (1 − hazard ratio) was 48% and 46% at 6 and 18 months (P= 0.061 and 0.018). Two weeks after the last dose, antibodies to P. falciparumcircumsporozoite protein and PfSPZ were higher in protected versus unprotected vaccinees. A three-dose regimen of PfSPZ Vaccine demonstrated safety and efficacy against malaria infection in malaria-experienced adults.

Published

2022

4. A double-blind, placebo-controlled phase 1/2a trial of the genetically attenuated malaria vaccine PfSPZ-GA1

Author

Roestenberg, Meta, Walk, Jona, van der Boor, Saskia C., Langenberg, Marijke C. C., Hoogerwerf, Marie-Astrid, Janse, Jacqueline J., Manurung, Mikhael, Yap, X. Zen, García, Amanda Fabra, Koopman, Jan Pieter R., Meij, Pauline, Wessels, Els, Teelen, Karina, van Waardenburg, Youri M., van de Vegte-Bolmer, Marga, van Gemert, Geert Jan, Visser, Leo G., van der Ven, André J. A. M., de Mast, Quirijn, Natasha, K. C., Abebe, Yonas, Murshedkar, Tooba, Billingsley, Peter F., Richie, Tom L., Sim, B. Kim Lee, Janse, Chris J., Hoffman, Stephen L., Khan, Shahid M., and Sauerwein, Robert W.

Abstract

The genetically attenuated malaria vaccine PfSPZ-GA1 is safe, immunogenic, and has suboptimal protective efficacy in people.

Published

2020