Author:
Ou Li, ,Kong Wing-Pui,Chuang Gwo-Yu,Ghosh Mridul,Gulla Krishana,O’Dell Sijy,Varriale Joseph,Barefoot Nathan,Changela Anita,Chao Cara W.,Cheng Cheng,Druz Aliaksandr,Kong Rui,McKee Krisha,Rawi Reda,Sarfo Edward K.,Schön Arne,Shaddeau Andrew,Tsybovsky Yaroslav,Verardi Raffaello,Wang Shuishu,Wanninger Timothy G.,Xu Kai,Yang Gengcheng J.,Zhang Baoshan,Zhang Yaqiu,Zhou Tongqing,Arnold Frank J.,Doria-Rose Nicole A.,Lei Q. Paula,Ryan Edward T.,Vann Willie F.,Mascola John R.,Kwong Peter D.
Abstract
AbstractThe vaccine elicitation of broadly neutralizing antibodies against HIV-1 is a long-sought goal. We previously reported the amino-terminal eight residues of the HIV-1-fusion peptide (FP8) – when conjugated to the carrier protein, keyhole limpet hemocyanin (KLH) – to be capable of inducing broadly neutralizing responses against HIV-1 in animal models. However, KLH is a multi-subunit particle derived from a natural source, and its manufacture as a clinical product remains a challenge. Here we report the preclinical development of recombinant tetanus toxoid heavy chain fragment (rTTHC) linked to FP8 (FP8-rTTHC) as a suitable FP-conjugate vaccine immunogen. We assessed 16 conjugates, made by coupling the 4 most prevalent FP8 sequences with 4 carrier proteins: the aforementioned KLH and rTTHC; the H. influenzae protein D (HiD); and the cross-reactive material from diphtheria toxin (CRM197). While each of the 16 FP8-carrier conjugates could elicit HIV-1-neutralizing responses, rTTHC conjugates induced higher FP-directed responses overall. A Sulfo-SIAB linker yielded superior results over an SM(PEG)2 linker but combinations of carriers, conjugation ratio of peptide to carrier, or choice of adjuvant (Adjuplex or Alum) did not significantly impact elicited FP-directed neutralizing responses in mice. Overall, SIAB-linked FP8-rTTHC appears to be a promising vaccine candidate for advancing to clinical assessment.
Publisher
Springer Science and Business Media LLC