A combined adjuvant approach primes robust germinal center responses and humoral immunity in non-human primates.
Ivy PhungKristen A RodriguesEster Marina-ZárateLaura MaiorinoBapi PaharWen-Hsin LeeMariane MeloAmitinder KaurCarolina AllersMarissa FahlbergBrooke F GraspergeJason P DufourFaith SchiroPyone P AyePaul G LopezJonathan L TorreGabriel OzorowskiSaman EskandarzadehMichael KubitzErik GeorgesonBettina GroschelRebecca NedellecMichael BickKatarzyna Kaczmarek MichaelsHongmei GaoXiaoying X ShenDiane G CarnathanGuido SilvestriDavid C MontefioriAndrew B WardLars HangartnerRonald S VeazeyDennis R BurtonWilliam R SchiefDarrell J IrvineShane CrottyPublished in: Nature communications (2023)
Adjuvants and antigen delivery kinetics can profoundly influence B cell responses and should be critically considered in rational vaccine design, particularly for difficult neutralizing antibody targets such as human immunodeficiency virus (HIV). Antigen kinetics can change depending on the delivery method. To promote extended immunogen bioavailability and to present antigen in a multivalent form, native-HIV Env trimers are modified with short phosphoserine peptide linkers that promote tight binding to aluminum hydroxide (pSer:alum). Here we explore the use of a combined adjuvant approach that incorporates pSer:alum-mediated antigen delivery with potent adjuvants (SMNP, 3M-052) in an extensive head-to-head comparison study with conventional alum to assess germinal center (GC) and humoral immune responses. Priming with pSer:alum plus SMNP induces additive effects that enhance the magnitude and persistence of GCs, which correlate with better GC-T FH cell help. Autologous HIV-neutralizing antibody titers are improved in SMNP-immunized animals after two immunizations. Over 9 months after priming immunization of pSer:alum with either SMNP or 3M-052, robust Env-specific bone marrow plasma cells (BM B PC ) are observed. Furthermore, pSer-modification of Env trimer reduce targeting towards immunodominant non-neutralizing epitopes. The study shows that a combined adjuvant approach can augment humoral immunity by modulating immunodominance and shows promise for clinical translation.
Keyphrases
- human immunodeficiency virus
- immune response
- antiretroviral therapy
- hiv infected
- hepatitis c virus
- hiv positive
- bone marrow
- hiv aids
- hiv testing
- early stage
- men who have sex with men
- dengue virus
- cell therapy
- induced apoptosis
- mesenchymal stem cells
- endothelial cells
- blood brain barrier
- signaling pathway
- toll like receptor
- zika virus
- drug delivery
- south africa
- machine learning
- big data
- platelet rich plasma
- cell death
- optic nerve
- mass spectrometry
- artificial intelligence
- cell proliferation
- gold nanoparticles
- endoplasmic reticulum stress
- cancer therapy