The Letter to the Editor commenting on our recent paper,Citation1 provides a concern regarding the statement “The immune-correlate analysis of the RV144 clinical trial revealed that human plasma IgA immune responses elicited by the RV144 vaccine correlated positively with a risk for HIV acquisition. This result once again emphasized that HIV vaccines can potentially have adverse effects leading to enhancement of infection.”
First of all, we would like to highlight that the statement regarding the RV144 trial is a minor speculation in the paper. We presented data that is statistically sound, and, for the purposes of discussion, also presented some speculative inferences from our data and data published by others, and we tried to make the latter quite easily distinguishable from the former for the average reader. Data in our paper pertains entirely to the AIDSVAX trial and not the RV144 trial.
Second, we would like to emphasize that nowhere in the paper did we conclude that the RV144 vaccine enhanced HIV infection in humans, only that this was a theoretical possibility for some subset of antibodies elicited by that vaccine. Specifically, the above-mentioned citation from our paper is a speculation that the simplest explanation for a direct correlation of any antibody level with infection generally is enhancement. As the IgA levels were a primary variable in the immune correlates analysis of the trial,Citation2 that result carries more weight than the subsequent follow-up studies as suggested by the Letter author. Nevertheless, our phrasing “can potentially” only means that occult enhancement by specific antibodies cannot be ruled out, not that it occurred to a physiologically significant degree. We fully agree that the RV144 trial clearly shows that antibodies can protect against HIV acquisition in humans, which is a major unprecedented positive result in the field.
Our paper suggests that, in the setting of improved prospects for a protective HIV vaccine, the field should be more cognizant of the possibility of enhancement by specific anti-HIV antibodies. The precise mechanisms leading to enhancement of HIV infection by vaccination remain poorly studied. This, in part, is due to the fact that vaccine-induced enhancement of HIV has been largely ignored by the HIV research community during the recent decades. In this light, our paper presenting statistical findings that may suggest potential enhancement of HIV infection in AIDSVAX VAX004 trialCitation3 can be helpful in distinguishing protective from enhancing antibodies in future research in this field.
References
- Shmelkov E, Nadas A, Cardozo T. Could vaccination with AIDSVAX immunogens have resulted in antibody-dependent enhancement of HIV infection in human subjects? Hum Vaccin Immunother 2014:1-4; PMID:25483466; http://dx.doi.org/10.4161/21645515.2014.972148
- Haynes BF, Gilbert PB, McElrath MJ, Zolla-Pazner S, Tomaras GD, Alam SM, et al. Immune-correlates analysis of an HIV-1 vaccine efficacy trial. N Engl J Med 2012; 366:1275-86; PMID:22475592; http://dx.doi.org/10.1056/NEJMoa1113425
- Flynn NM, Forthal DN, Harro CD, Judson FN, Mayer KH, Para MF. Placebo-controlled phase 3 trial of a recombinant glycoprotein 120 vaccine to prevent HIV-1 infection. J Infect Dis 2005; 191:654-65; PMID:15688278; http://dx.doi.org/10.1086/428404