Because available resources are limited, this will require coordinated decision-making by funders and research groups, likely at the cost of testing a smaller total number of candidates. In the process, it will be important not to stifle innovation and to inhibitors continue encouraging vaccine concepts with distinct immunological profiles. The field may learn from the Idelalisib mouse preventive HIV vaccines, where the Immune Space Template
[http://www.vaccineenterprise.org/immunespace] has been designed for a more rational comparison and prioritization of candidates. Rather than retreating in the face of the problems, therapeutic vaccination and development efforts – both privately and publicly funded – have continued (Fig. 3). The evidence that a therapeutic vaccine approach may be able to contribute to achieving a cure has now added impetus to efforts to refine and improve therapeutic vaccine candidates. At the same time, scientific progress in understanding HIV latency and in design of therapeutic
vaccines that modestly and temporarily reduce viral load provides an opportunity to begin to solve the problems that have impeded achieving significant clinical benefit. The therapeutic vaccine field lies on the intersection of several active areas of HIV research: preventive vaccines, treatment, and cure. Active links must be encouraged between researchers in those related fields through productive Vorinostat collaborations and common discussion to share ideas, latest discoveries, Oxalosuccinic acid and resources. Work by researchers, funders and advocates remains critically important for increasing awareness and understanding regarding the new era in therapeutic vaccine research and the possibility of ultimately benefitting public health. All authors: no conflicts. Participants in workshop and coauthors who participated in manuscript preparation: Nasra Aidarus (AVAC: Global Advocacy for HIV Prevention), Jean Boyer (University of Pennsylvania), Steven Deeks (University of California San Francisco), Jose Esparza (University of Maryland, School of Medicine),
Anders Fomsgaard (Statens Serum Institut, and University of Southern Denmark), Felipe Garcia (Hospital Clinic—HIVACAT IDIBAPS, University of Barcelona), Rowena Johnston (amfAR, The Foundation for AIDS Research), Yves Levy (Vaccine Research Institute), Jeff Lifson (AIDS and Cancer Virus Program, Frederick National Laboratory), Margaret McCluskey (U.S. Agency for International Development), George N. Pavlakis (Centre for Cancer Research, National Cancer Institute), Deborah Persaud (Johns Hopkins University School of Medicine), Harriet Robinson (GeoVax), Janet Siliciano (Johns Hopkins University School of Medicine). “
“Due to the high rate of influenza infection in children and the availability of safe and effective vaccines [1], [2], [3], [4] and [5], the US Centers for Disease Control and Prevention recommends influenza vaccination for all children 6 months and older for their own protection [6].