The Emerging Role for CTL Epitope Specificity in HIV Cure Efforts

The development of an effective human immunodeficiency virus (HIV) cure is a critical global health priority. A major obstacle to this effort is the establishment of a latent reservoir of HIV infected cells, which necessitates lifelong therapy, causing both logistical and adherence burdens for infected individuals. However, in a subset of these individuals, cytotoxic T lymphocytes (CTLs) can durably suppress viral outgrowth in the absence of therapy, providing a path towards a viable HIV cure. In this review, we discuss the emerging role that CTLs have in HIV cure efforts, with particular emphasis on epitope specificity. Recent studies have demonstrated that successful in vivo containment of the virus is rooted in the specific targeting of fitness-constrained, mutation-resistant regions of the HIV proteome. We highlight these new insights, providing context with previous observations in HIV and other models of viral control, and delineate their translation into a therapeutic vaccine.

Automated summary

The development of an effective HIV cure is crucial, with the role of CTLs in suppressing viral outgrowth without therapy being emphasized. Successful containment of the virus in vivo is dependent on targeting mutation-resistant regions within the HIV proteome, highlighting the potential for therapeutic vaccine development.