Abstract
In people living with HIV (PLWH), chronic inflammation can lead to cancer initiation and progression, besides driving a dysregulated and diminished immune responsiveness. HIV infection also leads to increased transcription of Human Endogenous Retroviruses (HERVs), which could increase an inflammatory environment and create a tumor growth suppressive environment with high expression of pro-inflammatory cytokines. In order to determine the impact of HIV infection to HERV expression on the breast cancer microenvironment, we sequenced total RNA from formalin-fixed paraffin-embedded (FFPE) breast cancer samples of women HIV-negative and HIV-positive for transcriptome and retrotranscriptome analyses. We performed RNA extraction from FFPE samples, library preparation and total RNA sequencing (RNA-seq). The RNA-seq analysis shows 185 differentially expressed genes: 181 host genes (178 upregulated and three downregulated) and four upregulated HERV transcripts in HIV-positive samples. We also explored the impact of HERV expression in its neighboring breast cancer development genes (BRCA1, CCND1, NBS1/NBN, RAD50, KRAS, PI3K/PIK3CA) and in long non-coding RNA expression (AC060780.1, also known as RP11-242D8.1). We found a significant positive association of HERV expression with RAD50 and with AC060780.1, which suggest a possible role of HERV in regulating breast cancer genes from PLWH with breast cancer. In addition, we found immune system, extracellular matrix organization and metabolic signaling genes upregulated in HIV-positive breast cancer. In conclusion, our findings provide evidence of transcriptional and retrotranscriptional changes in breast cancer from PLWH compared to non-HIV breast cancer, including dysregulation of HERVs, suggesting an indirect effect of the virus on the breast cancer microenvironment.
Highlights
The majority of mammary tumors in mice are caused by the mouse mammary tumor virus (MMTV) [1], and the suggestion that a retrovirus related to MMTV might be involved in breast cancer in humans is one of the longest running controversies in human retrovirology [2, 3]
We found a total of 181 differentially expressed genes (DEGs) when comparing both groups, HIV-positive and HIVnegative breast cancer [FDR < 0.05, absolute(log2FoldChange) > 1.0; Figures 1A,B]
To biologically validate these findings, we performed IHC assay to detect the expression of four proteins (PROM1, FIGURE 1 | Differentially expressed genes in breast cancer from HIV patients. (A) Volcano plot shows differentially expressed Human Endogenous Retroviruses (HERVs) and host genes, up-regulated and down-regulated in breast cancer HIV-positive samples
Summary
The majority of mammary tumors in mice are caused by the mouse mammary tumor virus (MMTV) [1], and the suggestion that a retrovirus related to MMTV might be involved in breast cancer in humans is one of the longest running controversies in human retrovirology [2, 3]. Studies of the breast cancer cell line T47D showed retroviral particles which were responsive to estradiol [4,5,6,7,8]. These were later identified as human endogenous retrovirus (HERV)-K envelope transcripts, and were found both in cell lines and in breast cancer tissues [9, 10]. HERVs are “fossil” retrovirus sequences remnant in the human genome, which originated millions of years ago from retrovirus germline cell infections. They are transmitted vertically, but they do not show infective capabilities in humans [11,12,13]. They comprise ∼8% of the human genome [14]
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