Abstract

The role of chemokine receptors in HIV infection across the placenta The main hypothesis of this proposal is that substances (cytokines, chemokines) suppress HIV-co-receptor expression in placenta cells. Despite the progress in preventing HIV-1 infection in children with prenatal ZDV treatment, the mechanism by which the virus penetrates the placental barrier and enters the fetal circulation is not clear. It has been shown that placental that placental macrophages (Hofbauer cells, HF) are susceptible cell free HIV while trophoblasts are susceptible only to transfected virus. We found that HF cells are less susceptible than monocyte derived macrophages (MDM) to infection with HIV-BaL, an R5 virus. Both trophoblasts and Hofbauer cells produce cytokines. Through the proposed experiments, we will investigate the mechanisms of increased resistance to HIV by HF cells and elucidate the specific mechanisms that limit HIV entry in placenta cells.
The specific aims of this period are: 1) To determine the in vivo HIV co-receptor and chemokine expression Hofbauer cells by immunohistochemistry on frozen term placenta sections. 2) To determine chemokine receptor expression (CXCR4, CC45, CCR3, and STRL33) in Hofbauer cells and Trophoblasts by immunofluorescence and 2-color cytofluorometry. 3) To determine the susceptibility of Hofbauer cells to HIV variants derived from vertical transmission. 4) To determine the effect of trophoblast and Hofbauer cells supernatants on HIV replication by PBMC and MDM. The in vitro HIV infection of Hofbauer cells will be conducted using primary isolates characterized for co-receptor utilization and derived from vertical transmission. Four of these viruses have been isolated from transmitter and non-transmitted mothers in Puerto Rico. Additional variants will be obtained from the NIH AIDS Reagent Program in order to identify viral isolates with distinct co-receptor usage. This study will elucidate the viral and host determinants associated with resistance of the placenta to vertical transmission.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Minority Biomedical Research Support - MBRS (S06)
Project #
2S06GM008224-16
Application #
6336532
Study Section
Project Start
2000-08-01
Project End
2001-07-31
Budget Start
Budget End
Support Year
16
Fiscal Year
2000
Total Cost
Indirect Cost

  Institution

Name
University of Puerto Rico Med Sciences
Department
Type
DUNS #
City
San Juan
State
PR
Country
United States
Zip Code
00936

  Publications

Rijpma, Sanna R; van der Velden, Maarten; González-Pons, Maria et al. (2016) Multidrug ATP-binding cassette transporters are essential for hepatic development of Plasmodium sporozoites. Cell Microbiol 18:369-83
Padín-Irizarry, Vivian; Colón-Lorenzo, Emilee E; Vega-Rodríguez, Joel et al. (2016) Glutathione-deficient Plasmodium berghei parasites exhibit growth delay and nuclear DNA damage. Free Radic Biol Med 95:43-54
Jardón, Javier; Izquierdo, Natalio J; Renta, Jessica Y et al. (2016) Ocular Findings in Patients with the Hermansky-Pudlak Syndrome (Types 1 and 3). Ophthalmic Genet 37:89-94
Rivera-Peña, Bianca; Ruíz-Fullana, Francisco J; Vélez-Reyes, Germán L et al. (2016) HPV-16 infection modifies overall survival of Puerto Rican HNSCC patients. Infect Agent Cancer 11:47
Velásquez-Martínez, Maria C; Vázquez-Torres, Rafael; Rojas, Legier V et al. (2015) Alpha-1 adrenoreceptors modulate GABA release onto ventral tegmental area dopamine neurons. Neuropharmacology 88:110-21
Vega-Rodríguez, Joel; Pastrana-Mena, Rebecca; Crespo-Lladó, Keila N et al. (2015) Implications of Glutathione Levels in the Plasmodium berghei Response to Chloroquine and Artemisinin. PLoS One 10:e0128212
Zenón, Frances; Cantres-Rosario, Yisel; Adiga, Radhika et al. (2015) HIV-infected microglia mediate cathepsin B-induced neurotoxicity. J Neurovirol 21:544-58
Ortiz, A P; Unger, E R; Muñoz, C et al. (2014) Cross-sectional study of HPV-16 infection in a population-based subsample of Hispanic adults. BMJ Open 4:e004203
Rosas, Odrick R; Torrado, Aranza I; Santiago, Jose M et al. (2014) Long-term treatment with PP2 after spinal cord injury resulted in functional locomotor recovery and increased spared tissue. Neural Regen Res 9:2164-73
Mosquera, Laurivette; Colón, Jennifer M; Santiago, José M et al. (2014) Tamoxifen and estradiol improved locomotor function and increased spared tissue in rats after spinal cord injury: their antioxidant effect and role of estrogen receptor alpha. Brain Res 1561:11-22

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