René Olivares-Navarrete, D.D.S, Ph.D.

Associate Professor, Department of Biomedical Engineering | D.D.S, National Autonomous University of Mexico | Ph.D., National Autonomous University of Mexico VCU DEPT OF BIOMEDICAL ENGINEERING

  • RICHMOND VA

Olivares-Navarrete’s research focuses on Tissue Engineering and Regenerative Medicine approaches for Craniofacial and Orthopaedic needs.

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VCU College of Engineering

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Biography

Olivares-Navarrete’s research at VCU focuses on Tissue Engineering and Regenerative Medicine approaches for Craniofacial and Orthopaedic needs. His lab uses different approaches such as biomaterial surface modifications, 3D bioprinting, decellularized tissue hydrogels, etc., aimed for immunomodulation, speed up healing process, and tissue regeneration. His lab also is constantly developing animal models that resemble disease conditions such smoking, e-cigarette use, diabetes, aging, obesity, etc., to implement tissue engineering and regenerative medicine approaches created in his lab. He is a member of the International Association for Dental Research, Society for Biomaterials, Biomedical Engineering Society, Orthopaedic Research Society, and The American Society for Bone and Mineral Research.

Industry Expertise

Education/Learning
Research

Areas of Expertise

Tissue Engineering
Stem Cell Biology and Engineering
Biomaterials for Craniofacial and Musculoskeletal Tissues
Immunomodulation and Immunoengineering
Wnt Signaling in Morphogenesis Healing and Regeneration
Craniofacial Development and Abnormalities

Accomplishments

Young Investigator Award, International Conference on the Chemistry and Biology of Mineralized Tissues

2007

National Research Prize in Dentistry by GlaxoSmithKline

2005

Fellowship DGEP, Georgia Institute of Technology

2003-2004

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Education

Georgia Institute of Technology

Postdoctoral Fellow

Biomedical Engineering

National Autonomous University of Mexico

Ph.D.

Biomaterials and Cell Biology

National Autonomous University of Mexico

D.D.S.

Dentistry

Affiliations

  • International Association for Dental Research
  • Society for Biomaterials
  • Orthopeadic Research Society
  • The American Society for Bone and Mineral Research
  • Biomedical Engineering Society

Media Appearances

Jeremy Meeks' Pregnant Girlfriend Chloe Green Caught Vaping

popculture.celebrity  online

2018-05-26

"Understanding if there is one or hundreds of molecules in e-cigarette vapor that negatively affect craniofacial development is a difficult task because the number of commercially available e-liquids is in the thousands." René Olivares-Navarrete, D.D.S., Ph.D., an assistant professor in the Department of Biomedical Engineering, said. "But finding these answers would give us a better understanding of the possible adverse effects of e-cigarettes."

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Are E-Cigarettes Safe While Pregnant?

Labmate  online

2017-12-13

For co-author René Olivares-Navarrete, the study has revealed just a small glimpse at the potential dangers and outcomes of e-cigarettes.

“Understanding if there is one or hundreds of molecules in e-cigarette vapor that negatively affect craniofacial development is a difficult task because the number of commercially available e-liquids is in the thousands,” comments Olivares-Navarrete. “But finding these answers would give us a better understanding of the possible adverse effects of e-cigarettes.”

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Some E-Cigarette Flavors May Be More Harmful Than Others

The Atlantic  online

2017-11-28

Many of these chemicals have never been tested on whether they’re safe to breathe in. And that makes vaping’s already unclear effects on health even murkier, because different flavors could be more or less dangerous.

A recent study investigated the effects of six different e-cig vapors on tadpoles, as a proxy test for how vaping while pregnant might affect human embryos. Some of the exposed tadpoles developed “clefts” in the bone behind the upper lip, somewhat similar to cleft palate in humans. These clefts only appeared in tadpoles exposed to two particular flavors out of six tested. When the researchers exposed tadpoles to nicotine-free versions of the same flavors, those tadpoles still developed clefts in the same ratios.

These initial studies are “just small steps,” says René Olivares-Navarrete, a bioengineering assistant professor at VCU and another coauthor on the tadpole study. As with Tarran’s cell lines, results in tadpoles and mice may or may not translate to humans. Olivares-Navarette says he hopes that e-cigarettes are as safe as vaping advocates claim, but first, “people need to have the information about what is possible.”

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Selected Articles

mplant Surface Design Regulates Mesenchymal Stem Cell Differentiation and Maturation

Advances in Dental Research

2016-03-04

Changes in dental implant materials, structural design, and surface properties can all affect biological response. While bulk properties are important for mechanical stability of the implant, surface design ultimately contributes to osseointegration. This article reviews the surface parameters of dental implant materials that contribute to improved cell response and osseointegration. In particular, we focus on how surface design affects mesenchymal cell response and differentiation into the osteoblast lineage. Surface roughness has been largely studied at the microscale, but recent studies have highlighted the importance of hierarchical micron/submicron/nanosurface roughness, as well as surface roughness in combination with surface wettability. Integrins are transmembrane receptors that recognize changes in the surface and mediate downstream signaling pathways. Specifically, the noncanonical Wnt5a pathway has been implicated in osteoblastic differentiation of cells on titanium implant surfaces. However, much remains to be elucidated. Only recently have studies been conducted on the differences in biological response to implants based on sex, age, and clinical factors; these all point toward differences that advocate for patient-specific implant design. Finally, challenges in implant surface characterization must be addressed to optimize and compare data across studies. An understanding of both the science and the biology of the materials is crucial for developing novel dental implant materials and surface modifications for improved osseointegration.

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In vitro cytotoxicity of amorphous carbon films

Biomedical Materials and Engineering

2005-04-15

Amorphous carbon (a-C), carbon nitride (a-CN) and titanium films were deposited on stainless steel substrates (SS) using a dc magnetron sputtering system attached to a high vacuum chamber. Films were deposited using a base pressure of 1.3x10(-4) Pa. For the carbon films a pure graphite target was eroded in an Argon plasma. For the case of the a-CN films, the Ar flux was substituted by 100% N2 gas. Titanium films were deposited in a different chamber, using a pure Ti target and an argon plasma. In vitro studies were carried out on the coated samples using human osteoblasts cells. Cytotoxicity of carbon films was assessed by cellular adhesion and proliferation, as determined by direct cellular counting using a spectroscopic technique and a well-defined standard curve. Osteoblasts cells were also grown on uncoated steel and prepared Petri dishes for comparison. The percentage of osteoblasts adhesion measured at 24 hrs attained maximum values for the a-C films. Similarly, cellular proliferation evaluated at three, five and seven days showed an outstanding increase of osteoblasts cells for the a-C and Ti coatings in contrast to the uncoated steel. The cell functionality was evaluated by the MTT test after incubation periods of 3, 5 and 7 days. The absorbance values obtained for a-C, a-CN and Ti surfaces resulted significantly higher with respect to the positive control, indicating that the surface did not induce any toxic effect. Preliminary bio-mineralization was evaluated by measuring the elemental composition of the mineral grown on the substrates after periods up to 14 days.

Integrin beta1 silencing in osteoblasts alters substrate-dependent responses to 1,25-dihydroxy vitamin D3

Biomaterials

2006-07-07

Surface microroughness increases osteoblast differentiation and enhances responses of osteoblasts to 1,25-dihydroxyvitamin D3 [1alpha,25(OH)2D3]. The observations that beta1 integrin expression is increased in osteoblasts grown on Ti substrates with rough microarchitecture, and that it is regulated by 1alpha,25(OH)2D3 in a surface-dependent manner, suggest that beta1 may play a role in mediating osteoblast response. To test this hypothesis, we silenced beta1 expression in MG63 human osteoblast-like cells using small interfering RNA (siRNA) and examined the responses of the beta1-silenced osteoblasts to surface microtopography and 1alpha,25(OH)2D3. To better understand the role of beta1, MG63 cells were also treated with two different monoclonal antibodies to human beta1 to block ligand binding. beta1-silenced MG63 cells grown on a tissue culture plastic had reduced alkaline phosphatase activity and levels of osteocalcin, transforming growth factor beta1, prostaglandin E2, and osteoprotegerin in comparison with control cells. Moreover, beta1-silencing inhibited the effects of surface roughness on these parameters and partially inhibited effects of 1alpha,25(OH)2D3. Anti beta1 antibody AIIB2 had no significant effect on cell number and osteocalcin, but decreased alkaline phosphatase; MAB2253Z caused dose-dependent decreases in cell number and alkaline phosphatase and an increase in osteocalcin. Effects of 1alpha,25(OH)2D3 on cell number and alkaline phosphatase were reduced and effects on osteocalcin were increased. These findings indicate that beta1 plays a major and complex role in osteoblastic differentiation modulated by either surface microarchitecture or 1alpha,25(OH)2D3. The results also show that beta1 mediates, in part, the synergistic effects of surface roughness and 1alpha,25(OH)2D3.

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