Graphene
family materials (GFMs) are extensively explored for various
biomedical applications due to their unique physical properties. The
prime challenge is to establish a conclusive safety profile of these
nanomaterials and their respective products or devices. Formulating
GFMs with appropriate ingredients (e.g., surfactant/compatibilizer)
will help to disperse them homogeneously (i.e., within the polymer
matrix in the case of polymer–graphene nanocomposites) and
aid in good interfacial interaction to achieve the desired properties.
However, no cytotoxicity report is available on the effects of the
additives on graphene and its incorporated materials. Here, we report
in vitro cytotoxicity of formulated FLG (FLG-C), i.e., a mixture of
FLG, melamine, and sodium poly(naphthalene sulfonate) (SPS), along
with natural rubber (NR) latex and FLG-C-included NR latex nanocomposite
(FLG-C-NR) thin films on human vaginal epithelial (HVE) cells. FLG-C
shows reduced cellular proliferation (∼55%) only at a longer
exposure time (72 h) even at a low concentration (50 μg/mL).
It also displays significant down- and upregulation in mitochondrial
membrane potential (MMP) and reactive oxygen species (ROS), respectively,
whereas no changes are observed in lactate dehydrogenase (LDH), propidium
iodide (PI), uptake, and cell cycle analysis at 48 h. In vitro experiments
on NR latex and FLG-C-NR latex thin films demonstrate that the incorporation
of FLG-C does not compromise the biocompatibility of the NR latex.
Further substantiation from the in vivo experiments on the thin films
recommends that FLG-C could be suitable to prepare a range of biocompatible
rubber latex nanocomposites-based products, viz., next-generation
condoms (male and female), surgical gloves, catheters, vaginal rings,
bladder–rectum spacer balloon, etc.
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