Nanoengineered Bifidobacterium bifidum with Optical Activity for Photothermal Cancer Immunotheranostics.

There is substantial interest regarding the understanding and designing of nanoengineered bacteria to combat various fatal diseases. Here, we report the nanoengineering of Bifidobacterium bifidum using Cremophor EL to encapsulate organic dye molecules by simple incubation and washing processes while maintaining the bacterial morphology and viability. The prepared functional bacteria exhibit characteristics such as optical absorbance, unique fluorescence, powerful photothermal conversion, low toxicity, excellent tumor targeting, and anticancer efficacy. They also displayed significant in vivo fluorescent expression in implanted colorectal cancerous tumors. Moreover, the powerful photothermal conversion of the functional bacteria could be spatiotemporally evoked by biologically penetrable near-infrared laser for effective tumor regression in mice, with the help of immunological responses. Our study demonstrates that a nanoengineering approach can provide the strong physicochemical traits and attenuation of living bacterial cells for cancer immunotheranostics.

Rational Chemical Multifunctionalization of Graphene Interface Enhances Targeted Cancer Therapy.

The synthesis of a drug delivery platform based on graphene was achieved through a step-by-step strategy of selective amine deprotection and functionalization. The multifunctional graphene platform, functionalized with indocyanine green, folic acid, and doxorubicin showed an enhanced anticancer activity. The remarkable targeting capacity for cancer cells in combination with the synergistic effect of drug release and photothermal properties prove the great advantage of a combined chemo- and phototherapy based on graphene against cancer, opening the doors to future therapeutic applications of this type of material.

Species-Specific Biodegradation of Sporopollenin-Based Microcapsules.

Sporoderms, the outer layers of plant spores and pollen grains, are some of the most robust biomaterials in nature. In order to evaluate the potential of sporoderms in biomedical applications, we studied the biodegradation in simulated gastrointestinal fluid of sporoderm microcapsules (SDMCs) derived from four different plant species: lycopodium (Lycopodium clavatum L.), camellia (Camellia sinensis L.), cattail (Typha angustifolia L.), and dandelion (Taraxacum officinale L.). Dynamic image particle analysis (DIPA) and field-emission scanning electron microscopy (FE-SEM) were used to investigate the morphological characteristics of the capsules, and Fourier-transform infrared (FTIR) spectroscopy was used to evaluate their chemical properties. We found that SDMCs undergo bulk degradation in a species-dependent manner, with camellia SDMCs undergoing the most extensive degradation, and dandelion and lycopodium SDMCs being the most robust.

Multifunctional Cancer Phototherapy Using Fluorophore-Functionalized Nanodiamond Supraparticles.

In this study, the preparation and characterization of self-assembled supraparticles (SPs) comprising fluorophore-conjugated nanodiamond (ND) nanoclusters are described. The SPs are further used in photohyperthermic, photodynamic, and chemotherapeutic multifunctional tumor therapy systems that use bio-optical-window near-infrared lasers. NDs with surface amino groups are conjugated with various fluorophores via carbodiimide chemistry and are spontaneously transformed into self-assembled ND-based SP (ND-SP) nanoclusters. The fluorophore-functionalized ND-SPs exhibit a uniform particle size, high dispersity in water, and low cytotoxicity. In addition, the energy or electron transfer between fluorophores and NDs can enhance the photothermal conversion efficiency. Further, it is demonstrated that the synthesized ND-SPs strongly fluoresce and penetrate the cellular transmembrane, making them attractive for the targeted delivery of conventional nanomedicines such as albumin-bound paclitaxel (Abraxane) and simple drug-loaded ND conjugates. The near-infrared-light-driven efficiency of the fluorophore-functionalized ND-SPs encapsulating anticancer drugs is confirmed by the targeted eradication of cancer cells both in vitro and in vivo. Thus, the fluorophore-functionalized ND-SP nanoclusters may be proven to be a valuable new therapeutic agent for use in cancer treatment.

Withaferin-A kills cancer cells with and without telomerase: chemical, computational and experimental evidences.

Maintenance of telomere length is the most consistent attribute of cancer cells. Tightly connected to their capacity to overcome replicative mortality, it is achieved either by activation of telomerase or an Alternative mechanism of Lengthening of Telomeres (ALT). Disruption of either of these mechanisms has been shown to induce DNA damage signalling leading to senescence or apoptosis. Telomerase inhibitors are considered as potential anticancer drugs but are ineffective for ALT cancers (~15% of all cancers). Withaferin-A (Wi-A), a major constituent of the medicinal plant, Withania somnifera (Ashwagandha), has been shown to exert anti-tumour activity. However, its effect on either telomerase or ALT mechanisms has not been investigated. Here, by using isogenic cancer cells with/without telomerase, we found that Wi-A caused stronger cytotoxicity to ALT cells. It was associated with inhibition of ALT-associated promyelocytic leukemia nuclear bodies, an established marker of ALT. Comparative analyses of telomerase positive and ALT cells revealed that Wi-A caused stronger telomere dysfunction and upregulation of DNA damage response in ALT cells. Molecular computational and experimental analyses revealed that Wi-A led to Myc-Mad mediated transcriptional suppression of NBS-1, an MRN complex protein that is an essential component of the ALT mechanism. The results suggest that Wi-A could be a new candidate drug for ALT cancers.