Autologous graft replacement as a strategy to treat diseased peripheral small diameter (≤6 mm) blood vessel is often challenged by prior vein harvesting. To address this issue, we fabricated native-tissue mimicking multilayered small diameter vascular graft (SDVG) using mulberry (Bombyx mori) and Indian endemic non-mulberry (Antheraea assama and Philosamia ricini) silk. Patterned silk films were fabricated on microgrooved PDMS mold, casted by soft lithography. The biodegradable patterned film templates with aligned cell sheets were rolled onto an inert mandrel to mimic vascular conduit. The hemocompatible and mechanically strong non-mulberry films with RGD motif supported ∼1.2 folds greater proliferation of vascular cells with aligned anchorage. Elicitation of minimal immune response on subcutaneous implantation of the films in mice was complemented by ∼45% lower TNF α secretion by in vitro macrophage culture post 7 days. Pattern-induced alignment favored the functional contractile phenotype of smooth muscle cells (SMCs), expressing the signature markers-calponin, α-smooth muscle actin (α-SMA), and smooth muscle myosin heavy chain (SM-MHC). Endothelial cells (ECs) exhibited a typical punctuated pattern of von Willebrand factor (vWF). Deposition of collagen and elastin by the SMCs substantiated the aptness of the graft with desired biomechanical attributes. Furthermore, the burst strength of the fabricated conduit was in the range of ∼915-1260 mmHg, a prerequisite to withstand physiological pressure. This novel fabrication approach may eliminate the need of maturation in a pulsatile bioreactor for obtaining functional cellular phenotype. This work is thereby an attestation to the immense prospects of exploring non-mulberry silk for bioengineering a multilayered vascular conduit similar to a native vessel in "form and function", befitting for in vivo transplantation.
Materials
at the nanoscale offer numerous avenues to be explored
and exploited in diverse realms. Among others, proteinaceous biomaterials
such as silk hold immense prospects in the domain of nanoengineering.
Silk offers a unique combination of desirable facets like biocompatibility;
extraordinary mechanical properties, such as elongation, elasticity,
toughness, and modulus; and tunable biodegradability which are far
better than most naturally occurring and engineered materials. Much
of these properties are due to the molecular structure of the silk
protein and it is self-assembly into hierarchical structures. Taking
advantage of the hierarchical assembly, a large number of fabrication
strategies have now emerged that allow the tailoring of silk structure
of at the nanoscale. Harnessing the favorable properties of silk,
such methods offer a promising direction toward producing structurally
and functionally optimized silk nanomaterials. This review discusses
the critical structure–property relationship in silk that occurs
at the nanoscale and also aims to bring out the recent status in the
approaches for fabrication, characterization, and the gamut of applications
of various silk-based nanomaterials (nanoparticles, nanofibers, and
nanocomposites) in the niche of translational research. Harnessing
the favorable nanostructure of silk, the review also takes into account
the impetus of silk in avant-garde applications such
as chemo-biosensing, energy harvesting, microfluidics, and environmental
applications.
Conventional
systemic chemotherapeutic regimens suffer from challenges
such as nonspecificity, shorter half-life, clearance of drugs, and
dose-limiting toxicity. Localized delivery of chemotherapeutic drugs
through noninvasive spatiotemporally controllable stimuli-responsive
drug delivery systems could overcome these drawbacks while utilizing
drugs approved for cancer treatment. In this regard, we developed
photoelectro active nanocomposite silk-based drug delivery systems
(DDS) exhibiting on-demand drug release in vivo. A functionally modified
single-walled carbon nanotube loaded with doxorubicin (DOX) was embedded
within a cross-linker free silk hydrogel. The resultant nanocomposite
silk hydrogel showed electrical field responsiveness and near-infrared
(NIR) laser-induced hyperthermal effect. The remote application of
these stimuli in tandem or independent manner led to the increased
thermal and electrical conductivity of nanocomposite hydrogel, which
effectively triggered the intermittent on-demand drug release. In
a proof-of-concept in vivo tumor regression study, the nanocomposite
hydrogel was administered in a minimally invasive way at the periphery
of the tumor by covering most of it. During the 21-day study, drastic
tumor regression was recorded upon regular stimulation of nanocomposite
hydrogel with simultaneous or individual external application of an
electric field and NIR laser. Tumor cell death marker expression analysis
uncovered the induction of apoptosis in tumor cells leading to its
shrinkage. Heart ultrasound and histology revealed no cardiotoxicity
associated with localized DOX treatment. To our knowledge, this is
also the first report to show the simultaneous application of electric
field and NIR laser in vivo for localized tumor therapy, and our results
suggested that such strategy might have high clinical translational
potential.
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