Rhodamine B‑Conjugated Fluorescent Block Copolymer
Micelles for Efficient Chlorambucil Delivery and Intracellular Imaging
Posted on 2023-06-14 - 23:33
The clinical development
of the anticancer drug chlorambucil (CHL)
is limited by its low solubility in water, poor bioavailability, and
off-target toxicity. Besides, another constraint for monitoring intracellular
drug delivery is the non-fluorescent nature of CHL. Nanocarriers based
on block copolymers of poly(ethylene glycol)/poly(ethylene oxide)
(PEG/PEO) and poly(ε-caprolactone) (PCL) are an elegant choice
for drug delivery applications due to their high biocompatibility
and inherent biodegradability properties. Here, we have designed and
prepared block copolymer micelles (BCM) containing CHL (BCM-CHL) from
a block copolymer having fluorescent probe rhodamine B (RhB) end-groups
to achieve efficient drug delivery and intracellular imaging. For
this purpose, the previously reported tetraphenylethylene (TPE)-containing
poly(ethylene oxide)-b-poly(ε-caprolactone)
[TPE-(PEO-b-PCL)2] triblock copolymer
was conjugated with RhB by a feasible and effective post-polymerization
modification method. In addition, the block copolymer was obtained
by a facile and efficient synthetic strategy of one-pot block copolymerization.
The amphiphilicity of the resulting block copolymer TPE-(PEO-b-PCL-RhB)2 led to the spontaneous formation
of micelles (BCM) in aqueous media and successful encapsulation of
the hydrophobic anticancer drug CHL (CHL-BCM). Dynamic light scattering
and transmission electron microscopy analyses of BCM and CHL-BCM revealed
a favorable size (10–100 nm) for passive targeting of tumor
tissues via the enhanced permeability and retention
effect. The fluorescence emission spectrum (λex 315
nm) of BCM demonstrated Förster resonance energy transfer between
TPE aggregates (donor) and RhB (acceptor). On the other hand, CHL-BCM
revealed TPE monomer emission, which may be attributed to the π–π
stacking interaction between TPE and CHL molecules. The in
vitro drug release profile showed that CHL-BCM exhibits drug
release in a sustained manner over 48 h. A cytotoxicity study proved
the biocompatibility of BCM, while CHL-BCM revealed significant toxicity
to cervical (HeLa) cancer cells. The inherent fluorescence of RhB
in the block copolymer offered an opportunity to directly monitor
the cellular uptake of the micelles by confocal laser scanning microscopy
imaging. These results demonstrate the potential of these block copolymers
as drug nanocarriers and as bioimaging probes for theranostic applications.
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Kulkarni, Bhagyashree; Qutub, Somayah; Khashab, Niveen M.; Hadjichristidis, Nikos (1753). Rhodamine B‑Conjugated Fluorescent Block Copolymer
Micelles for Efficient Chlorambucil Delivery and Intracellular Imaging. ACS Publications. Collection. https://doi.org/10.1021/acsomega.3c01514