Abstract

PurposeUterine anomalies are prevalent in women, and the major treatment assisted to them is hysterectomy as donor availability is extremely low. To overcome this, engineering uterine myometrium smooth muscle tissue has become very important. Several studies have shown that polycaprolactone (PCL) nanofibers are very effective in engineering smooth muscles, as this type of scaffold has structural similarities to the extracellular matrices of the cells. Here, we hypothesize that by electrospinning PCL nanofibers, they form a suitable scaffold for uterine tissue engineering.MethodsPolycaprolactone nanofibrous scaffolds were fabricated, and surface modification was performed following two step wet chemistry method. First step is aminolysis which introduces the primary amine groups on the PCL scaffolds following which maltose is conjugated on the scaffolds. This was confirmed by the ninhydrin assay for the presence of amine groups. This was followed by ELLA assay where the presence of maltose on the scaffold was quantified. Modified scaffolds were further characterized by scanning electron microscope (SEM), contact angle analysis and Fourier transform infrared spectroscopy (FTIR). MTT assay, live-dead assay and actin staining were performed on the maltose immobilization to study the improvement of the cell attachment and proliferation rates on the modified scaffolds.ResultsHuman uterine fibroblast (HUF) cells displayed significant proliferation on the maltose-modified PCL scaffolds, and they also exhibited appropriate morphology indicating that these modified fibers are highly suitable for uterine cell growth.ConclusionOur results indicate that the fabricated maltose PCL (MPCL) scaffolds would be a potential biomaterial to treat uterine injuries and promote regeneration.Lay Summary and Future WorkUterine anomalies are prevalent in women, and the major treatment is hysterectomy as donor availability is extremely low. Over the past few years, considerable efforts have been directed towards uterine tissue regeneration. This study is to design a tissue engineered scaffold that could act as a human uterine myometrial patch. We propose to create uterine fibroblast-based synthetic scaffolds that act in a condition similar to the intrauterine microenvironment where the embryos are embedded in the uterine wall. For understanding of the efficiency of the myometrial patch, functional characterization will be performed to study the effects of estrogen and prostaglandins on myometrial activity of the designed patch. Results from these experiments will assist a deeper understanding of how to construct a total bioengineered uterus which can substitute the uterus transplantation procedure, which nonetheless is in its initial stages of development.Graphical

Highlights

  • Uterus is a muscular organ consisting of the fundus, corpus and cervix

  • Fiber morphology and fiber quality, scanning electron microscope (SEM) analysis was done for PCL, aminolysed PCL (APCL) and maltose PCL (MPCL)

  • The results showed that cells plated on PCL aggregated in one place and appeared to be growing on top of the other due to the hydrophobic nature of the scaffold, whereas cells plated on maltose-conjugated PCL were distributed and had intact morphology and better cytoskeletal arrangement than cells plated on other scaffolds

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Summary

Introduction

Uterus is a muscular organ consisting of the fundus, corpus and cervix. Anatomically it is positioned between the urinary bladder anteriorly and rectum posteriorly. The uterine and ovarian arteries supply blood to the uterus; the uterine arteries being the main source of blood supply They branch into arcuate and radial arteries when. Regenerative Engineering and Translational Medicine they enter the myometrium and the endometrium, and they branch into basal and spiral arteries These arteries play an important role in maintaining blood supply during menstrual cycles and pregnancy [1]. The acquired anomalies that a female suffers from are of several kinds. Of these disorders, 13%–50% are polyps, out of which 1.0% turn malignant [2]. It is seen that approximately 80% of women with abnormal uterine conditions suffer from adenomyosis

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