Your search keyword '"Donor cells"' showing total 29 results

1. Proliferation ability of particulated juvenile allograft cartilage

Author

Changgui Zhang, Xingyu Zhao, Yunong Ao, Jin Cao, Liu Yang, and Xiaojun Duan

Subjects

Particulated juvenile allograft cartilage, Autologous cartilage chip transplantation, Donor cells, Ki-67, Lin28, Proliferation, Orthopedic surgery, RD701-811, Diseases of the musculoskeletal system, RC925-935

Abstract

Abstract Background Particulated juvenile allograft cartilage (PJAC) has a good short-term clinical efficacy in repairing articular cartilage defects, but the proliferation ability of PJAC and the biological characteristics of transplanted cells after transplantation are still unclear. Purpose To study the cartilage proliferation ability of PJAC in repairing full-thickness cartilage defects and the reasons for proliferation to provide experimental evidence for its clinical application. Study design Controlled laboratory study. Methods Twenty Guizhou minipigs were randomly divided into the experimental group and control group. In all minipigs, an 8-mm cylindrical full-thickness cartilage defect was created in the femoral trochlea of one knee. The experimental group received PJAC transplantation from five juvenile donors of Guizhou minipigs (PJAC group; n = 10) and the control group received transplantation of autologous cartilage chips (ACC group; n = 10). Both groups were followed at 1 and 3 months after surgery, immunohistochemical evaluation of the tissue sections Ki-67 and Lin28 was conducted, the positive rate was calculated according to the staining, and the proliferation ability of PJAC was analyzed. Results All 20 Guizhou minipigs were followed, and there was no infection or incision healing disorder after surgery. By Ki-67 and Lin28 immunohistochemical tests, the positive rate of Ki-67 was 88.9 ± 0.2% in the PJAC group and 28.3 ± 3.6% in the ACC group at 1 month, and the difference was statistically significant (P

Published

2021

2. Locus-specific analysis of DNA methylation patterns in cloned and in vitro fertilized porcine embryos

Author

Weihua XU, Hongyi LI, Mao ZHANG, Junsong SHI, and Zhengchao WANG

Subjects

cloned embryos, dna methylation, donor cells, in vitro fertilized embryos, porcine, Reproduction, QH471-489, Internal medicine, RC31-1245

Abstract

Porcine somatic cell nuclear transfer (SCNT) is currently inefficient, as 1–3.95% of reconstructed embryos survive to term; inadequate or erroneous epigenetic reprogramming of the specialized donor somatic nucleus could be a primary reason. Therefore, a locus-specific analysis of DNA methylation dynamics in embryogenesis and the DNA methylation status of gametes and donor cells used for SCNT were conducted in the following developmentally important gene loci: POU5F1, NANOG, SOX2, H19, IGF2, IGF2R, XIST; and the retrotransposon LINE-1. There were significant epigenetic differences between the gametes and the somatic donor cells. Three gamete-specific differentially methylated regions (DMRs) in POU5F1, XIST, and LINE-1 were identified. A delayed demethylation process at POU5F1 and LINE-1 loci occurred after three successive cleavages, compared to the in vitro fertilized (IVF) embryos. Although cloned embryos could undergo de-methylation and re-methylation dynamics at the DMRs of imprinted genes (H19, IGF2R, and XIST), the re-methylation process was compromised, unlike in fertilized embryos. LINE-1 loci are widely dispersed across the whole genome, and LINE-1 DMR might be a potential porcine nuclear reprogramming epi-marker. Data from observations in our present and previous studies, and two published articles were pooled to produce a schematic diagram of locus-specific, DNA methylation dynamics of cloned and IVF embryos during porcine early embryogenesis. This also indicated aberrant DNA methylation reprogramming events, including inadequate DNA demethylation and insufficient re-methylation in cloned embryos. Further research should focus on mechanisms underlying demethylation during the early cleavage of embryos and de novo DNA methylation at the blastocyst stage.

Published

2020

3. Combined refinements to somatic cell nuclear transfer methods improve porcine embryo development

Author

Thanh Quang DANG-NGUYEN, David WELLS, Seiki HARAGUCHI, Nguyen Thi MEN, Hiep Thi NGUYEN, Junko NOGUCHI, Hiroyuki KANEKO, and Kazuhiro KIKUCHI

Subjects

donor cells, embryonic development competence, pigs, somatic cell nuclear transfer, Reproduction, QH471-489, Internal medicine, RC31-1245

Abstract

The discovery of how to utilize CRISPR (clustered, regularly interspaced, short, palindromic repeats)-Cas (CRISPR-associated) systems for genome modification has accelerated development of the field of genome editing, especially in large animals such as pigs. The low efficiency of somatic cell nuclear transfer (SCNT) is now becoming a major obstacle in the production of genome-edited animals via cell-mediated approaches and improving efficacy of this technique is crucial. In this study, we propose a few simple modifications to a zona-free SCNT protocol that are effective to produce numerous high-quality blastocysts. To refine the SCNT protocol we modified the following steps/factors: 1) culture medium for SCNT embryos, 2) chemical treatment to prevent precocious activation of the manipulated/reconstructed oocytes and 3) donor cell serum starvation treatment. Although changes in each of these steps only resulted in small improvements, the combination of all modifications altogether significantly enhanced developmental competence of SCNT embryos. Our modified method yielded approximately three times greater blastocyst formation rates. Moreover, resulting blastocysts had roughly twice as many cells as compared to blastocysts produced by the conventional SCNT method. With these significant in vitro improvements, our refined SCNT method is potentially suited for use in the production of genome edited pigs.

Published

2020

4. Technical, Biological and Molecular Aspects of Somatic Cell Nuclear Transfer – A Review.

Author

Mrowiec, Patrycja and Bugno-Poniewierska, Monika

Subjects

*SOMATIC cell nuclear transfer, *ANIMAL cloning, *ANIMAL rescue, *CELL nuclei, *SOMATIC cells

Abstract

Since the announcement of the birth of the first cloned mammal in 1997, Dolly the sheep, 24 animal species including laboratory, farm, and wild animals have been cloned. The technique for somatic cloning involves transfer of the donor nucleus of a somatic cell into an enucleated oocyte at the metaphase II (MII) stage for the generation of a new individual, genetically identical to the somatic cell donor. There is increasing interest in animal cloning for different purposes such as rescue of endangered animals, replication of superior farm animals, production of genetically engineered animals, creation of biomedical models, and basic research. However, the efficiency of cloning remains relatively low. High abortion, embryonic, and fetal mortality rates are frequently observed. Moreover, aberrant developmental patterns during or after birth are reported. Researchers attribute these abnormal phenotypes mainly to incomplete nuclear remodeling, resulting in incomplete reprogramming. Nevertheless, multiple factors influence the success of each step of the somatic cloning process. Various strategies have been used to improve the efficiency of nuclear transfer and most of the phenotypically normal born clones can survive, grow, and reproduce. This paper will present some technical, biological, and molecular aspects of somatic cloning, along with remarkable achievements and current improvements. [ABSTRACT FROM AUTHOR]

Published

2022

5. Proliferation ability of particulated juvenile allograft cartilage.

Author

Zhang, Changgui, Zhao, Xingyu, Ao, Yunong, Cao, Jin, Yang, Liu, and Duan, Xiaojun

Subjects

CELL proliferation, ANIMAL experimentation, ARTICULAR cartilage, BIOLOGICAL models, CARTILAGE diseases, TISSUE fixation (Histology), HOMOGRAFTS, IMMUNOHISTOCHEMISTRY, SWINE, TUMOR markers, DESCRIPTIVE statistics

Abstract

Background: Particulated juvenile allograft cartilage (PJAC) has a good short-term clinical efficacy in repairing articular cartilage defects, but the proliferation ability of PJAC and the biological characteristics of transplanted cells after transplantation are still unclear. Purpose: To study the cartilage proliferation ability of PJAC in repairing full-thickness cartilage defects and the reasons for proliferation to provide experimental evidence for its clinical application. Study design: Controlled laboratory study. Methods: Twenty Guizhou minipigs were randomly divided into the experimental group and control group. In all minipigs, an 8-mm cylindrical full-thickness cartilage defect was created in the femoral trochlea of one knee. The experimental group received PJAC transplantation from five juvenile donors of Guizhou minipigs (PJAC group; n = 10) and the control group received transplantation of autologous cartilage chips (ACC group; n = 10). Both groups were followed at 1 and 3 months after surgery, immunohistochemical evaluation of the tissue sections Ki-67 and Lin28 was conducted, the positive rate was calculated according to the staining, and the proliferation ability of PJAC was analyzed. Results: All 20 Guizhou minipigs were followed, and there was no infection or incision healing disorder after surgery. By Ki-67 and Lin28 immunohistochemical tests, the positive rate of Ki-67 was 88.9 ± 0.2% in the PJAC group and 28.3 ± 3.6% in the ACC group at 1 month, and the difference was statistically significant (P < 0.05); the positive rate of Lin28 was 34.6 ± 3.3% in the PJAC group and 7.6 ± 1.4% in the ACC group at 1 month, and the difference was statistically significant (P < 0.05). At 3 months, the positive rates of Ki-67 in the PJAC group and ACC group were 53.6 ± 6.9% and 1.97 ± 0.3%, respectively (P < 0.05); the positive rates of Lin28 were 86.6 ± 3.3% and 1.4 ± 0.3%, respectively (P < 0.01). Conclusion: A large animal model was established with Guizhou minipigs, and the expressions of Ki-67 protein and Lin28 protein detected by immunohistochemistry in the repaired transplanted tissue of the PJAC group were stronger than those of adult cartilage. The proliferation of PJAC within 3 months of transplantation was stronger than that of adult cartilage. The enhanced expression of Lin28 may be one of the mechanisms by which PJAC achieved stronger proliferation ability than adult cartilage. PJAC technology has shown good application prospects for repairing cartilage defects. [ABSTRACT FROM AUTHOR]

Published

2021

6. Donor Cell Fate in Particulated Juvenile Allograft Cartilage for the Repair of Articular Cartilage Defects.

Author

Zhang, Changgui, Ao, Yunong, Cao, Jin, Yang, Liu, and Duan, Xiaojun

Subjects

*CARTILAGE transplantation, *ANIMAL experimentation, *ANIMALS, *ARTICULAR cartilage, *CULTURE, *HOMOGRAFTS, *IN situ hybridization, *SWINE, *DESCRIPTIVE statistics, *IN vitro studies

Abstract

Background: Particulated juvenile allograft cartilage (PJAC) has demonstrated good clinical efficacy in repairing articular cartilage defects, but the related repair mechanism after transplant and the biological characteristics of the transplanted cells are still unclear. Purpose: To study the efficacy of PJAC in repairing full-thickness cartilage defects and the specific fate of donor cells to provide experimental evidence for its clinical application. Study Design: Controlled laboratory study. Methods: Twenty female Guizhou minipigs were randomly divided into an experimental group and a control group. An 8-mm cylindrical full-thickness cartilage defect was created in the femoral trochlea of 1 knee in all minipigs. The experimental group received transplant of PJAC from 5 male juvenile Guizhou minipigs (PJAC group; n = 10) and the control group received autologous cartilage chips (ACC group; n = 10). Follow-up assessments were conducted at 1 month and 3 months to track the transplanted cells by the male-specific sex-determining region Y-linked (SRY) gene; tissue sections were hybridized in situ, and O'Driscoll histological scoring was performed according to hematoxylin and eosin staining, safranin O and fast green staining, and toluidine blue O staining, as well as immunohistochemical evaluation of aggrecan and Sry-type HMG-box 9 (SOX9). Results: All 20 Guizhou minipigs were followed; no infection or incision healing disorder occurred after the operation. By SRY in situ hybridization, the SRY signal of the transplanted cells was positive in the repaired tissue of the defect, and the SRY positive signal could still be detected in repaired tissue at 3 months postoperatively. The average number of positive cells was 68.6 ± 11.91 at 1 month and 32.6 ± 3.03 at 3 months (confocal microscope: ×400), and the difference was statistically significant. The O'Driscoll histological scores were 14 ± 0.71 in the ACC group and 9.8 ± 0.84 in the PJAC group at 1 month, and 18 ± 1.20 in the ACC group and 17.4 ± 1.14 in the PJAC group at 3 months. The scores were statistically significant between the ACC group and PJAC group at 1 month. The positive rates of SOX9 in the PJAC and ACC groups at 1 month were 67.6% ± 3.78% and 63.4% ± 5.30%, respectively, and the difference was not statistically significant (P >.05). The positive rates of SOX9 in the PJAC and ACC groups at 3 months were 68.8% ± 2.69% and 17.1% ± 1.26%, respectively, and the difference was statistically significant (P <.05). The positive rates of aggrecan in the PJAC and ACC groups at 1 month were 40.5% ± 2.78% and 42.4% ± 0.54% respectively, and the difference was not statistically significant (P >.05). The positive rates of aggrecan in the PJAC and ACC groups at 3 months were 40.8% ± 1.50% and 30.1% ± 2.44%, respectively, and the difference was not statistically significant (P >.05). Conclusion: An animal model was established with Guizhou minipigs, and the cartilage defect was repaired with PJAC from male minipigs. The SRY gene positive signal could be detected from the repaired tissue by in situ hybridization, indicating that the transplanted cells survived at least 3 months. The key genes of cartilage formation, SOX9 and aggrecan, were expressed at 1 month and 3 months, and SOX9 expression was stronger in the PJAC group than the ACC group at 3 months. Clinical Relevance: This study suggests that it is feasible to study the biological characteristics of transplanted cells in the cartilage region by the sex-determining gene. [ABSTRACT FROM AUTHOR]

Published

2020

7. Influences of somatic donor cell sex on and embryo development following somatic cell nuclear transfer in pigs

Author

Jae-Gyu Yoo, Byeong-Woo Kim, Mi-Rung Park, Deug-Nam Kwon, Yun-Jung Choi, Teak-Soon Shin, Byung-Wook Cho, Jakyeom Seo, Jin-Hoi Kim, and Seong-Keun Cho

Subjects

Somatic Cell Nuclear Transfer, Pigs, Donor Cells, Sex, Animal culture, SF1-1100, Animal biochemistry, QP501-801

Abstract

Objective The present study investigates pre- and post-implantation developmental competence of nuclear-transferred porcine embryos derived from male and female fetal fibroblasts. Methods Male and female fetal fibroblasts were transferred to in vitro-matured enucleated oocytes and in vitro and in vivo developmental competence of reconstructed embryos was investigated. And, a total of 6,789 female fibroblast nuclear-transferred embryos were surgically transferred into 41 surrogate gilts and 4,746 male fibroblast nuclear-transferred embryos were surgically transferred into 25 surrogate gilts. Results The competence to develop into blastocysts was not significantly different between the sexes. The mean cell number of female and male cloned blastocysts obtained by in vivo culture (143.8±10.5 to 159.2±14.8) was higher than that of in vitro culture of somatic cell nuclear transfer (SCNT) groups (31.4±8.3 to 33.4±11.1). After embryo transfer, 5 pregnant gilts from each treatment delivered 15 female and 22 male piglets. The average birth weight of the cloned piglets, gestation length, and the postnatal survival rates were not significantly different (p

Published

2017

8. Production of Transgenic Porcine Embryos Reconstructed with Induced Pluripotent Stem-Like Cells Derived from Porcine Endogenous Factors Using piggyBac System.

Author

Kim, Su-Jin, Kwon, Hee-Sun, Kwon, Dae-kee, Koo, Ok-Jae, Moon, Joon-Ho, Park, Eun-Jung, Yum, Soo-Young, Lee, Byeong-Chun, and Jang, Goo

Subjects

*PLURIPOTENT stem cells, *STEM cells, *GENE expression, *T cells, *CANCER cells

Abstract

The potential of induced pluripotent stem (iPS) cells, which have self-renewal ability and can differentiate into three germ layers, led us to hypothesize that iPS cells in pigs can be useful and suitable source for producing transgenic pigs. In this study, we generated iPS-like cells using doxycycline-inducible piggyBac (PB) expression vectors encoding porcine 4 transcription factors. After transfection, transfected cells were cultured until the formation of outgrowing colonies taking least of 7–10 days. The iPS-like cells demonstrated pluripotent characteristics such as self-renewal, high proliferation, expression of pluripotent markers, and aggregation ability. The embryo development through somatic cell nuclear transfer (SCNT), cleavage rate, and blastocyst formation rate did not show any significant differences. However, the total cell number of blastocysts was significantly increased with the established cell line. In conclusion, the iPS-like cell line, generated from porcine transcriptional factors using the PB transposon system, demonstrated pluripotency with the capacity for unlimited self-renewal, and could be used as donor cells to produce cloned embryos by SCNT. These cells will be suitable for gene modification and would contribute to the stability or safety of pig models in biomedical research. [ABSTRACT FROM AUTHOR]

Published

2019

9. Influences of somatic donor cell sex on in vitro and in vivo embryo development following somatic cell nuclear transfer in pigs.

Author

Jae-Gyu Yoo, Byeong-Woo Kim, Mi-Rung Park, Deug-Nam Kwon, Yun-Jung Choi, Teak-Soon Shin, Byung-Wook Cho, Jakyeom Seo, Jin-Hoi Kim, and Seong-Keun Cho

Subjects

SWINE embryos, SOMATIC cell nuclear transfer, FIBROBLASTS, EMBRYO transfer, POSTNATAL care

Abstract

Objective: The present study investigates pre- and post-implantation developmental competence of nuclear-transferred porcine embryos derived from male and female fetal fibroblasts. Methods: Male and female fetal fibroblasts were transferred to in vitro-matured enucleated oocytes and in vitro and in vivo developmental competence of reconstructed embryos was investigated. And, a total of 6,789 female fibroblast nuclear-transferred embryos were surgically transferred into 41 surrogate gilts and 4,746 male fibroblast nuclear-transferred embryos were surgically transferred into 25 surrogate gilts. Results: The competence to develop into blastocysts was not significantly different between the sexes. The mean cell number of female and male cloned blastocysts obtained by in vivo culture (143.8±10.5 to 159.2±14.8) was higher than that of in vitro culture of somatic cell nuclear transfer (SCNT) groups (31.4±8.3 to 33.4±11.1). After embryo transfer, 5 pregnant gilts from each treatment delivered 15 female and 22 male piglets. The average birth weight of the cloned piglets, gestation length, and the postnatal survival rates were not significantly different (p<0.05) between sexes. Conclusion: The present study found that the sex difference of the nuclear donor does not affect the developmental rate of porcine SCNT embryos. Furthermore, postnatal survivability of the cloned piglets was not affected by the sex of the donor cell. [ABSTRACT FROM AUTHOR]

Published

2017

10. Locus-specific analysis of DNA methylation patterns in cloned and in vitro fertilized porcine embryos

Author

XU, Weihua, LI, Hongyi, ZHANG, Mao, SHI, Junsong, and WANG, Zhengchao

Subjects

Male, Nuclear Transfer Techniques, Retroelements, Porcine, Swine, Fertilization in Vitro, In Vitro Techniques, Epigenesis, Genetic, Donor cells, Animals, In vitro fertilized embryos, DNA methylation, Genome, Fibroblasts, Cellular Reprogramming, Embryo Transfer, Spermatozoa, Cloned embryos, Blastocyst, Long Interspersed Nucleotide Elements, embryonic structures, Oocytes, Original Article, Female, RNA, Long Noncoding, Octamer Transcription Factor-3

Abstract

Porcine somatic cell nuclear transfer (SCNT) is currently inefficient, as 1-3.95% of reconstructed embryos survive to term; inadequate or erroneous epigenetic reprogramming of the specialized donor somatic nucleus could be a primary reason. Therefore, a locus-specific analysis of DNA methylation dynamics in embryogenesis and the DNA methylation status of gametes and donor cells used for SCNT were conducted in the following developmentally important gene loci: POU5F1, NANOG, SOX2, H19, IGF2, IGF2R, XIST; and the retrotransposon LINE-1. There were significant epigenetic differences between the gametes and the somatic donor cells. Three gamete-specific differentially methylated regions (DMRs) in POU5F1, XIST, and LINE-1 were identified. A delayed demethylation process at POU5F1 and LINE-1 loci occurred after three successive cleavages, compared to the in vitro fertilized (IVF) embryos. Although cloned embryos could undergo de-methylation and re-methylation dynamics at the DMRs of imprinted genes (H19, IGF2R, and XIST), the re-methylation process was compromised, unlike in fertilized embryos. LINE-1 loci are widely dispersed across the whole genome, and LINE-1 DMR might be a potential porcine nuclear reprogramming epi-marker. Data from observations in our present and previous studies, and two published articles were pooled to produce a schematic diagram of locus-specific, DNA methylation dynamics of cloned and IVF embryos during porcine early embryogenesis. This also indicated aberrant DNA methylation reprogramming events, including inadequate DNA demethylation and insufficient re-methylation in cloned embryos. Further research should focus on mechanisms underlying demethylation during the early cleavage of embryos and de novo DNA methylation at the blastocyst stage.

Published

2020

11. Cardiac Allograft Vasculopathy: A Donor or Recipient Induced Pathology?

Author

Hoogen, Patricia, Huibers, Manon, Sluijter, Joost, and Weger, Roel

Abstract

Cardiac allograft vasculopathy (CAV) is one of the main causes of late-stage heart failure after heart transplantation. CAV is characterized by concentric luminal narrowing of the coronary arteries, but the exact pathogenesis of CAV is still not unraveled. Many researchers show evidence of an allogeneic immune response of the recipient, whereas others show contrasting results in which donor-derived cells induce an immune response against the graft. In addition, fibrosis of the neo-intima can be induced by recipient-derived circulating cells or donor-derived cells. In this review, both donor and recipient sides of the story are described to obtain better insight in the pathogenesis of CAV. Dual outcomes were found regarding the contribution of donor and recipient cells in the initiation of the immune response and the development of fibrosis during CAV. Future research could focus more on the potential synergistic interaction of donor and recipient cells leading to CAV. [ABSTRACT FROM AUTHOR]

Published

2015

12. In vitro development of porcine transgenic nuclear-transferred embryos derived from newborn Guangxi Bama mini-pig kidney fibroblasts.

Author

Liu, Hongbo, Lv, Peiru, Zhu, Xiangxing, Wang, Xianwei, Yang, Xiaogan, Zuo, Erwei, Lu, Yangqing, Lu, Shengsheng, and Lu, Kehuan

Abstract

Porcine transgenic cloning has potential applications for improving production traits and for biomedical research purposes. To produce a transgenic clone, kidney fibroblasts from a newborn Guangxi Bama mini-pig were isolated, cultured, and then transfected with red and green fluorescent protein genes using lipofectamine for nuclear transfer. The results of the present study show that the kidney fibroblasts exhibited excellent proliferative capacity and clone-like morphology, and were adequate for generation of somatic cell nuclear transfer (SCNT)-derived embryos, which was confirmed by their cleavage activity and blastocyst formation rate of 70.3% and 7.9%, respectively. Cells transfected with red fluorescent protein genes could be passed more than 35 times. Transgenic embryos cloned with fluorescent or blind enucleation methods were not significantly different with respect to cleavage rates (92.5% vs. 86.8%, p > 0.05) and blastocyst-morula rates (26.9% vs. 34.0%, p > 0.05), but were significantly different with respect to blastocyst rates (3.0% vs. 13.2%, p < 0.05). Cleavage (75.3%, 78.5% vs. 78.0%, p > 0.05), blastocyst (14.1%, 16.1% vs. 23.1%, p > 0.05) and morula/blastocyst rates (43.5%, 47.0% vs. 57.6%, p > 0.05) were not significantly different between the groups of transgenic cloned embryos, cloned embryos, and parthenogenetic embryos. This indicates that long-time screening by G418 caused no significant damage to kidney fibroblasts. Thus, kidney fibroblasts represent a promising new source for transgenic SCNT, and this work lays the foundation for the production of genetically transformed cloned Guangxi Bama mini-pigs. [ABSTRACT FROM AUTHOR]

Published

2014

13. Comparative analysis of various donor cell types for somatic cell nuclear transfer and its association with apoptosis and senescence.

Author

EUNHYE KIM and SANG-HWAN HYUN

Subjects

*COMPARATIVE studies, *SOMATIC cells, *TRANSPLANTATION of cell nuclei, *APOPTOSIS, *AGING, *MESSENGER RNA

Abstract

The aim of the present study was to characterize potential somatic cell nuclear transfer (SCNT) donor cells by comparing two lines of transfected cells with their non-modified parental controls in culture. Fetal fibroblasts used in the study originated from crossbred Landrace x Yorkshire x Duroc (LYD) or Yucatan mini-pigs. The LYD fibroblasts were modified by the transfection of a tetracycline on/off gene, whereas Yucatan fibroblasts were triple transfected with the complement regulatory factors, human decay-accelerating factor and human CD59, as well as H-transferase. At the 9th doubling passage, parameters associated with senescence and apoptosis, including morphology, mRNA expression (TP53, Bcl-2, Bax) and reactive oxygen species (ROS) levels, were evaluated. Population doubling (PD) time was calculated by assessing the time required for cell numbers to double by averaging the three cell passages. Quantitative polymerase chain reaction revealed that when comparing LYD with Yucatan fibroblasts, the latter exhibited a lower relative expression of TP53 and a higher relative expression of antiproliferative Bcl-2, which correlated with the PD time results (26 and 40 h, respectively). Tetracycline on/off transfected cell lines exhibited a lower relative expression of antiapoptotic Bcl-2 compared with their originating LYD cells. Similarly, triple transgenic cells exhibited higher TP53 and Bax mRNA expression levels than their non-transgenic counterparts. For ROS measurement, cells were incubated with 2',7'-dichlorofluorescin diacetate under the same conditions and were analyzed by flow cytometry. Yucatan fibroblasts exhibited higher ROS content than LYD cells. In addition, the two transgenic cell lines produced higher ROS levels than their corresponding non-transfected cell lines. In conclusion, these results indicate that characteristics associated with senescence and apoptosis in transfected cells during culture may affect the efficiency of SCNT when used as donor cells for the production of transgenic swine. [ABSTRACT FROM AUTHOR]

Published

2014

14. Construction of Ipr1 expression vector and development of cloned embryos in vitro.

Author

Song, Yongli, He, Xiaoning, Hua, Song, Lan, Jie, Liu, Yonggang, Cheng, Pang, Zhang, Hailin, Li, Jixia, He, Xiaoying, Liu, Jun, and Zhang, Yong

Abstract

The purpose of this study was to prepare intracellular pathogen resistance 1 (Ipr1) transgenic donor cells for somatic cell nuclear transfer (SCNT). Based on our current understanding of Ipr1, a macrophage special expression vector pSP–EGFP–Ipr1was constructed. Bovine fetal fibroblasts were transfected with pSP-EGFP-Ipr1. The green fluorescent protein (GFP)-expressing cells were selected and transferred into enucleated bovine oocytes. Then, the rates of oocyte cleavage and blastocyst formation of transgenic cells and non-transgenic cells were observed, respectively. The results showed that reconstructed embryos derived from transgenic cells could successfully develop into blastocysts, most of which were GFP-positive. This study may provide cloned embryos for the production of anti-tuberculosis transgenic animals. [ABSTRACT FROM PUBLISHER]

Published

2013

15. Differentiation of Oligodendrocytes from Mouse Induced Pluripotent Stem Cells Without Serum.

Author

Misumi, Sachiyo, Nishigaki, Ruriko, Ueda, Yoshitomo, Watanabe, Yoko, Shimizu, Yuko, Ishida, Akimasa, Jung, ChaGyun, and Hida, Hideki

Abstract

Cell therapy using induced pluripotent stem (iPS) cells might become a new approach for treating neonatal hypoxic-ischemic injury such as periventricular leukomalacia. To obtain appropriate donor cells for transplantation, we differentiated oligodendrocyte (OL) lineage cells from mouse iPS cells. Induction of OL lineage cell differentiation from iPS cells was carried out with a seven-step culture method. Mouse iPS cells (stage 1) were induced to form embryoid bodies for 4 days under a serum-free condition that was suitable for ectoderm induction (stage 2), following by selection of nestin-positive neural stem cells (NSCs) for 10-12 days (stage 3). NSCs were cultured in expansion medium containing fibroblast growth factor (FGF)-2 for 4 days (stage 4), induced to differentiate into glial progenitor cells by epidermal growth factor and fibroblast growth factor (FGF-2) treatment for 4-5 days (stage 5), and then into OL progenitor cells by culture in neurobasal A medium containing FGF-2 and platelet-derived growth factor for 6-8 days (stage 6). Terminal differentiation into O4-positive OLs was carried out by culture in neurobasal A containing T3 and ciliary neurotrophic factor for 7 days (stage 7). Inwardly rectifying K currents, which are characteristic of OLs, were detected in iPS cell-derived cells at stage 7 in whole cell clamp mode. Our data suggest that OLs can be effectively differentiated from mouse iPS cells without serum in a stepwise manner, which may be appropriate for use as donor cells in transplantation. [ABSTRACT FROM AUTHOR]

Published

2013

16. Generation of human lactoferrin transgenic cloned goats using donor cells with dual markers and a modified selection procedure

Author

An, Li-You, Yuan, Yu-Guo, Yu, Bao-Li, Yang, Ting-Jia, and Cheng, Yong

Subjects

*TRANSGENIC animals, *ANIMAL breeding, *GOATS, *LACTOFERRIN, *CLONING, *SOMATIC cells, *TRANSPLANTATION of cell nuclei

Abstract

Abstract: The objective was to use dual markers to accurately select genetically modified donor cells and ensure that the resulting somatic cell nuclear transfer kids born were transgenic. Fetal fibroblast cells were transfected with dual marking gene vector (pCNLF-ng) that contained the red-shifted variant of the jellyfish green fluorescent protein (LGFP) and neomycin resistance (Neo) markers. Cell clones that were G418-resistant and polymerase chain reaction-positive were subcultured for several passages; individual cells of the clones were examined with fluorescence microscopy to confirm transgenic integration. Clones in which every cell had bright green fluorescence were used as donor cells for nuclear transfer. In total, 86.7% (26/30) cell clones were confirmed to have transgenic integration of the markers by polymerase chain reaction, 76.7% (23/30) exhibited fluorescence, but only 40% (12/30) of these fluorescent cell clones had fluorescence in all cell populations. Moreover, through several cell passages, only 20% (6/30) of the cell clones exhibited stable LGFP expression. Seven transgenic cloned offspring were produced from these cells by nuclear transfer. Overall, the reconstructed embryo fusion rate was 76.6%, pregnancy rates at 35 and 60 days were 39.1% and 21.7%, respectively, and the offspring birth rate was 1.4%. There were no significant differences between nuclear transfer with dual versus a single (Neo) marker (overall, 73.8% embryo fusion rate, 53.8% and 26.9% pregnancy rates, and 1.9% birth rate with five offspring). In conclusion, the use of LGFP/Neo dual markers and an optimized selection procedure reliably screened genetically modified donor cells, excluded pseudotransgenic cells, and led to production of human lactoferrin transgenic goats. Furthermore, the LGFP/Neo markers had no adverse effects on the efficiency of somatic cell nuclear transfer. [Copyright &y& Elsevier]

Published

2012

17. X-ray irradiation selectively kills thymocytes of different stages and impairs the maturation of donor – derived CD4 +CD8 + thymocytes in recipient thymus

Author

Li, Jinbo, Cai, Hongquan, Jin, Jianliang, Wang, Qian, and Miao, Dengshun

Subjects

*IRRADIATION, *X-rays, *THYMOCYTES, *CD4 antigen, *CD8 antigen, *THYMUS, *BONE marrow transplantation, *GREEN fluorescent protein

Abstract

Abstract: The aim of the present study was to determine whether the sensitivity of thymocytes to X-ray radiation depends on their proliferative states and whether radiation impairs the maturation of donor-derived thymocytes in recipient thymus. We assigned 8-week-old C57BL/6J mice into three treatment groups: 1) untreated; 2) X-ray radiation; 3) X-ray radiation plus bone marrow transplantation with donor bone marrow cells from transgenic mice expressing enhanced green fluorescent protein (GFP) on a universal promoter. After 4 weeks, the size of the thymus, the number and proliferation of thymocytes and ratios of different stage thymocytes were analyzed by immunohisto-chemistry and flow cytometry. The results showed that: 1) CD4+CD8+ thymocytes were more sensitive to X-ray radiation-induced cell death than other thymocytes; 2) the proliferative capacity of CD4+CD8+ thymocytes was higher than that of other thymocytes; 3) the size of the thymus, the number of thymocytes and ratios of thymo-cytes of different stages in irradiated mice recovered to the normal level of untreated mice by bone marrow trans-plantation; 4) the ratio of GFP-positive CD4+CD8+ thymocytes increased significantly, whereas the ratio of GFP-positive CD4+ or CD8+ thymocytes decreased significantly. These results indicate that the degree of sensitivity of thymocytes to X-ray radiation depends on their proliferative states and radiation impairs the maturation of donor-derived CD4+CD8+ thymocytes in recipient thymus. [Copyright &y& Elsevier]

Published

2012

18. Promises of stem cell therapy for retinal degenerative diseases.

Author

Wong, Ian, Poon, Ming-Wai, Pang, Rosita, Lian, Qizhou, and Wong, David

Subjects

*STEM cell treatment, *RETINAL degeneration treatment, *VISION disorders, *MEDICAL technology evaluation, *THERAPEUTICS, *CLINICAL trials, *RISK assessment

Abstract

With the development of stem cell technology, stem cell-based therapy for retinal degeneration has been proposed to restore the visual function. Many animal studies and some clinical trials have shown encouraging results of stem cell-based therapy in retinal degenerative diseases. While stem cell-based therapy is a promising strategy to replace damaged retinal cells and ultimately cure retinal degeneration, there are several important challenges which need to be overcome before stem cell technology can be applied widely in clinical settings. In this review, different types of donor cell origins used in retinal treatments, potential target cell types for therapy, methods of stem cell delivery to the eye, assessments of potential risks in stem cell therapy, as well as future developments of retinal stem cells therapy, will be discussed. [ABSTRACT FROM AUTHOR]

Published

2011

19. Different reprogramming ability of fibroblast and cumulus cells after treated with trichostatin A for nuclear transfer.

Author

LI XIANGCHEN, YAO YAXIN, ZHANG YONG, JIN DAPENG, YIPENG WANG, GUAN WEIJUN, and MA YUEHUI

Abstract

The article discusses a research study on fibroblasts and cumulus cells being prone for reprogramming than other cell types after being treated with Trichostatin A (TSA). Treated with different concentrations of TSA were sheep cumulus cells (SCCs) and sheep fibroblast cells (SFCs) to determine influences on reprogramming ability. Result showed that 10 nanograms per milliliter of TSA can increase histone acetylatin level or decrease deoxuribonuclein methylation and inhibit SFC proliferation aftwerwards.

Published

2011

20. An immortalized goat mammary epithelial cell line induced with human telomerase reverse transcriptase (hTERT) gene transfer

Author

He, Y.L., Wu, Y.H., He, X.N., Liu, F.J., He, X.Y., and Zhang, Y.

Subjects

*EPITHELIAL cells, *CELL lines, *MAMMARY glands, *GENETIC transformation, *TELOMERASE, *REVERSE transcriptase polymerase chain reaction, *GOATS as laboratory animals

Abstract

Abstract: Although mammary epithelial cell lines can provide a rapid and reliable indicator of gene expression efficiency of transgenic animals, their short lifespan greatly limits this application. To provide stable and long lifespan cells, goat mammary epithelial cells (GMECs) were transduced with pLNCX2-hTERT by retrovirus-mediated gene transfer. Transduced GMECs were evaluated by reverse transcriptase polymerase chain reaction (RT-PCR), proliferation assays, karyotype analysis, telomerase activity assay, western blotting, soft agar assay, and injection into nude mice. Non-transduced GMECs were used as a control. The hTERT-GMECs had higher telomerase activity and extended proliferative lifespan compared to non-transfected GMECs; even after Passage 50, hTERT-GMECs had a near diploid complement of chromosomes. Furthermore, they did not gain the anchorage-independent growth property and were not associated with a malignant phenotype in vitro or in vivo. [Copyright &y& Elsevier]

Published

2009

21. Efficiency of human lactoferrin transgenic donor cell preparation for SCNT

Author

Zhao, M.T., Lin, H., Liu, F.J., Quan, F.S., Wang, G.H., Liu, J., Hua, S., and Zhang, Y.

Subjects

*LACTOFERRIN, *MILK proteins, *TRANSGENIC animals, *POLYMERASE chain reaction, *GENE expression, *FIBROBLASTS, *TRANSPLANTATION of cell nuclei

Abstract

Abstract: The combination of somatic cell nuclear transfer (SCNT) and transgenic technology leads to the production of transgenic cloned animals, wherein the preparation of competent transgenic donor cells is the pivotal upstream step. The purpose of this study was to establish an efficient procedure to prepare human lactoferrin (hLTF) transgenic donor cells for SCNT. Thus, two cell culture systems were employed: caprine mammary epithelial cells (for evaluation of the hTLF transgenic expression in vitro), and fetal-derived fibroblast cells (for identification of competent transgenic donor cells). Induced by hormonal signals, recombinant hLTF was detected in the supernatant of transfected mammary epithelial cells by Western blot. Reliable hLTF transgenic fibroblast cell clones were identified by screening with multiple PCR amplification, EGFP fluorescence, and chromosomal counting (32.5±2.3%). This study may provide an effective upstream system to prepare SCNT donor cells for the production of human recombinant pharmaceuticals from the milk of transgenic animals. [Copyright &y& Elsevier]

Published

2009

22. Donor cell transplantation for myocardial disease: does it complement current pharmacological therapies?

Author

McMullen, Nichole M. and Pasumarthi, Kishore B. S.

Subjects

*CARDIOMYOPATHIES, *CELL transplantation, *PHARMACOLOGY, *HEART diseases, *THERAPEUTICS, DEVELOPED countries

Abstract

Heart failure secondary to ischemic heart disease, hypertension, and myocardial infarction is a common cause of death in developed countries. Although pharmacological therapies are very effective, poor prognosis and shorter life expectancy of heart disease patients clearly indicate the need for alternative interventions to complement the present therapies. Since the progression of heart disease is associated with the loss of myocardial cells, the concept of donor cell transplantation into host myocardium is emerging as an attractive strategy to repopulate the damaged tissue. To this end, a number of donor cell types have been tested for their ability to increase the systolic function of diseased hearts in both experimental and clinical settings. Although initial clinical trials with bone marrow stem cells are encouraging, long-term consequences of such interventions are yet to be rigorously examined. While additional laboratory studies are required to address several issues in this field, there is also a clear need for further characterization of drug interactions with donor cells in these interventions. Here, we provide a brief summary of current pharmacological and cell-based therapies for heart disease. Further, we discuss the potential of various donor cell types in myocardial repair, mechanisms underlying functional improvement in cell-based therapies, as well as potential interactions between pharmacological and cell-based therapies. [ABSTRACT FROM AUTHOR]

Published

2007

23. Infusion of donor spleen cells and rejection in liver transplant recipients.

Author

Scornik, Juan C, Lauwers, Gregory Y, Reed, Alan I, Howard, Richard J, Dickson, Rolland C, and Rosen, Charles B

Subjects

*LIVER transplantation, SPLEEN transplantation

Abstract

Intact or inactivated donor lymphoid cells have been found to downregulate the alloimmune response in a number of experimental models. We conducted a randomized, prospective, double blind, and placebo-controlled trial to determine whether heat-treated donor spleen cells would affect early rejection after liver transplantation. Donor spleen was obtained during organ procurement for 40 patients undergoing liver transplantation. All patients were treated with cyclosporine, azathioprine and steroids. The patients were randomized after surgery to receive either heat-treated (45°C for 1 h) spleen cells or placebo. Patients underwent protocol biopsies at 1 wk, 4 and 12 months, or as needed. Biopsies were reviewed in a blind fashion and scored according to the Banff consensus criteria. Randomization resulted in 19 patients in the spleen cell group and 21 in the placebo group. One-yr graft survival was 94 and 100%, respectively. Early rejection was more frequent in the spleen cell group (61 vs. 35%, p, not significant). The histopathological rejection activity index at 7 d was also higher for the patients in the spleen cell group: 39% of spleen cell treated patients had a score of 4 or higher as opposed to 5% in the placebo group (p<0.01). The mean score was 2.9±2.8 for the spleen cell group versus 1.3±1.7 for the placebo group (p=0.034). It is concluded that heat-treated donor spleen cells given within 24 h after liver transplantation were not clinically beneficial and increased the intensity of rejection in 7-d protocol liver biopsies. [ABSTRACT FROM AUTHOR]

Published

2000

24. Cardiac Allograft Vasculopathy: A Donor or Recipient Induced Pathology?

Author

Joost P.G. Sluijter, Roel A. de Weger, Manon M. H. Huibers, and Patricia van den Hoogen

Subjects

Neointima, Graft Rejection, Pathology, medicine.medical_specialty, Recipient cells, medicine.medical_treatment, Pharmaceutical Science, Review, Coronary Artery Disease, Heart transplantation, Article, Pathogenesis, Immune system, Donor cells, Fibrosis, Risk Factors, medicine, Journal Article, Genetics, Animals, Humans, Genetics(clinical), Immune response, Genetics (clinical), Heart Failure, business.industry, Cardiac allograft vasculopathy, medicine.disease, Allografts, Molecular medicine, Coronary Vessels, Circulating cells, Tissue Donors, Transplant Recipients, Coronary arteries, medicine.anatomical_structure, Mismatch, Treatment Outcome, Heart failure, cardiovascular system, Molecular Medicine, business, Cardiology and Cardiovascular Medicine

Abstract

Cardiac allograft vasculopathy (CAV) is one of the main causes of late-stage heart failure after heart transplantation. CAV is characterized by concentric luminal narrowing of the coronary arteries, but the exact pathogenesis of CAV is still not unraveled. Many researchers show evidence of an allogeneic immune response of the recipient, whereas others show contrasting results in which donor-derived cells induce an immune response against the graft. In addition, fibrosis of the neo-intima can be induced by recipient-derived circulating cells or donor-derived cells. In this review, both donor and recipient sides of the story are described to obtain better insight in the pathogenesis of CAV. Dual outcomes were found regarding the contribution of donor and recipient cells in the initiation of the immune response and the development of fibrosis during CAV. Future research could focus more on the potential synergistic interaction of donor and recipient cells leading to CAV.

Published

2015

25. Cardiac Allograft Vasculopathy: A Donor or Recipient Induced Pathology?

Author

van den Hoogen, Patricia, Huibers, Manon M. H., Sluijter, Joost P. G., and de Weger, Roel A.

Published

2015

26. Promises of stem cell therapy for retinal degenerative diseases

Author

David Wong, Ian Y. H. Wong, Qizhou Lian, Rosita Tsz-Wai Pang, and Ming-Wai Poon

Subjects

Retinal degeneration, Cell type, Pathology, medicine.medical_specialty, Donor cell, Retinal degenerative diseases, medicine.medical_treatment, Method of cell delivery, Target cell types, Review Article, Biology, Clinical applications, chemistry.chemical_compound, Cellular and Molecular Neuroscience, Donor cells, medicine, Humans, Stem cell therapy, Retinal Degeneration, Retinal, Stem-cell therapy, medicine.disease, Sensory Systems, Clinical trial, Ophthalmology, Treatment Outcome, chemistry, Stem cell, Neuroscience, Retinal treatments, Potential risks, Stem Cell Transplantation

Abstract

With the development of stem cell technology, stem cell-based therapy for retinal degeneration has been proposed to restore the visual function. Many animal studies and some clinical trials have shown encouraging results of stem cell-based therapy in retinal degenerative diseases. While stem cell-based therapy is a promising strategy to replace damaged retinal cells and ultimately cure retinal degeneration, there are several important challenges which need to be overcome before stem cell technology can be applied widely in clinical settings. In this review, different types of donor cell origins used in retinal treatments, potential target cell types for therapy, methods of stem cell delivery to the eye, assessments of potential risks in stem cell therapy, as well as future developments of retinal stem cells therapy, will be discussed., published_or_final_version, Springer Open Choice, 21 Feb 2012

Published

2011

27. Epigenetic marks in cloned rhesus monkey embryos: Comparison with counterparts produced in vitro

Author

Yang, Jifeng, Yang, Shihua, Beaujean, Nathalie, Niu, Yuyu, He, Xiechao, Xie, Yunhua, Tang, Xianghui, Wang, Liu, Zhou, Qi, Ji, Weizhi, Chinese Academy of Sciences (CAS), University of Chinese Academy of Sciences, CAS (UCAS), Biologie du développement et reproduction (BDR), and Centre National de la Recherche Scientifique (CNRS)-École nationale vétérinaire d'Alfort (ENVA)-Institut National de la Recherche Agronomique (INRA)

Subjects

EMBRYONIC DEVELOPMENT, EPIGENETIC REPROGRAMMING, HISTONE ACETYLATION, EARLY DEVELOPMENT, EMBRYO, IN VITRO FERTILIZATION, [SDV.BDLR]Life Sciences [q-bio]/Reproductive Biology, SOMATIC CELL NUCLEAR TRANSFER, DNA METHYLATION, RHESUS MONKEY, ComputingMilieux_MISCELLANEOUS, DONOR CELLS

Abstract

International audience

Published

2007

28. Donor cell-derived myelodysplastic syndrome with ring chromosome 7 after allogeneic hematopoietic stem cell transplant in 2 patients with lymphomas as primary disease.

Author

Hamdi A, Afrough A, Muzzafar T, Popat UR, Hosing CM, Qazilbash MH, and Lu G

Subjects

Allografts, Antibodies, Monoclonal administration & dosage, Antibodies, Monoclonal, Murine-Derived administration & dosage, Biomarkers, Tumor, Bone Marrow pathology, Chromosomes, Human, Pair 7 genetics, Cyclophosphamide administration & dosage, Disease Progression, Female, Humans, In Situ Hybridization, Fluorescence, Leukemia, Myeloid, Acute genetics, Leukemia, Myeloid, Acute pathology, Living Donors, Lymphoma, Follicular drug therapy, Lymphoma, Mantle-Cell drug therapy, Male, Middle Aged, Myelodysplastic Syndromes genetics, Myelodysplastic Syndromes pathology, Neoplasms, Second Primary pathology, Proto-Oncogene Proteins c-ets deficiency, Proto-Oncogene Proteins c-ets genetics, Repressor Proteins deficiency, Repressor Proteins genetics, Rituximab, Transplantation Chimera genetics, Vidarabine administration & dosage, Vidarabine analogs & derivatives, ETS Translocation Variant 6 Protein, Cell Transformation, Neoplastic genetics, Chromosome Deletion, Chromosomes, Human, Pair 7 ultrastructure, Gene Deletion, Leukemia, Myeloid, Acute etiology, Lymphoma, Follicular therapy, Lymphoma, Mantle-Cell therapy, Myelodysplastic Syndromes etiology, Neoplasms, Second Primary etiology, Peripheral Blood Stem Cell Transplantation, Ring Chromosomes

Published

2014

29. Epigenetic Marks in Cloned Rhesus Monkey Embryos: Comparison with Counterparts Produced In Vitro1

Author

Yang, Jifeng, Yang, Shihua, Beaujean, Nathalie, Niu, Yuyu, He, Xiechao, Xie, Yunhua, Tang, Xianghui, Wang, Liu, Zhou, Qi, and Ji, Weizhi

Published

2006