【 摘 要 】

Background

We investigated the capacity of expanded cord blood-derived CD34+ hematopoietic progenitor cells to undergo respiratory epithelial differentiation ex vivo, and to engraft and attenuate alveolar disruption in injured newborn murine lungs in vivo.

Methods

Respiratory epithelial differentiation was studied in CD34+ cells expanded in the presence of growth factors and cytokines (“basic” medium), in one group supplemented with dexamethasone (“DEX”). Expanded or freshly isolated CD34+ cells were inoculated intranasally in newborn mice with apoptosis-induced lung injury. Pulmonary engraftment, lung growth and alveolarization were studied at 8 weeks post-inoculation.

Results

SP-C mRNA expression was seen in 2/7 CD34+ cell isolates expanded in basic media and in 6/7 isolates expanded in DEX, associated with cytoplasmic SP-C immunoreactivity and ultrastructural features suggestive of type II cell-like differentiation. Administration of expanding CD34+ cells was associated with increased lung growth and, in animals treated with DEX-exposed cells, enhanced alveolar septation. Freshly isolated CD34+ cells had no effect of lung growth or remodeling. Lungs of animals treated with expanded CD34+ cells contained intraalveolar aggregates of replicating alu-FISH-positive mononuclear cells, whereas epithelial engraftment was extremely rare.

Conclusion

Expanded cord blood CD34+ cells can induce lung growth and alveolarization in injured newborn lungs. These growth-promoting effects may be linked to paracrine or immunomodulatory effects of persistent cord blood-derived mononuclear cells, as expanded cells showed limited respiratory epithelial transdifferentiation.

【 授权许可】

   
2013 Mao et al.; licensee BioMed Central Ltd.

【 预 览 】

附件列表

Files	Size	Format	View
20140705073655600.pdf	1740KB	PDF	download
Figure 7.	129KB	Image	download
Figure 6.	76KB	Image	download
Figure 5.	81KB	Image	download
Figure 4.	82KB	Image	download
Figure 3.	104KB	Image	download
Figure 2.	72KB	Image	download
Figure 1.	81KB	Image	download

【 图 表 】

【 参考文献 】

• [1]Jobe AH, Bancalari E: Bronchopulmonary dysplasia. Am J Respir Crit Care Med 2001, 163:1723-1729.
• [2]Husain AN, Siddiqui NH, Stocker JT: Pathology of arrested acinar development in postsurfactant bronchopulmonary dysplasia. Hum Pathol 1998, 29:710-717.
• [3]Jobe AJ: The new BPD: an arrest of lung development. Pediatr Res 1999, 46:641-643.
• [4]De Paepe ME, Mao Q, Powell J, Rubin SE, DeKoninck P, Appel N, Dixon M, Gundogan F: Growth of pulmonary microvasculature in ventilated preterm infants. Am J Respir Crit Care Med 2006, 173:204-211.
• [5]Alphonse RS, Rajabali S, Thebaud B: Lung injury in preterm neonates: the role and therapeutic potential of stem cells. Antioxid Redox Signal 2012, 17:1013-1040.
• [6]O’Reilly M, Thebaud B: Cell-based strategies to reconstitute lung function in infants with severe bronchopulmonary dysplasia. Clin Perinatol 2012, 39:703-725.
• [7]De Paepe ME, Mao Q, Ghanta S, Hovanesian V, Padbury JF: Alveolar epithelial cell therapy with human cord blood-derived hematopoietic progenitor cells. Am J Pathol 2011, 178:1329-1339.
• [8]Ikegami M, Jobe AH, Huffman Reed JA, Whitsett JA: Surfactant metabolic consequences of overexpression of GM-CSF in the epithelium of GM-CSF-deficient mice. Am J Physiol 1997, 273:L709-L714.
• [9]Pelaez A, Bechara RI, Joshi PC, Brown LA, Guidot DM: Granulocyte/macrophage colony-stimulating factor treatment improves alveolar epithelial barrier function in alcoholic rat lung. Am J Physiol Lung Cell Mol Physiol 2004, 286:L106-L111.
• [10]Baytur YB, Ozbilgin K, Yuksel H, Kose C: Antenatal administration of granulocyte-macrophage colony-stimulating factor increases fetal lung maturation and endothelial nitric oxide synthase expression in the fetal rat lung. Eur J Obstet Gynecol Reprod Biol 2008, 136:171-177.
• [11]Massaro D, De Carlo Massaro G: Retinoids, alveolus formation, and alveolar deficiency: clinical implications. Am J Respir Cell Mol Biol 2003, 28:271-274.
• [12]Chytil F: Retinoids in lung development. FASEB J 1996, 10:986-992.
• [13]Ware LB, Matthay MA: Keratinocyte and hepatocyte growth factors in the lung: roles in lung development, inflammation, and repair. Am J Physiol Lung Cell Mol Physiol 2002, 282:L924-L940.
• [14]Sugahara K, Rubin JS, Mason RJ, Aronsen EL, Shannon JM: Keratinocyte growth factor increases mRNAs for SP-A and SP-B in adult rat alveolar type II cells in culture. Am J Physiol 1995, 269:L344-L350.
• [15]Deterding RR, Jacoby CR, Shannon JM: Acidic fibroblast growth factor and keratinocyte growth factor stimulate fetal rat pulmonary epithelial growth. Am J Physiol 1996, 271:L495-L505.
• [16]Mason RJ, Lewis MC, Edeen KE, McCormick-Shannon K, Nielsen LD, Shannon JM: Maintenance of surfactant protein A and D secretion by rat alveolar type II cells in vitro. Am J Physiol Lung Cell Mol Physiol 2002, 282:L249-L258.
• [17]Gonzales LW, Guttentag SH, Wade KC, Postle AD, Ballard PL: Differentiation of human pulmonary type II cells in vitro by glucocorticoid plus cAMP. Am J Physiol Lung Cell Mol Physiol 2002, 283:L940-L951.
• [18]Fritzell JA Jr, Mao Q, Gundavarapu S, Pasquariello T, Aliotta JM, Ayala A, Padbury JF, De Paepe ME: Fate and effects of adult bone marrow cells in lungs of normoxic and hyperoxic newborn mice. Am J Respir Cell Mol Biol 2009, 40:575-587.
• [19]De Paepe ME, Gundavarapu S, Tantravahi U, Pepperell JR, Haley SA, Luks FI, Mao Q: Fas-ligand-induced apoptosis of respiratory epithelial cells causes disruption of postcanalicular alveolar development. Am J Pathol 2008, 173:42-56.
• [20]De Paepe ME, Haley SA, Lacourse Z, Mao Q: Effects of Fas-ligand overexpression on alveolar type II cell growth kinetics in perinatal murine lungs. Pediatr Res 2010, 68:57-62.
• [21]De Paepe ME, Mao Q, Chao Y, Powell JL, Rubin LP, Sharma S: Hyperoxia-induced apoptosis and Fas/FasL expression in lung epithelial cells. Am J Physiol Lung Cell Mol Physiol 2005, 289:L647-L659.
• [22]Tichelaar JW, Lu W, Whitsett JA: Conditional expression of fibroblast growth factor-7 in the developing and mature lung. J Biol Chem 2000, 275:11858-11864.
• [23]De Paepe ME, Johnson BD, Papadakis K, Luks FI: Lung growth response after tracheal occlusion in fetal rabbits is gestational age-dependent. Am J Respir Cell Mol Biol 1999, 21:65-76.
• [24]De Paepe ME, Johnson BD, Papadakis K, Sueishi K, Luks FI: Temporal pattern of accelerated lung growth after tracheal occlusion in the fetal rabbit. Am J Pathol 1998, 152:179-190.
• [25]Aherne WA, Dunnill MS: The estimation of whole organ volume. In Morphometry. Edited by Aherne WA, Dunnill MS. London: Edward Arnold Ltd; 1982:10-18.
• [26]Migliaccio G, Sanchez M, Masiello F, Tirelli V, Varricchio L, Whitsett C, Migliaccio AR: Humanized culture medium for clinical expansion of human erythroblasts. Cell Transplant 2010, 19:453-469.
• [27]Ganguli G, Back J, Sengupta S, Wasylyk B: The p53 tumour suppressor inhibits glucocorticoid-induced proliferation of erythroid progenitors. EMBO Rep 2002, 3:569-574.
• [28]England SJ, McGrath KE, Frame JM, Palis J: Immature erythroblasts with extensive ex vivo self-renewal capacity emerge from the early mammalian fetus. Blood 2011, 117:2708-2717.
• [29]Sueblinvong V, Loi R, Eisenhauer PL, Bernstein IM, Suratt BT, Spees JL, Weiss DJ: Derivation of lung epithelium from human cord blood-derived mesenchymal stem cells. Am J Respir Crit Care Med 2008, 177:701-711.
• [30]Berger MJ, Minnerath SR, Adams SD, Tigges BM, Sprague SL, McKenna DH Jr: Gene expression changes with differentiation of cord blood stem cells to respiratory epithelial cells: a preliminary observation. Stem Cell Res Ther 2011, 2:19. BioMed Central Full Text
• [31]Berger MJ, Adams SD, Tigges BM, Sprague SL, Wang XJ, Collins DP, McKenna DH: Differentiation of umbilical cord blood-derived multilineage progenitor cells into respiratory epithelial cells. Cytotherapy 2006, 8:480-487.
• [32]Alphonse RS, Thebaud B: Growth factors, stem cells and bronchopulmonary dysplasia. Neonatology 2011, 99:326-337.
• [33]Pierro M, Ionescu L, Montemurro T, Vadivel A, Weissmann G, Oudit G, Emery D, Bodiga S, Eaton F, Peault B: Short-term, long-term and paracrine effect of human umbilical cord-derived stem cells in lung injury prevention and repair in experimental bronchopulmonary dysplasia. Thorax 2012. Epub ahead of print
• [34]Chang YS, Oh W, Choi SJ, Sung DK, Kim SY, Choi EY, Kang S, Jin HJ, Yang YS, Park WS: Human umbilical cord blood-derived mesenchymal stem cells attenuate hyperoxia-induced lung injury in neonatal rats. Cell Transplant 2009, 18:869-886.
• [35]Ahn SY, Chang YS, Kim SY, Sung DK, Kim ES, Rime SY, Yu WJ, Choi SJ, Oh WI, Park WS: Long-term (postnatal day 70) outcome and safety of intratracheal transplantation of human umbilical cord blood-derived mesenchymal stem cells in neonatal hyperoxic lung injury. Yonsei Med J 2013, 54:416-424.
• [36]Qi Y, Li RM, Kong FM, Li H, Yu JP, Ren XB: How do tumor stem cells actively escape from host immunosurveillance? Biochem Biophys Res Commun 2012, 420:699-703.