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Expression levels of ABCG2 on cord red blood cells and study of fetal anemia associated with anti-Jr(a).

作者信息

Fujita Satoko, Kashiwagi Hirokazu, Tomimatsu Takuji, Ito Shoichi, Mimura Kazuya, Kanagawa Takeshi, Endo Masayuki, Miyoshi Tomomitsu, Okamura Yasushi, Tani Yoshihiko, Tomiyama Yoshiaki, Kimura Tadashi

机构信息

Department of Obstetrics and Gynecology.

Department of Hematology and Oncology.

出版信息

Transfusion. 2016 May;56(5):1171-81. doi: 10.1111/trf.13515. Epub 2016 Feb 11.

Abstract

BACKGROUND

The Jr(a) antigen of JR blood group systems is located on ABCG2 and Jr(a-) subjects whose red blood cells (RBCs) lack ABCG2 have been identified mostly among the Japanese. Although anti-Jr(a) can cause fetal anemia, little is known regarding its mechanism.

STUDY DESIGN AND METHODS

We reviewed clinical courses of all reported cases with fetal anemia due to anti-Jr(a) . We analyzed the ABCG2 expressions of cord RBCs at various gestational ages. We examined the effects of sera containing anti-Jr(a) from three pregnancies with fetal anemia or monoclonal anti-Jr(a) on erythropoiesis and phagocytosis. We also examined epitopes of anti-Jr(a) .

RESULTS

Case series suggested that the majority of fetal anemia with anti-Jr(a) may not be progressive in the later gestational ages. ABCG2 expression levels of cord RBCs were significantly higher than those of adults and neonates with high individual variation and gradually decreased with advancing gestational ages. Anti-Jr(a) did not significantly impact erythroid colony formation, although we detected a tendency toward the suppression of erythroid burst-forming unit formation by anti-Jr(a) using feline marrow cells. Anti-Jr(a) did not induce phagocytosis of sensitized RBCs by monocytes. While many anti-Jr(a) recognized the same regions as a monoclonal anti-ABCG2, 5D3, epitopes of anti-Jr(a) did not correlate with the incidence of fetal anemia.

CONCLUSION

ABCG2 expression levels in cord RBCs are higher than those of adults, and the change of ABCG2 expression in erythroid lineage cells may influence the clinical course of fetal anemia with anti-Jr(a) , although we could not detect significant effects of anti-Jr(a) on erythroid colony formation or phagocytosis.

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