Plasma from human mothers of fetuses with severe arthrogryposis multiplex congenita causes deformities in mice
Leslie Jacobson, … , Gillian Morriss-Kay, Angela Vincent
Leslie Jacobson, … , Gillian Morriss-Kay, Angela Vincent
Published April 1, 1999
Citation Information: J Clin Invest. 1999;103(7):1031-1038. https://doi.org/10.1172/JCI5943.
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Article

Plasma from human mothers of fetuses with severe arthrogryposis multiplex congenita causes deformities in mice

Abstract

Arthrogryposis multiplex congenita (AMC) is characterized by fixed joint contractures and other deformities, sometimes resulting in fetal death. The cause is unknown in most cases, but some women with fetuses affected by severe AMC have serum antibodies that inhibit fetal acetylcholine receptor (AChR) function, and antibodies to fetal antigens might play a pathogenic role in other congenital disorders. To investigate this possibility, we have established a model by injecting pregnant mice with plasma from four anti-AChR antibody–positive women whose fetuses had severe AMC. We found that human antibodies can be transferred efficiently to the mouse fetus during the last few days of fetal life. Many of the fetuses of dams injected with AMC maternal plasmas or Ig were stillborn and showed fixed joints and other deformities. Moreover, similar changes were found in mice after injection of a serum from one anti-AChR antibody–negative mother who had had four AMC fetuses. Thus, we have confirmed the role of maternal antibodies in cases of AMC associated with maternal anti-AChR, and we have demonstrated the existence of pathogenic maternal factors in one other case. Importantly, this approach can be used to look at the effects of other maternal human antibodies on development of the fetus.

Authors

Leslie Jacobson, Agata Polizzi, Gillian Morriss-Kay, Angela Vincent

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Anti-AChR antibodies tested for binding to adult and fetal human acetylc...
Anti-AChR antibodies tested for binding to adult and fetal human acetylcholine receptor (AChR) in plasma from AMC-M2 and AMC-M7. Approximately equal amounts of fetal AChR (from TE671 cells) and adult AChR (from TE671-ε, a subline that expresses predominantly the adult form; ref. 20) were used. Dilutions of each plasma were added to the 125I-αbungarotoxin (125I-αBuTx)–labeled AChR preparations for 2 h, followed by immunoprecipitation with goat anti–human IgG. Results are given as femtomoles of 125I-αbungarotoxin AChR precipitated by each dilution of serum. All antibody measurements in this study are based on titrations similar to these. AMC, arthrogryposis multiplex congenita.