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Published July 1, 1982 | public
Journal Article Open

Joining of Immunoglobulin Heavy Chain Gene Segments: Implications from a Chromosome with Evidence of Three D-JH Fusions

Abstract

A chromosomal segment with a unique structure around the immunoglobulin heavy chain joining region (JH) has been molecularly cloned from an Abelson murine leukemia virus-transformed cell line. Attached to JH3 in the cloned DNA, in inverted sequence, is the DNA from JH1 to the JH2 recognition sequence. The inverted segment is attached at its other end to the 5' recognition sequence of a diversity segment (D). To form this structure, three joining events must have occurred on the same chromosome. One of these events could have been a normal D-JH joining but the others must have been irregular events including ones that result in inversions. One of the joining events left fused recognition elements from JH2 and a D whose sequence shows that, during joining, reciprocal joinings of the recognition elements must occur to fuse the heptameric elements back to back. Because joined D and JH undergo deletion of terminal coding sequence during recombination but the joined heptameric recognition sequences do not contain the deleted sequence, joining must be a nonreciprocal event. Also, extra nucleotides are inserted between D and JH as part of the joining process; it is suggested that this added sequence is a product of the activity of terminal deoxynucleotidyltransferase at the D/JH (and probably the VH/D) joints and that it represents a new element of heavy chain gene structure, the N region.

Additional Information

Copyright © 1982 by the National Academy of Sciences Contributed by David Baltimore, March 8, 1982 We thank Elise Thomas for expert technical assistance and Dr. Michael Boss and Ms. Nancy Andrews for their advice and assistance. We are also indebted to Drs. Y. Kurosawa and S. Tonegawa for making available unpublished data and for their stimulating discussions -- particularly their observation that no bases are added to joints between Ds and Js that contain overlapping bases. This work was supported by Grant MV-34M from the American Cancer Society, Grant CA14051 (core grant to S.E. Luria) from The National Cancer Institute, and by a contribution from The Whitehead Charitable Foundation. D.B. is an American Cancer Society Research Professor. The publication costs of this article were defrayed in part by page charge payment. This article must therefore be hereby marked "advertisement" in accordance with 18 U. S. C. §1734 solely to indicate this fact.

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August 22, 2023
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