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Featured researches published by Renee Reijo.


Nature Genetics | 1995

Diverse spermatogenic defects in humans caused by Y chromosome deletions encompassing a novel RNA–binding protein gene

Renee Reijo; Tien-Yi Lee; Pia Salo; Raaji K. Alagappan; Laura G. Brown; Michael Rosenberg; Steve Rozen; Tom Jaffe; Donald Straus; Outi Hovatta; Albert de la Chapelle; Sherman J. Silber; David C. Page

We have detected deletions of portions of the Y chromosome long arm in 12 of 89 men with azoospermia (no sperm in semen). No Y deletions were detected in their male relatives or in 90 other fertile males. The 12 deletions overlap, defining a region likely to contain one or more genes required for spermatogenesis (the Azoospermia Factor, AZF). Deletion of the AZF region is associated with highly variable testicular defects, ranging from complete absence of germ cells to spermatogenic arrest with occasional production of condensed spermatids. We find no evidence of YRRM genes, recently proposed as AZF candidates, in the AZF region. The region contains a single–copy gene, DAZ (Deleted in AZoospermia), which is transcribed in the adult testis and appears to encode an RNA binding protein. The possibility that DAZ is AZF should now be explored.


Nature Genetics | 1996

The DAZ gene cluster on the human Y chromosome arose from an autosomal gene that was transposed, repeatedly amplified and pruned

Richa Saxena; Laura G. Brown; Trevor Hawkins; Raaji K. Alagappan; Helen Skaletsky; Mary Pat Reeve; Renee Reijo; Steve Rozen; Mary Beth Dinulos; Christine M. Disteche; David C. Page

It is widely believed that most or all Y–chromosomal genes were once shared with the X chromosome. The DAZ gene is a candidate for the human Y–chromosomal Azoospermia Factor (AZF). We report multiple copies of DAZ (>99% identical in DNA sequence) clustered in the AZF region and a functional DAZ homologue (DAZH) on human chromosome 3. The entire gene family appears to be expressed in germ cells. Sequence analysis indicates that the Y–chromosomal DAZ cluster arose during primate evolution by (i) transposing the autosomal gene to the Y, (ii) amplifying and pruning exons within the transposed gene and (iii) amplifying the modified gene. These results challenge prevailing views of sex chromosome evolution, suggesting that acquisition of autosomal fertility genes is an important process in Y chromosome evolution.


Biology of Reproduction | 2000

DAZ Family Proteins Exist Throughout Male Germ Cell Development and Transit from Nucleus to Cytoplasm at Meiosis in Humans and Mice

Renee Reijo; David M. Dorfman; Roger Slee; Andrew A. Renshaw; Kevin R. Loughlin; Howard J. Cooke; David C. Page

Abstract The human DAZ gene family is expressed in germ cells and consists of a cluster of nearly identical DAZ (deleted in azoospermia) genes on the Y chromosome and an autosomal homolog, DAZL (DAZ-like). Only the autosomal gene is found in mice. Y-chromosome deletions that encompass the DAZ genes are a common cause of spermatogenic failure in men, and autosomal homologs of DAZ are essential for testicular germ cell development in mice and Drosophila. Previous studies have reported that mouse DAZL protein is strictly cytoplasmic and that human DAZ protein is restricted to postmeiotic cells. By contrast, we report here that human DAZ and human and mouse DAZL proteins are present in both the nuclei and cytoplasm of fetal gonocytes and in spermatogonial nuclei. The proteins relocate to the cytoplasm during male meiosis. Further observations using human tissues indicate that, unlike DAZ, human DAZL protein persists in spermatids and even spermatozoa. These results, combined with findings in diverse species, suggest that DAZ family proteins function in multiple cellular compartments at multiple points in male germ cell development. They may act during meiosis and much earlier, when spermatogonial stem cell populations are established.


The Lancet | 1996

Severe oligozoospermia resulting from deletions of azoospermia factor gene on Y chromosome

Renee Reijo; Raaji K. Alagappan; David C. Page; P. Patrizio


American Journal of Human Genetics | 1995

Gonadoblastoma: molecular definition of the susceptibility region on the Y chromosome.

Karen D. Tsuchiya; Renee Reijo; David C. Page; Christine M. Disteche


Human Reproduction | 1997

Azoospermic men with deletion of the DAZ gene cluster are capable of completing spermatogenesis: fertilization, normal embryonic development and pregnancy occur when retrieved testicular spermatozoa are used for intracytoplasmic sperm injection.

J.P. Mulhall; Renee Reijo; Raaji K. Alagappan; Laura G. Brown; David C. Page; R. Carson; Robert D. Oates


Genomics | 1996

Mouse autosomal homolog of DAZ, a candidate male sterility gene in humans, is expressed in male germ cells before and after puberty

Renee Reijo; Judith Seligman; Mary Beth Dinulos; Tom Jaffe; Laura G. Brown; Christine M. Disteche; David C. Page


Human Reproduction | 1998

Male infertility: analysis of the markers and genes on the human Y chromosome.

Dana R. Kostiner; Paul J. Turek; Renee Reijo


Archive | 1996

Daz: a gene associated with azoospermia

David C. Page; Renee Reijo


Archive | 1996

DAZ: a gene family associated with azoospermia

David C. Page; Renee Reijo; Richa Saxena; Trevor Hawkins; Mary Pat Reeve

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David C. Page

University of Wisconsin-Madison

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Raaji K. Alagappan

Massachusetts Institute of Technology

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Laura G. Brown

Massachusetts Institute of Technology

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Tom Jaffe

Howard Hughes Medical Institute

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Steve Rozen

National University of Singapore

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Mary Pat Reeve

Massachusetts Institute of Technology

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Michael Rosenberg

Howard Hughes Medical Institute

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