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Dive into the research topics where Lynn R. Fraser is active.

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Featured researches published by Lynn R. Fraser.


Molecular Reproduction and Development | 1997

TCP-11, the product of a mouse t-complex gene, plays a role in stimulation of capacitation and inhibition of the spontaneous acrosome reaction

Lynn R. Fraser; Ramine Hosseini; Alon Talmor; R. Keith Dudley

Tcp‐11 is a candidate for a distorter gene within the t‐complex on mouse chromosome 17; although t‐complex genes appear to affect sperm function, relatively little is known about mechanisms whereby these genes might play a specific physiological role. We present evidence that the protein TCP‐11 is found on the surface of mature epididymal spermatozoa. Although detected on both the acrosomal cap region of the head and the flagellum of acrosome‐intact cells, it is absent from the heads of acrosome‐reacted cells. When epididymal spermatozoa were incubated in the presence of anti‐TCP‐11 IgG Fab fragments for a total of 120 min and assessed using chlortetracycline fluorescence, we observed a stimulation of capacitation and an inhibition of spontaneous acrosome loss, suggestive of enhanced fertility compared with untreated suspensions. In vitro fertilization experiments confirmed that Fab‐treated suspensions became fertile more quickly and then maintained high fertility. Because these responses were remarkably similar to those obtained using the TRH‐related peptide FPP (fertilization promoting peptide; pGlu‐Glu‐ProNH2) and adenosine, we investigated responses to Fab fragments, FPP, and adenosine. Results indicated that the Fab fragments appear to work at the same extracellular site as FPP, one that is distinct from the adenosine site of action. Further evidence for this conclusion was obtained using pGlu‐Gln‐ProNH2, an FPP‐related tripeptide known to competitively inhibit responses to FPP; as with FPP, pGlu‐Gln‐ProNH2 inhibited the stimulatory effect of Fab fragments in a concentration‐dependent manner. From these results we suggest that TCP‐11 may be the receptor for FPP and that the adenylate clyclase/cyclic AMP pathway may be the signal transduction pathway activated by interactions between extracellular effector molecules (e.g., Fab fragments or FPP acting as an agonist) and TCP‐11. A mechanism such as this that promotes capacitation but inhibits spontaneous acrosome loss in vivo would play a very important role by helping to maximize the fertilizing potential of the few spermatozoa that reach the site of fertilization. The fact that there is a human homolog of Tcp‐11 suggests that this gene could play an important role in regulation of human, as well as mouse, sperm function. Mol. Reprod. Dev. 48:375–382, 1997.


Human Reproduction | 1998

The modulation of sperm function by fertilization promoting peptide

Lynn R. Fraser


Molecular Human Reproduction | 1996

Protein kinase C activation during progesterone-stimulated acrosomal exocytosis in human spermatozoa

Christine M.B.O Toole; Eduardo R. S. Roldan; Lynn R. Fraser


Human Reproduction | 1996

Fertilization promoting peptide, a tripeptide similar to thyrotrophin-releasing hormone, stimulates the capacitation and fertilizing ability of human spermatozoa in vitro

C.M. Green; S.M. Cockle; P.F. Watson; Lynn R. Fraser


Human Reproduction | 1998

Sperm capacitation and the acrosome reaction

Lynn R. Fraser


Gamete Research | 1986

Adenosine and Gpp(NH)p modulate mouse sperm adenylate cyclase

D. M. Stein; Lynn R. Fraser; Nicola J. Monks


Molecular Human Reproduction | 1996

Regulators of sperm function: A role for diacylglycerol in human sperm acrosomal exocytosis

Christine M.B. O'Toole; Eduardo R. S. Roldan; Paul Hampton; Lynn R. Fraser


Human Reproduction | 1995

Cellular biology of capacitation and the acrosome reaction

Lynn R. Fraser


Gamete Research | 1988

Inhibition of adenosine‐metabolizing enzymes modulates mouse sperm fertilizing ability: A changing role for endogenously generated adenosine during capacitation

Nicola J. Monks; Lynn R. Fraser


Gamete Research | 1986

A comparison of fertility in vitro and in vivo after exposure of male mice to high environmental pressure

Lynn R. Fraser; Susan J. Monk; Bridget Wardley-Smith; Shara Cohen; M.J. Halsey

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Eduardo R. S. Roldan

Spanish National Research Council

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C.M. Green

University of Cambridge

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M.J. Halsey

Northwick Park Hospital

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Paul Hampton

University of Cambridge

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