G Mayer scite author profile

A 13-year-old patient developed severe shock due to administration of a Yersinia enterocolitica-contaminated red blood cell concentrate. Y. enterocolitica (serotype O:9, biotype II) was cultivated from the residual blood in the blood bag and from a stool sample of the blood donor. In the donor's plasma immunoglobulin M (IgM), IgA, and IgG antibodies against Yersinia outer proteins (YopM, -H, -D, and -E) were found. Since the donor remembered a short-lasting, mild diarrhea 14 days prior to blood donation, a transient attack of Yersinia enteritis may be associated with a longer than expected period of asymptomatic bacteremia that causes contamination of donor blood. Serological screening for IgM antibodies against Yersinia outer proteins might offer a way to reduce the risk of transfusion-associated Y. enterocolitica sepsis.

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Segregation of HLA genes in multicase narcolepsy families

Mayer

Lattermann

Mueller‐Eckhardt

et al. 1998

Journal of Sleep Research

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SUMMARYIn the past 15 years, 411 sporadic narcolepsy patients have been diagnosed in the Hephata Klinik, Schwalmstadt, Germany. They were explored for presence or absence of excessive daytime sleepiness and narcolepsy in their relatives. A subset of 39 patients were explored for presence or absence of parasomnias. Six patients had more than one relative affected by narcolepsy-cataplexy. Forty-seven family members were investigated with the Stanford Center for Narcolepsy Sleep Inventory and a standardized parasomnia questionnaire. Twenty-four relatives had nocturnal polysomnographies and Multiple Sleep Latency Tests. HLA class I typing was performed in all sporadic and familial cases, class II and microsatellite typing was performed in all members of multicase families. Based on the Finnish prevalence study by Hublin et al., 1994, the relative risk for first degree relatives to develop narcolepsy-cataplexy was in our sample 16.5, 34.2 for excessive daytime sleepiness and 426.9 for parasomnias. Cataplexy, excessive daytime sleepiness and single narcoleptic symptoms in the multicase families segregate with the DRB1 * 1501, CARII:200, CARI: 103, DQB1 * 0602 haplotype. In two families, members with narcolepsy and isolated symptoms have inherited the DRB1 * 1501/DQB1 * 0602 haplotype from the nonaffected parent. The observed segregations in these two families may support the view that narcoleptic symptoms are expressed by DRB1 * 1501/DQB1 * 0602 carriers, independent of haplotype origin. Parasomnias do not segregate with a specific haplotype. The frequency of parasomnias in narcolepsy is much higher than in the general population. The empirical risk for first degree family members of narcolepsy patients to develop cataplexy seems to be low, whereas it is higher for EDS and highest for parasomnias.

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Circadian Temperature and Activity Rhythms in Unmedicated Narcoleptic Patients

Mayer¹,

F²,

Leonhard³

et al. 1997

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Modafinil in Diurnal Sleepiness. A Study of 123 Patients

Laffont

Mayer

Minz

1994

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G Mayer

Selegeline Hydrochloride Treatment in Narcolepsy. A Double-Blind, Placebo-Controlled Study

Bacteriological and Serological Findings in a Further Case of Transfusion-MediatedYersinia enterocoliticaSepsis

Segregation of HLA genes in multicase narcolepsy families

Circadian Temperature and Activity Rhythms in Unmedicated Narcoleptic Patients

Modafinil in Diurnal Sleepiness. A Study of 123 Patients

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