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1. Frequency, morbidity and equity — the case for increased research on male fertility

Author

Kimmins, Sarah, Anderson, Richard A., Barratt, Christopher L. R., Behre, Hermann M., Catford, Sarah R., De Jonge, Christopher J., Delbes, Geraldine, Eisenberg, Michael L., Garrido, Nicolas, Houston, Brendan J., Jørgensen, Niels, Krausz, Csilla, Lismer, Ariane, McLachlan, Robert I., Minhas, Suks, Moss, Tim, Pacey, Allan, Priskorn, Lærke, Schlatt, Stefan, Trasler, Jacquetta, Trasande, Leonardo, Tüttelmann, Frank, Vazquez-Levin, Mónica Hebe, Veltman, Joris A., Zhang, Feng, and O’Bryan, Moira K.

Published
2024
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4. Human fertilization in vivo and in vitro requires the CatSper channel to initiate sperm hyperactivation

Author

Young, Samuel, Schiffer, Christian, Wagner, Alice, Patz, Jannika, Potapenko, Anton, Herrmann, Leonie, Nordhoff, Verena, Pock, Tim, Krallmann, Claudia, Stallmeyer, Birgit, Ropke, Albrecht, Kierzek, Michelina, Biagioni, Cristina, Wang, Tao, Haalck, Lars, Deuster, Dirk, Hansen, Jan N., Wachten, Dagmar, Risse, Benjamin, Behre, Hermann M., Schlatt, Stefan, Kliesch, Sabine, Tuttelmann, Frank, Brenker, Christoph, and Strunker, Timo

Subjects
Infertility, Male -- Risk factors -- Prevention, Fertilization in vitro -- Patient outcomes, Spermatogenesis -- Health aspects, Evidence-based medicine -- Methods, Health care industry
Abstract

The infertility of many couples rests on an enigmatic dysfunction of the man's sperm. To gain insight into the underlying pathomechanisms, we assessed the function of the sperm-specific multisubunit CatSper-channel complex in the sperm of almost 2,300 men undergoing a fertility workup, using a simple motility-based test. We identified a group of men with normal semen parameters but defective CatSper function. These men or couples failed to conceive naturally and upon medically assisted reproduction via intrauterine insemination and in vitro fertilization. Intracytoplasmic sperm injection (ICSI) was, ultimately, required to conceive a child. We revealed that the defective CatSper function was caused by variations in CATSPER genes. Moreover, we unveiled that CatSper-deficient human sperm were unable to undergo hyperactive motility and, therefore, failed to penetrate the egg coat. Thus, our study provides the experimental evidence that sperm hyperactivation is required for human fertilization, explaining the infertility of CatSper-deficient men and the need of ICSI for medically assisted reproduction. Finally, our study also revealed that defective CatSper function and ensuing failure to hyperactivate represents the most common cause of unexplained male infertility known thus far and that this sperm channelopathy can readily be diagnosed, enabling future evidence-based treatment of Affected couples., Introduction Infertility is on the rise, but the underlying causes still remain mostly unknown. In fact, for about a third of infertile men, semen parameters are within reference limits (normozoospermia) [...]

Published
2024
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5. European Academy of Andrology (EAA): Report of activities in 2023.

Author

Rajpert‐De Meyts, Ewa and Behre, Hermann M.

Subjects
*MALE reproductive organs, *MALE reproductive health, *GERM cell tumors, *MEDICAL personnel, *SEMEN analysis, *VARICOCELE, TESTIS surgery
Abstract

The European Academy of Andrology (EAA) merged with the International Network of Young Researchers in Andrology (NYRA) in 2023, benefiting both organizations. The EAA held various educational events, including Schools in Ultrasound, Microsurgery, and Semen Analysis. The EAA also accredited a new Andrology Training Center in Doha, Qatar, and re-accredited several existing centers. Andrology, the official journal of EAA and ASA, celebrated its second decade with a high impact factor and published important guidelines and thematic issues. [Extracted from the article]

Published
2024
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6. Hormonal male contraception.

Author

Wang, Christina, Meriggiola, Maria Cristina, Behre, Hermann M., and Page, Stephanie T.

Subjects
GONADOTROPIN releasing hormone, MALE contraceptives, CONTRACEPTION, ANABOLIC steroids, LUTEINIZING hormone
Abstract

Introduction: Male contraception with exogenously administered hormones suppresses both luteinizing hormone and follicle stimulating hormone leading to low intratesticular testosterone concentration. This results in reversible suppression of spermatogenesis and marked decrease in sperm output in the ejaculate and preventing pregnancy in the female partner. Prior Studies: Studies of testosterone administered alone or in combination of another gonadotropin suppressive agent such as a progestin or gonadotropin releasing hormone (GnRH) analog showed decisively that the exogenous hormone administrations are effective in suppressing sperm output with few adverse events that are not anticipated. In contraceptive efficacy studies, testosterone alone or combined with a progestin are as effective in preventing pregnancies as female contraceptive methods. Conclusion: Hormone combinations for male contraception are in late‐phase clinical trials and hold the promise of being the new, reversible contraception method for men in over half a century. Lessons learned from the male hormonal contraceptive development pave the way for new targeted approached to regulate male fertility. [ABSTRACT FROM AUTHOR]

Published
2024
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7. Practice and development of male contraception: European Academy of Andrology and American Society of Andrology guidelines.

Author

Wang, Christina, Meriggiola, Maria Cristina, Amory, John K., Barratt, Christopher L. R., Behre, Hermann M., Bremner, William J., Ferlin, Alberto, Honig, Stanton, Kopa, Zsolt, Lo, Kirk, Nieschlag, Eberhard, Page, Stephanie T., Sandlow, Jay, Sitruk‐Ware, Regine, Swerdloff, Ronald S., Wu, Frederick C. W., and Goulis, Dimitrios G.

Subjects
CONTRACEPTION, UNPLANNED pregnancy, MALE contraceptives, SEMEN analysis, FAMILY planning
Abstract

Backgrounds: Despite a wide spectrum of contraceptive methods for women, the unintended pregnancy rate remains high (45% in the US), with 50% resulting in abortion. Currently, 20% of global contraceptive use is male‐directed, with a wide variation among countries due to limited availability and lack of efficacy. Worldwide studies indicate that >50% of men would opt to use a reversible method, and 90% of women would rely on their partner to use a contraceptive. Additional reasons for novel male contraceptive methods to be available include the increased life expectancy, sharing the reproductive risks among partners, social issues, the lack of pharma industry involvement and the lack of opinion makers advocating for male contraception. Aim: The present guidelines aim to review the status regarding male contraception, the current state of the art to support the clinical practice, recommend minimal requirements for new male contraceptive development and provide and grade updated, evidence‐based recommendations from the European Society of Andrology (EAA) and the American Society of Andrology (ASA). Methods: An expert panel of academicians appointed by the EAA and the ASA generated a consensus guideline according to the GRADE (Grading of Recommendations, Assessment, Development and Evaluation) system. Results: Sixty evidence‐based and graded recommendations were produced on couple‐centered communication, behaviors, barrier methods, semen analysis and contraceptive efficacy, physical agents, surgical methods, actions before initiating male contraception, hormonal methods, non‐hormonal methods, vaccines, and social and ethical considerations. Conclusion: As gender roles transform and gender equity is established in relationships, the male contribution to family planning must be facilitated. Efficient and safe male‐directed methods must be evaluated and introduced into clinical practice, preferably reversible, either hormonal or non‐hormonal. From a future perspective, identifying new hormonal combinations, suitable testicular targets, and emerging vas occlusion methods will produce novel molecules and products for male contraception. [ABSTRACT FROM AUTHOR]

Published
2024
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8. The sperm-specific K+ channel Slo3 is inhibited by albumin and steroids contained in reproductive fluids.

Author

Lorenz, Johannes, Eisenhardt, Clara, Mittermair, Teresa, Kulle, Alexandra E., Holterhus, Paul Martin, Fobker, Manfred, Boenigk, Wolfgang, Nordhoff, Verena, Behre, Hermann M., Strünker, Timo, and Brenker, Christoph

Subjects
GENITALIA, OPTICAL modulation, ION channels, SPERMATOZOA, OVIDUCT
Abstract

To locate and fertilize the egg, sperm probe the varying microenvironment prevailing at different stages during their journey across the female genital tract. To this end, they are equipped with a unique repertoire of mostly sperm-specific proteins. In particular, the flagellar Ca2+ channel CatSper has come into focus as a polymodal sensor used by human sperm to register ligands released into the female genital tract. Here, we provide the first comprehensive study on the pharmacology of the sperm-specific human Slo3 channel, shedding light on its modulation by reproductive fluids and their constituents. Weshow that seminal fluid and contained prostaglandins and Zn2+ do not affect the channel, whereas human Slo3 is inhibited in a non-genomic fashion by diverse steroids as well as by albumin, which are released into the oviduct along with the egg. This indicates that not only CatSper but also Slo3 harbours promiscuous ligandbinding sites that can accommodate structurally diverse molecules, suggesting that Slo3 is involved in chemosensory signalling in human sperm. [ABSTRACT FROM AUTHOR]

Published
2024
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9. Identification of two hidden clinical subgroups among men with idiopathic cryptozoospermia.

Author

Schülke, Lena Charlotte, Wistuba, Joachim, Nordhoff, Verena, Behre, Hermann M, Cremers, Jann-Frederik, Kliesch, Sabine, Persio, Sara Di, and Neuhaus, Nina

Subjects
SPERMATOGENESIS, MALE infertility, SERTOLI cells, OPEN access publishing, SEMINIFEROUS tubules, REPRODUCTIVE technology, PRINCIPAL components analysis
Abstract

STUDY QUESTION Are there subgroups among patients with cryptozoospermia pointing to distinct etiologies? SUMMARY ANSWER We reveal two distinct subgroups of cryptozoospermic (Crypto) patients based on testicular tissue composition, testicular volume, and FSH levels. WHAT IS KNOWN ALREADY Cryptozoospermic patients present with a sperm concentration below 0.1 million/ml. While the etiology of the severely impaired spermatogenesis remains largely unknown, alterations of the spermatogonial compartment have been reported including a reduction of the reserve stem cells in these patients. STUDY DESIGN, SIZE, DURATION To assess whether there are distinct subgroups among cryptozoospermic patients, we applied the statistical method of cluster analysis. For this, we retrospectively selected 132 cryptozoospermic patients from a clinical database who underwent a testicular biopsy in the frame of fertility treatment at a university hospital. As controls (Control), we selected 160 patients with obstructive azoospermia and full spermatogenesis. All 292 patients underwent routine evaluation for endocrine, semen, and histological parameters (i.e. the percentage of tubules with elongated spermatids). Moreover, outcome of medically assisted reproduction (MAR) was assessed for cryptozoospermic (n = 73) and Control patients (n = 87), respectively. For in-depth immunohistochemical and histomorphometrical analyses, representative tissue samples from cryptozoospermic (n = 27) and Control patients (n = 12) were selected based on cluster analysis results and histological parameters. PARTICIPANTS/MATERIALS, SETTING, METHODS This study included two parts: firstly using clinical parameters of the entire cohort of 292 patients, we performed principal component analysis (PCA) followed by hierarchical clustering on principal components (i.e. considering hormonal values, ejaculate parameters, and histological information). Secondly, for histological analyses seminiferous tubules were categorized according to the most advanced germ cell type present in sections stained with Periodic acid Schif. On the selected cohort of 39 patients (12 Control, 27 cryptozoospermic), we performed immunohistochemistry for spermatogonial markers melanoma-associated antigen 4 (MAGEA4) and piwi like RNA-mediated gene silencing 4 (PIWIL4) followed by quantitative analyses. Moreover, the morphologically defined Adark spermatogonia, which are considered to be the reserve stem cells, were quantified. MAIN RESULTS AND THE ROLE OF CHANCE The PCA and hierarchical clustering revealed three different clusters, one of them containing all Control samples. The main factors driving the sorting of patients to the clusters were the percentage of tubules with elongated spermatids (Cluster 1, all Control patients and two cryptozoospermic patients), the percentage of tubules with spermatocytes (Cluster 2, cryptozoospermic patients), and tubules showing a Sertoli cells only phenotype (Cluster 3, cryptozoospermic patients). Importantly, the percentage of tubules containing elongated spermatids was comparable between Clusters 2 and 3. Additional differences were higher FSH levels (P  < 0.001) and lower testicular volumes (P  < 0.001) in Cluster 3 compared to Cluster 2. In the spermatogonial compartment of both cryptozoospermic Clusters, we found lower numbers of MAGEA4+ and Adark spermatogonia but higher proportions of PIWIL4+ spermatogonia, which were significantly correlated with a lower percentage of tubules containing elongated spermatids. In line with this common alteration, the outcome of MAR was comparable between Controls as well as both cryptozoospermic Clusters. LIMITATIONS, REASONS FOR CAUTION While we have uncovered the existence of subgroups within the cohort of cryptozoospermic patients, comprehensive genetic analyses remain to be performed to unravel potentially distinct etiologies. WIDER IMPLICATIONS OF THE FINDINGS The novel insight that cryptozoospermic patients can be divided into two subgroups will facilitate the strategic search for underlying genetic etiologies. Moreover, the shared alterations of the spermatogonial stem cell compartment between the two cryptozoospermic subgroups could represent a general response mechanism to the reduced output of sperm, which may be associated with a progressive phenotype. This study therefore offers novel approaches towards the understanding of the etiology underlying the reduced sperm formation in cryptozoospermic patients. STUDY FUNDING/COMPETING INTEREST(S) German research foundation CRU 326 (grants to: SDP, NN). Moreover, we thank the Faculty of Medicine of the University of Münster for the financial support of Lena Charlotte Schülke through the MedK-program. We acknowledge support from the Open Access Publication Fund of the University of Münster. The authors have no potential conflicts of interest. TRIAL REGISTRATION NUMBER N/A. [ABSTRACT FROM AUTHOR]

Published
2024
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10. Leading at the vanguard of andrology: The Network for Young Researchers in Andrology joins forces with the European Academy of Andrology.

Author

de la Iglesia, Alberto, Egeberg, Dorte L., Marcu, Daniel, Richer, Guillaume, Houston, Brendan J., Ammar, Omar, Saritas, Gülizar, Delgouffe, Emily, Jezek, Davor, Krausz, Csilla, Rajpert‐De Meyts, Ewa, and Behre, Hermann M.

Subjects
RESEARCH personnel, ANDROLOGY, MALE infertility
Abstract

The Network for Young Researchers in Andrology (NYRA) was founded in 2006 with the goal of creating safe spaces for early-stage researchers to exchange scientific advances and promote networking in the field of male reproductive health. Over the years, NYRA has evolved and rebranded, and it has become a dynamic organization with board members from around the world. NYRA collaborates closely with the European Academy of Andrology (EAA) and has now merged with the EAA, becoming its "young arm." This merger aims to support the development of educational and scientific activities in andrology and provide mutual benefits for both organizations. The NYRA-EAA merger has already introduced a reduced registration fee for younger members, allowing them to access EAA membership benefits. The NYRA board and EAA Executive Council are excited about the future and the opportunities this merger will bring for the andrology community. [Extracted from the article]

Published
2024
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12. Quality of Life and Sexual Function Benefits of Long-Term Testosterone Treatment: Longitudinal Results From the Registry of Hypogonadism in Men (RHYME)

Author

Maggi, M., Behre, H.M., Meuleman, E., Dohle, G., Arver, S., Wu, F., Porst, H., Jones, T.H., Quinton, R., Lenzi, A., Bouloux, P.-M., Morales, A.M., Hackett, G., Stroberg, P., Maggio, M., Cruz, N., Balercia, G., Yassin, A., Reisman, C., Bassas, L., Pescatori, E., Salamanca, J.I. Martinez, Otero, J. Romero, Jockenhoevel, F., Debruyne, F., Rosen, Raymond C., Wu, Frederick, Behre, Hermann M., Porst, Hartmut, Meuleman, Eric J.H., Maggi, Mario, Romero-Otero, Javier, Martinez-Salamanca, Juan I., Jones, Thomas Hugh, Debruyne, Frans M.J., Kurth, Karl-Heinz, Hackett, Geoff I., Quinton, Richard, Stroberg, Peter, Reisman, Yacov, Pescatori, Edoardo S., Morales, Antonio, Bassas, Lluis, Cruz, Natalio, Cunningham, Glenn R., and Wheaton, Olivia A.

Published
2017
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13. The human sperm proteome—Toward a panel for male fertility testing.

Author

Greither, Thomas, Dejung, Mario, Behre, Hermann M., Butter, Falk, and Herlyn, Holger

Subjects
FERTILITY, Y chromosome, SPERMATOZOA, HUMAN fertility, MALE infertility, INFERTILITY
Abstract

Background: Although male factor accounts for 40%–50% of unintended childlessness, we are far from fully understanding the detailed causes. Usually, affected men cannot even be provided with a molecular diagnosis. Objectives: We aimed at a higher resolution of the human sperm proteome for better understanding of the molecular causes of male infertility. We were particularly interested in why reduced sperm count decreases fertility despite many normal‐looking spermatozoa and which proteins might be involved. Material and methods: Applying mass spectrometry analysis, we qualitatively and quantitatively examined the proteomic profiles of spermatozoa from 76 men differing in fertility. Infertile men had abnormal semen parameters and were involuntarily childless. Fertile subjects exhibited normozoospermia and had fathered children without medical assistance. Results: We discovered proteins from about 7000 coding genes in the human sperm proteome. These were mainly known for involvements in cellular motility, response to stimuli, adhesion, and reproduction. Numbers of sperm proteins showing at least threefold deviating abundances increased from oligozoospermia (N = 153) and oligoasthenozoospermia (N = 154) to oligoasthenoteratozoospermia (N = 368). Deregulated sperm proteins primarily engaged in flagellar assembly and sperm motility, fertilization, and male gametogenesis. Most of these participated in a larger network of male infertility genes and proteins. Discussion: We expose 31 sperm proteins displaying deviant abundances under infertility, which already were known before to have fertility relevance, including ACTL9, CCIN, CFAP47, CFAP65, CFAP251 (WDR66), DNAH1, and SPEM1. We propose 18 additional sperm proteins with at least eightfold differential abundance for further testing of their diagnostic potential, such as C2orf16, CYLC1, SPATA31E1, SPATA31D1, SPATA48, EFHB (CFAP21), and FAM161A. Conclusion: Our results shed light on the molecular background of the dysfunctionality of the fewer spermatozoa produced in oligozoospermia and syndromes including it. The male infertility network presented may prove useful in further elucidating the molecular mechanism of male infertility. [ABSTRACT FROM AUTHOR]

Published
2023
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17. Testosterone treatment is not associated with increased risk of prostate cancer or worsening of lower urinary tract symptoms: prostate health outcomes in the Registry of Hypogonadism in Men

Author

Debruyne, Frans M.J., Behre, Hermann M., Roehrborn, Claus G., Maggi, Mario, Wu, Frederick C.W., Schröder, Fritz H., Jones, Thomas Hugh, Porst, Hartmut, Hackett, Geoffrey, Wheaton, Olivia A., Martin-Morales, Antonio, Meuleman, Eric, Cunningham, Glenn R., Divan, Hozefa A., Rosen, Raymond C., Dohle, G., Arver, S., Lenzi, A., Stroberg, P., Maggio, M., Cruz, N., Balercia, G., Yassin, A., Reisman, C., Bassa, L., Pescatori, E., Salamanca, Martinez J.I., Otero, Romero J., and Jockenhoevel, F.

Published
2017
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19. Genome-Wide Association Screening Determines Peripheral Players in Male Fertility Maintenance.

Author

Greither, Thomas, Behre, Hermann M., and Herlyn, Holger

Subjects
*GENOME-wide association studies, *HEREDITY, *FERTILITY, *HUMAN fertility, *SINGLE nucleotide polymorphisms, *MALE infertility, *PHENOTYPES, *GENETIC sex determination
Abstract

Deciphering the functional relationships of genes resulting from genome-wide screens for polymorphisms that are associated with phenotypic variations can be challenging. However, given the common association with certain phenotypes, a functional link should exist. We have tested this prediction in newly sequenced exomes of altogether 100 men representing different states of fertility. Fertile subjects presented with normal semen parameters and had naturally fathered offspring. In contrast, infertile probands were involuntarily childless and had reduced sperm quantity and quality. Genome-wide association study (GWAS) linked twelve non-synonymous single-nucleotide polymorphisms (SNPs) to fertility variation between both cohorts. The SNPs localized to nine genes for which previous evidence is in line with a role in male fertility maintenance: ANAPC1, CES1, FAM131C, HLA-DRB1, KMT2C, NOMO1, SAA1, SRGAP2, and SUSD2. Most of the SNPs residing in these genes imply amino acid exchanges that should only moderately affect protein functionality. In addition, proteins encoded by genes from present GWAS occupied peripheral positions in a protein–protein interaction network, the backbone of which consisted of genes listed in the Online Mendelian Inheritance in Man (OMIM) database for their implication in male infertility. Suggestive of an indirect impact on male fertility, the genes focused were indeed linked to each other, albeit mediated by other interactants. Thus, the chances of identifying a central player in male infertility by GWAS could be limited in general. Furthermore, the SNPs determined and the genes containing these might prove to have potential as biomarkers in the diagnosis of male fertility. [ABSTRACT FROM AUTHOR]

Published
2023
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21. The European Academy of Andrology (EAA) ultrasound study on healthy, fertile men: An overview on male genital tract ultrasound reference ranges.

Author

Lotti, Francesco, Frizza, Francesca, Balercia, Giancarlo, Barbonetti, Arcangelo, Behre, Hermann M., Calogero, Aldo E., Cremers, Jann‐Frederik, Francavilla, Felice, Isidori, Andrea M., Kliesch, Sabine, La Vignera, Sandro, Lenzi, Andrea, Marcou, Marios, Pilatz, Adrian, Poolamets, Olev, Punab, Margus, Godoy, Maria Fernanda Peraza, Quintian, Claudia, Rajmil, Osvaldo, and Salvio, Gianmaria

Subjects
MALE reproductive organs, SEMINAL vesicles, VAS deferens, ENDORECTAL ultrasonography, ULTRASONIC imaging
Abstract

Background: So far, male genital tract color‐Doppler ultrasound (MGT‐CDUS) was not standardized. Recently, the European Academy of Andrology (EAA) published the results of a multicenter study assessing the CDUS characteristics of healthy‐fertile men (HFM) to obtain normative parameters. Objectives: To report the EAA US study (i) standard operating procedures (SOPs) for assessing MGT‐CDUS, (ii) main MGT‐CDUS normative parameters, and (iii) compare the EAA and previously published "normal" CDUS values. Methods: A cohort of 248 HFM (35.3 ± 5.9 years) was studied, evaluating MGT‐CDUS before and after ejaculation following SOPs. Results: SOPs for MGT‐CDUS assessment are summarized here. All subjects underwent scrotal CDUS and 188 men underwent transrectal ultrasound before and after ejaculation. The main CDUS reference ranges and characteristics of the HFM‐MGT are reported here. The mean testicular volume was ∼17 mL. The lower limit for right and left testis was 12 and 11 mL, defining testicular hypotrophy. The upper limit for epididymal head, body, tail, and vas deferens was 11.5, 5, 6, and 4.5 mm, respectively. Testicular and epididymal arterial reference ranges are reported. The EAA varicocoele classification is reported. CDUS‐varicocoele was detected in ∼37% of men. Prostate mean volume was ∼25 mL, while lower and upper limits were 15 and 35 mL, defining hypotrophy and enlargement, respectively. Prostate arterial reference ranges are reported. Prostate calcifications and inhomogeneity were frequent; midline prostatic cysts were rare and small. Ejaculatory duct abnormalities were absent. The upper limit for periprostatic venous plexus was 4.5 mm. Lower and upper limits of seminal vesicles (SV) anterior–posterior diameter were 6 and 16 mm, defining hypotrophy or dilation, respectively. Seminal vesicle volume and ejection fraction reference ranges are reported. SV‐US abnormalities were rare. Deferential ampullas upper limit was 6 mm. A discussion on the EAA and previously published "normal" CDUS values is reported here. Conclusions: The EAA findings will help in reproductive and general male health management. [ABSTRACT FROM AUTHOR]

Published
2022
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22. The European Academy of Andrology (EAA) ultrasound study on healthy, fertile men: Prostate‐vesicular transrectal ultrasound reference ranges and associations with clinical, seminal and biochemical characteristics.

Author

Lotti, Francesco, Frizza, Francesca, Balercia, Giancarlo, Barbonetti, Arcangelo, Behre, Hermann M., Calogero, Aldo E., Cremers, Jann‐Frederik, Francavilla, Felice, Isidori, Andrea M., Kliesch, Sabine, La Vignera, Sandro, Lenzi, Andrea, Marcou, Marios, Pilatz, Adrian, Poolamets, Olev, Punab, Margus, Godoy, Maria Fernanda Peraza, Quintian, Claudia, Rajmil, Osvaldo, and Salvio, Gianmaria

Subjects
ENDORECTAL ultrasonography, RECURRENT miscarriage, MALE infertility, ANDROLOGY, SEMINAL vesicles, ULTRASONIC imaging, PROSTATE hypertrophy
Abstract

Background: Transrectal ultrasound (TRUS) parameters are not standardized, especially in men of reproductive age. Hence, the European Academy of Andrology (EAA) promoted a multicenter study to assess the TRUS characteristics of healthy‐fertile men (HFM) to establish normative parameters. Objectives: To report and discuss the prostate and seminal vesicles (SV) reference ranges and characteristics in HFM and their associations with clinical, seminal, biochemical parameters. Methods: 188 men (35.6 ± 6.0 years) from a cohort of 248 HFM were studied, evaluating, on the same day, clinical, biochemical, seminal, TRUS parameters following Standard Operating Procedures. Results: TRUS reference ranges and characteristics of the prostate and SV of HFM are reported herein. The mean PV was ∼25 ml. PV lower and upper limits were 15 and 35 ml, defining prostate hypotrophy and enlargement, respectively. PV was positively associated with age, waistline, current smoking (but not with T levels), seminal volume (and negatively with seminal pH), prostate inhomogeneity, macrocalcifications, calcification size and prostate arterial parameters, SV volume before and after ejaculation, deferential and epididymal size. Prostate calcifications and inhomogeneity were frequent, while midline prostatic cysts were rare and small. Ejaculatory duct abnormalities were absent. Periprostatic venous plexus size was positively associated with prostate calcifications, SV volume and arterial peak systolic velocity. Lower and upper limits of SV anterior‐posterior diameter after ejaculation were 6 and 16 mm, defining SV hypotrophy or dilation, respectively. SV total volume before ejaculation and delta SV total volume (DSTV) positively correlated with ejaculate volume, and DSTV correlated positively with sperm progressive motility. SV total volume after ejaculation was associated negatively with SV ejection fraction and positively with distal ampullas size. SV US abnormalities were rare. No association between TRUS and time to pregnancy, number of children or history of miscarriage was observed. Conclusions: The present findings will help in better understanding male infertility pathophysiology and the meaning of specific TRUS findings. [ABSTRACT FROM AUTHOR]

Published
2022
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23. Corifollitropin Alfa Combined With Human Chorionic Gonadotropin in Adolescent Boys With Hypogonadotropic Hypogonadism.

Author

Shankar, R. Ravi, Shah, Suneri, Hee-Koung Joeng, Mendizabal, Geraldine, DiBello, Julia R., Guan, Yanfen, Stegmann, Barbara J., Nieschlag, Eberhard, Behre, Hermann M., Swerdloff, Ronald S., Fox, Michelle C., and Kaufman, Keith D.

Subjects
HYPOGONADISM, TESTOSTERONE
Abstract

Context: Adolescent males with hypogonadotropic hypogonadism (HH) have traditionally been treated with exogenous testosterone (T) or human chorionic gonadotropin (hCG) to produce virilization; however, those modalities do not result in growth of the testes and may promote premature maturation and terminal differentiation of Sertoli cells prior to their proliferation, which may impact future fertility. Another option is to use gonadotropins in those individuals to induce testicular growth, proliferation and maturation of Sertoli cells, and production of endogenous T with consequent virilization. Objective: We examined the efficacy and safety of corifollitropin alfa (CFA) combined with hCG for the induction of testicular growth and pubertal development in adolescent boys with HH. Methods: This was a 64-week, multicenter, open-label, single-group study of CFA in adolescent boys, aged 14 to younger than 18 years, with HH. Seventeen participants initiated a 12-week priming period with CFA (100 μg if weight ≤ 60 kg, or 150 μg if weight > 60 kg) given subcutaneously once every 2 weeks, after which they entered a 52-week combined treatment period with CFA, once every 2 weeks, and subcutaneous hCG, twice-weekly (hCG dose adjusted between 500 IU and 5000 IU to keep total T and estradiol levels within protocol-specified ranges). The primary efficacy end point was change from baseline in testicular volume (TV), measured as the sum of volumes of left and right testes by ultrasound. Results: After 64 weeks of therapy with CFA/CFA combined with hCG, geometric mean fold increase from baseline in TV was 9.43 (95% CI, 7.44-11.97) (arithmetic mean of change from baseline at week 64, 13.0 mL). Hormonal, Tanner stage, and growth velocity changes were consistent with initiation and progression of puberty. Treatment was generally well tolerated. No participant developed anti-CFA antibodies. Conclusion: Treatment of adolescent boys with HH with CFA alone for 12 weeks followed by CFA combined with hCG for 52 weeks induced testicular growth accompanied by pubertal progression, increased T, and a pubertal growth spurt (EudraCT: 2015-001878-18). [ABSTRACT FROM AUTHOR]

Published
2022
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30. Effect of Genetic Variants of Gonadotropins and Their Receptors on Ovarian Stimulation Outcomes: A Delphi Consensus.

Author

Conforti, Alessandro, Tüttelmann, Frank, Alviggi, Carlo, Behre, Hermann M., Fischer, Robert, Hu, Liang, Polyzos, Nikolaos P., Chuderland, Dana, Rama Raju, Gottumukkala Achyuta, D'Hooghe, Thomas, Simoni, Manuela, Sunkara, Sesh K., and Longobardi, Salvatore

Subjects
INDUCED ovulation, GENETIC variation, OVARIAN hyperstimulation syndrome, SINGLE nucleotide polymorphisms, REPRODUCTIVE technology
Abstract

Background: A Delphi consensus was conducted to evaluate the influence of single nucleotide polymorphisms (SNPs) in genes encoding gonadotropin and gonadotropin receptors on clinical ovarian stimulation outcomes following assisted reproductive technology (ART) treatment. Methods: Nine experts plus two Scientific Coordinators discussed and amended statements plus supporting references proposed by the Scientific Coordinators. The statements were distributed via an online survey to 36 experts, who voted on their level of agreement or disagreement with each statement. Consensus was reached if the proportion of participants agreeing or disagreeing with a statement was >66%. Results: Eleven statements were developed, of which two statements were merged. Overall, eight statements achieved consensus and two statements did not achieve consensus. The statements reaching consensus are summarized here. (1) SNP in the follicle stimulating hormone receptor (FSHR), rs6166 (c.2039A>G, p.Asn680Ser) (N=5 statements): Ser/Ser carriers have higher basal FSH levels than Asn/Asn carriers. Ser/Ser carriers require higher amounts of gonadotropin during ovarian stimulation than Asn/Asn carriers. Ser/Ser carriers produce fewer oocytes during ovarian stimulation than Asn/Asn or Asn/Ser carriers. There is mixed evidence supporting an association between this variant and ovarian hyperstimulation syndrome. (2) SNP of FSHR , rs6165 (c.919G>A, p.Thr307Ala) (N=1 statement): Few studies suggest Thr/Thr carriers require a shorter duration of gonadotropin stimulation than Thr/Ala or Ala/Ala carriers. (3) SNP of FSHR , rs1394205 (−29G>A) (N=1 statement): Limited data in specific ethnic groups suggest that A/A allele carriers may require higher amounts of gonadotropin during ovarian stimulation and produce fewer oocytes than G/G carriers. (4) SNP of FSH β-chain (FSHB), rs10835638 (−211G>T) (N=1 statement): There is contradictory evidence supporting an association between this variant and basal FSH levels or oocyte number. (5) SNPs of luteinizing hormone β-chain (LHB) and LH/choriogonadotropin receptor (LHCGR) genes (N=1 statement): these may influence ovarian stimulation outcomes and could represent potential future targets for pharmacogenomic research in ART, although data are still very limited. Conclusions: This Delphi consensus provides clinical perspectives from a diverse international group of experts. The consensus supports a link between some variants in gonadotropin/gonadotropin receptor genes and ovarian stimulation outcomes; however, further research is needed to clarify these findings. [ABSTRACT FROM AUTHOR]

Published
2022
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31. Male Hormonal Contraception: A Double-Blind, Placebo-Controlled Study

Author

Mommers, Ellen, Kersemaekers, Wendy M., Elliesen, Jörg, Kepers, Marc, Apter, Dan, Behre, Hermann M., Beynon, Jennifer, Bouloux, Pierre M., Costantino, Antonietta, Gerbershagen, Hans-Peter, Grønlund, Lars, Heger-Mahn, Doris, Huhtaniemi, Ilpo, Koldewijn, Evert L., Lange, Corinna, Lindenberg, Svend, Meriggiola, M Cristina, Meuleman, Eric, Mulders, Peter F. A., Nieschlag, Eberhard, Perheentupa, Antti, Solomon, Andrew, Väisälä, Leena, Wu, Frederick C., and Zitzmann, Michael

Published
2008

38. Fertility Relevance Probability Analysis Shortlists Genetic Markers for Male Fertility Impairment.

Author

Greither, Thomas, Schumacher, Julia, Dejung, Mario, Behre, Hermann M., Zischler, Hans, Butter, Falk, and Herlyn, Holger

Subjects
HUMAN fertility, GENETIC markers, LOGISTIC regression analysis, MALE infertility, KNOCKOUT mice, SPERMATOGENESIS
Abstract

Impairment of male fertility is one of the major public health issues worldwide. Nevertheless, genetic causes of male sub- and infertility can often only be suspected due to the lack of reliable and easy-to-use routine tests. Yet, the development of a marker panel is complicated by the large quantity of potentially predictive markers. Actually, hundreds or even thousands of genes could have fertility relevance. Thus, a systematic method enabling a selection of the most predictive markers out of the many candidates is required. As a criterion for marker selection, we derived a gene-specific score, which we refer to as fertility relevance probability (FRP). For this purpose, we first categorized 2,753 testis-expressed genes as either candidate markers or non-candidates, according to phenotypes in male knockout mice. In a parallel approach, 2,502 genes were classified as candidate markers or non-candidates based on phenotypes in men. Subsequently, we conducted logistic regression analyses with evolutionary rates of genes (dN/dS), transcription levels in testis relative to other organs, and connectivity of the encoded proteins in a protein-protein interaction network as covariates. In confirmation of the procedure, FRP values showed the expected pattern, thus being overall higher in genes with known relevance for fertility than in their counterparts without corresponding evidence. In addition, higher FRP values corresponded with an increased dysregulation of protein abundance in spermatozoa of 37 men with normal and 38 men with impaired fertility. Present analyses resulted in a ranking of genes according to their probable predictive power as candidate markers for male fertility impairment. Thus, AKAP4, TNP1, DAZL, BRDT, DMRT1, SPO11, ZPBP, HORMAD1, and SMC1B are prime candidates toward a marker panel for male fertility impairment. Additional candidate markers are DDX4, SHCBP1L, CCDC155, ODF1, DMRTB1, ASZ1, BOLL, FKBP6, SLC25A31, PRSS21, and RNF17. FRP inference additionally provides clues for potential new markers, thereunder TEX37 and POU4F2. The results of our logistic regression analyses are freely available at the PreFer Genes website (https://prefer-genes.uni-mainz.de/). [ABSTRACT FROM AUTHOR]

Published
2020
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39. The European Academy of Andrology (EAA) ultrasound study on healthy, fertile men: clinical, seminal and biochemical characteristics.

Author

Lotti, Francesco, Frizza, Francesca, Balercia, Giancarlo, Barbonetti, Arcangelo, Behre, Hermann M., Calogero, Aldo E., Cremers, Jann‐Frederik, Francavilla, Felice, Isidori, Andrea M., Kliesch, Sabine, La Vignera, Sandro, Lenzi, Andrea, Marcou, Marios, Pilatz, Adrian, Poolamets, Olev, Punab, Margus, Peraza Godoy, Maria Fernanda, Rajmil, Osvaldo, Salvio, Gianmaria, and Shaeer, Osama

Subjects
MALE reproductive organs, ANDROLOGY, EJACULATION, SPERMATOZOA, SEMEN
Abstract

Background: Infertility affects 7%‐12% of men, and its etiology is unknown in half of cases. To fill this gap, use of the male genital tract color‐Doppler ultrasound (MGT‐CDUS) has progressively expanded. However, MGT‐CDUS still suffers from lack of standardization. Hence, the European Academy of Andrology (EAA) has promoted a multicenter study ("EAA ultrasound study") to assess MGT‐CDUS characteristics of healthy, fertile men to obtain normative parameters. Objectives: To report (a) the development and methodology of the "EAA ultrasound study," (b) the clinical characteristics of the cohort of healthy, fertile men, and (c) the correlations of both fertility history and seminal features with clinical parameters. Methods: A cohort of 248 healthy, fertile men (35.3 ± 5.9 years) was studied. All subjects were asked to undergo, within the same day, clinical, biochemical, and seminal evaluation and MGT‐CDUS before and after ejaculation. Results: The clinical, seminal, and biochemical characteristics of the cohort have been reported here. The seminal characteristics were consistent with those reported by the WHO (2010) for the 50th and 5th centiles for fertile men. Normozoospermia was observed in 79.6% of men, while normal sperm vitality was present in almost the entire sample. Time to pregnancy (TTP) was 3.0[1.0‐6.0] months. TTP was negatively correlated with sperm vitality (Adj.r =−.310, P =.011), but not with other seminal, clinical, or biochemical parameters. Sperm vitality and normal morphology were positively associated with fT3 and fT4 levels, respectively (Adj.r =.244, P <.05 and Adj.r =.232, P =.002). Sperm concentration and total count were negatively associated with FSH levels and positively, along with progressive motility, with mean testis volume (TV). Mean TV was 20.4 ± 4.0 mL, and the lower reference values for right and left testes were 15.0 and 14.0 mL. Mean TV was negatively associated with gonadotropin levels and pulse pressure. Varicocoele was found in 33% of men. Conclusions: The cohort studied confirms the WHO data for all semen parameters and represents a reference with which to assess MGT‐CDUS normative parameters. [ABSTRACT FROM AUTHOR]

Published
2020
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40. MiR-130a in the adipogenesis of human SGBS preadipocytes and its susceptibility to androgen regulation.

Author

Greither, Thomas, Wenzel, Carina, Jansen, Julia, Kraus, Matthias, Wabitsch, Martin, and Behre, Hermann M.

Subjects
ADIPOGENESIS, ANDROGENS, MESENCHYMAL stem cells, ANDROGEN receptors
Abstract

Objectives: Adipogenesis is the differentiation process generating mature adipocytes from undifferentiated mesenchymal stem cells. The differentiation can be inhibited by androgens, although knowledge about intracellular effectors of this inhibition is scarce. Recently, androgen-regulated microRNAs were detected as interesting candidates in this context. In this study, we analyse the role of miR-130a and miR-301 in the adipogenesis of human SGBS preadipocytes and whether they are prone to androgen regulation. Materials and Methods: microRNA expression during adipogenic differentiation with or without androgen stimulation was measured by qPCR. Putative target genes of miR-130a and miR-301 were identified by target database search and validated in luciferase reporter assays. Results: miR-130a and miR-301 are both significantly downregulated on day 3 and day 5 of adipogenic differentiation in comparison to day 0. Under androgen stimulation, a significant upregulation of miR-130a was detected after 7 days of adipogenesis lasting to day 14, while miR-301 did not change significantly until day 14. Luciferase reporter assays revealed the androgen receptor (AR), adiponectin (ADIPOQ) and tumour necrosis factor alpha (TNFα) as miR-130a target genes. Conclusions: miR-130a is an androgen-regulated microRNA that is downregulated during the early phase of adipogenesis and exerts its functions by regulating AR and ADIPOQ translation. These data may help to identify new signalling pathways associated with the androgen-mediated inhibition of adipogenesis. [ABSTRACT FROM AUTHOR]

Published
2020
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41. Diagnosis and Treatment Before Assisted Reproductive Treatments. Guideline of the DGGG, OEGGG and SGGG (S2k Level, AWMF Register Number 015-085, February 2019) – Part 2, Hemostaseology, Andrology, Genetics and History of Malignant Disease.

Author

Toth, Bettina, Baston-Büst, Dunja Maria, Behre, Hermann M., Bielfeld, Alexandra, Bohlmann, Michael, Bühling, Kai, Dittrich, Ralf, Goeckenjan, Maren, Hancke, Katharina, Kliesch, Sabine, Köhn, Frank-Michael, Krüssel, Jan, Kuon, Ruben, Liebenthron, Jana, Nawroth, Frank, Nordhoff, Verena, Pinggera, Germar-Michael, Rogenhofer, Nina, Rudnik-Schöneborn, Sabine, and Schuppe, Hans-Christian

Published
2019
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42. Diagnosis and Therapy Before Assisted Reproductive Treatments. Guideline of the DGGG, OEGGG and SGGG (S2k Level, AWMF Register Number 015-085, February 2019) – Part 1, Basic Assessment of the Woman.

Author

Toth, Bettina, Baston-Büst, Dunja Maria, Behre, Hermann M, Bielfeld, Alexandra, Bohlmann, Michael, Bühling, Kai, Dittrich, Ralf, Goeckenjan, Maren, Hancke, Katharina, Kliesch, Sabine, Köhn, Frank-Michael, Krüssel, Jan, Kuon, Ruben, Liebenthron, Jana, Nawroth, Frank, Nordhoff, Verena, Pinggera, Germar-Michael, Rogenhofer, Nina, Rudnik-Schöneborn, Sabine, and Schuppe, Hans-Christian

Published
2019
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44. Clinical Use of FSH in Male Infertility.

Author

Behre, Hermann M.

Subjects
MALE infertility, FEMALE infertility, CHILDBIRTH, OLIGOSPERMIA, CLINICAL indications
Abstract

The established clinical indication for FSH use in male infertility is the treatment of patients with hypogonadotropic hypogonadism for stimulation of spermatogenesis that allows the induction of a clinical pregnancy in the female partner and finally the birth of a healthy child. Several clinical studies with urinary, purified, and recombinant FSH preparations in combination with hCG have demonstrated the high treatment efficacy regarding these clinical endpoints. Shortcomings of this hormone therapy are the long duration of treatment, sometimes longer than 2 years, and the inconvenience of injections every second or third day. However, improvements of therapy might be expected with new hormonal treatment options already available for infertility treatment in the female. FSH use for treatment of patients with normogonadotropic idiopathic infertility and oligozoospermia is still considered experimental in most countries. Recent meta-analyses have shown that FSH can significantly increase pregnancy rates in the female partners of these patients, but the effect-size is relatively low. Therefore, predictive factors for treatment success have to be identified, including FSH pharmacogenetics, to select the right normogonadotropic patients with idiopathic infertility for FSH therapy. [ABSTRACT FROM AUTHOR]

Published
2019
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45. Differential Regulation of PIWI-LIKE 2 Expression in Primordial Germ Cell Tumor Cell Lines by Promoter Methylation.

Author

Giebler, Maria, Greither, Thomas, and Behre, Hermann M.

Subjects
TERATOCARCINOMA, PROMOTERS (Genetics), GENETIC regulation
Abstract

PIWI-LIKE 2 , a member of the ARGONAUTE protein family, is exclusively expressed in pre-pachytene and pachytene stages of spermatogenesis. PIWI-LIKE 2 acts in the germ cell development and the silencing of retrotransponsons to maintain the genomic integrity and stem cell character. In the present study we investigated DNA methylation as potential mechanism for the regulation of human PIWI-LIKE 2 expression in cell lines related to spermatozoa precursor cells. We detected a high methylation of the PIWI-LIKE 2 promoter in TCam-2 cells, while in NT2/D1 cells the promoter was hypomethylated. Concordantly, PIWI-LIKE 2 expression is higher in NT2/D1 cells than in TCam-2 cells. By demethylation of the promoter with 5′-Aza-2′-deoxycytidine, PIWI-LIKE 2 expression in TCam-2 was increased, while in NT2/D1 no alterations in PIWI-LIKE 2 expression could be detected. In conclusion, we analyzed the DNA methylation driving PIWI-LIKE 2 expression in undifferentiated germ cell tumors and demonstrated an epigenetic basis for PIWI-LIKE 2 expression in this cell type. [ABSTRACT FROM AUTHOR]

Published
2018
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46. Altered PIWI-LIKE 1 and PIWI-LIKE 2 mRNA expression in ejaculated spermatozoa of men with impaired sperm characteristics.

Author

Giebler, Maria, Greither, Thomas, Müller, Lisa, Mösinger, Carina, and Behre, Hermann M.

Abstract

In about half the cases of involuntary childlessness, a male infertility factor is involved. The PIWI-LIKE genes, a subclade of the Argonaute protein family, are involved in RNA silencing and transposon control in the germline. Knockout of murine Piwi-like 1 and 2 homologs results in complete infertility in males. The aim of this study was to analyze whether the mRNA expression of human PIWI-LIKE 1-4 genes is altered in ejaculated spermatozoa of men with impaired sperm characteristics. Ninety male participants were included in the study, among which 47 were with normozoospermia, 36 with impaired semen characteristics according to the World Health Organization (WHO) manual, 5th edition, and 7 with azoospermia serving as negative control for the PIWI-LIKE 1-4 mRNA expression in somatic cells in the ejaculate. PIWI-LIKE 1-4 mRNA expression in the ejaculated spermatozoa of the participants was measured by quantitative real-time PCR. In nonazoospermic men, PIWI-LIKE 1-4 mRNA was measurable in ejaculated spermatozoa in different proportions. PIWI-LIKE 1 (100.0%) and PIWI-LIKE 2 (49.4%) were more frequently expressed than PIWI-LIKE 3 (9.6%) and PIWI-LIKE 4 (15.7%). Furthermore, a decreased PIWI-LIKE 2 mRNA expression showed a significant correlation with a decreased sperm count ( P = 0.022) and an increased PIWI-LIKE 1 mRNA expression with a decreased progressive motility ( P = 0.048). PIWI-LIKE 1 and PIWI-LIKE 2 mRNA expression exhibited a significant association with impaired sperm characteristics and may be a useful candidate for the evaluation of the impact of PIWI-LIKE 1-4 mRNA expression on male infertility. [ABSTRACT FROM AUTHOR]

Published
2018
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47. An open-label clinical trial to investigate the efficacy and safety of corifollitropin alfa combined with hCG in adult men with hypogonadotropic hypogonadism.

Author

Nieschlag, Eberhard, Bouloux, Pierre-Marc G., Stegmann, Barbara J., Ravi Shankar, R., Guan, Yanfen, Tzontcheva, Anjela, Sisk, Christine McCrary, and Behre, Hermann M.

Subjects
CLINICAL trials, DRUG efficacy, FOLLICLE-stimulating hormone, CHORIONIC gonadotropins, HYPOGONADISM, SPERMATOGENESIS, THERAPEUTICS
Abstract

Background: Hypogonadotropic hypogonadism (HH) in men results in insufficient testicular function and deficiencies in testosterone and spermatogenesis. Combinations of human chorionic gonadotropin (hCG) and recombinant follicle-stimulating hormone (recFSH) have been successful in the treatment of HH. Corifollitropin alfa is a long-acting FSH-analog with demonstrated action in women seeking infertility care. The aim of this study was to investigate the efficacy and safety of corifollitropin alfa combined with hCG to increase testicular volume and induce spermatogenesis in men with HH. Methods: This was a Phase III, multi-center, open-label, single-arm trial of corifollitropin alfa in azoospermic men aged 18 to 50 years with HH. After 16 weeks of pretreatment of 23 subjects with hCG alone, 18 subjects with normalized testosterone (T) levels who remained azoospermic entered the 52-week combined treatment phase with hCG twice-weekly and 150 μg corifollitropin alfa every other week. The increase in testicular volume (primary efficacy endpoint) and induction of spermatogenesis resulting in a sperm count ≥1 × 106/mL (key secondary efficacy endpoint) during 52 weeks of combined treatment were assessed. Safety was evaluated by the presence of anti-corifollitropin alfa antibodies and the occurrence of adverse events (AEs). Results: Mean (±SD) testicular volume increased from 8.6 (±6.09) mL to 17.8 (±8.93) mL (geometric mean fold increase, 2.30 [95% CI: 2.03, 2.62]); 14 (77.8%) subjects reached a sperm count ≥1 × 106/mL. No subject developed confirmed anti-corifollitropin alfa antibodies during the trial. Treatment was generally well tolerated. Conclusions: Corifollitropin alfa 150 μg administrated every other week combined with twice-weekly hCG for 52 weeks increased testicular volume significantly, and induced spermatogenesis in >75% of men with HH who had remained azoospermic after hCG treatment alone. [ABSTRACT FROM AUTHOR]

Published
2017
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48. Testosterone treatment is not associated with increased risk of adverse cardiovascular events: results from the Registry of Hypogonadism in Men (RHYME).

Author

Maggi, Mario, Wu, Frederick C.W., Jones, Thomas H., Jackson, Graham, Behre, Hermann M., Hackett, Geoffrey, Martin‐Morales, Antonio, Balercia, Giancarlo, Dobs, Adrian S., Arver, Stefan T.E., Maggio, Marcello, Cunningham, Glenn R., Isidori, Andrea M., Quinton, Richard, Wheaton, Olivia A., Siami, Flora S., Rosen, Raymond C., Meuleman, E., Dohle, G., and Wu, F.

Subjects
ANDROGEN drugs, THERAPEUTIC use of testosterone, CARDIOVASCULAR diseases, COMPARATIVE studies, HYPOGONADISM, LONGITUDINAL method, RESEARCH methodology, MEDICAL cooperation, RESEARCH, EVALUATION research, ACQUISITION of data
Abstract

Aims: The aim of this study was to assess cardiovascular (CV) safety of testosterone replacement therapy (TRT) in a large, diverse cohort of European men with hypogonadism (HG).Methods: The Registry of Hypogonadism in Men (RHYME) was designed as a multi-national, longitudinal disease registry of men diagnosed with hypogonadism (HG) at 25 clinical sites in six European countries. Data collection included a complete medical history, physical examination, blood sampling and patient questionnaires at multiple study visits over 2-3 years. Independent adjudication was performed on all mortalities and CV outcomes.Results: Of 999 patients enrolled with clinically diagnosed HG, 750 (75%) initiated some form of TRT. Registry participants, including both treated and untreated patients, contributed 23 900 person-months (99.6% of the targeted) follow-up time. A total of 55 reported CV events occurred in 41 patients. Overall, five patients died of CV-related causes (3 on TRT, 2 untreated) and none of the deaths were adjudicated as treatment-related. The overall CV incidence rate was 1522 per 100 000 person-years. CV event rates for men receiving TRT were not statistically different from untreated men (P=.70). Regardless of treatment assignment, CV event rates were higher in older men and in those with increased CV risk factors or a prior history of CV events.Conclusions: Age and prior CV history, not TRT use, were predictors of new-onset CV events in this multi-national, prospective hypogonadism registry. [ABSTRACT FROM AUTHOR]

Published
2016
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49. A 6-month observational study of energy, sexual desire, and body proportions in hypogonadal men treated with a testosterone 1% gel.

Author

Pexman-Fieth, Claire, Behre, Hermann M., Morales, Alvaro, Kan-Dobrosky, Natalia, and Miller, Michael G.

Subjects
*HYPOGONADISM, *AGING, *SEXUAL desire disorders, *MEN'S health, *MEDICAL statistics, *HEALTH outcome assessment, *THERAPEUTICS
Abstract

Aims and Methods: This was a 6-month, open label, multinational, observational study in hypogonadal men treated with daily titrated dose of 50, 75, or 100 mg 1% testosterone gel (AndroGel®) in community practice. Primary outcome was effect of treatment on hypogonadal symptoms and quality of life as assessed by Aging Males' Symptoms (AMS) scale. Secondary objectives included erectile dysfunction (International Index of Erectile Function [IIEF]), fatigue (Multidimensional Fatigue Inventory [MFI]), and surrogates for body composition (waist circumference, body mass index [BMI]). Results: Seven hundred and ninety-nine of the 1053 men enrolled had follow-up data at 6 months, 81.2% had ≥1 testosterone value in the normal range during the study. Substantial and significant improvements were observed in mean AMS score (−29%), IIEF score (+115.7%), and MFI scores (−21.5%). Further beneficial effects were significant decreases in mean BMI (−0.8 kg/m2) and waist circumference (−3.3 cm). Younger age quartiles showed greater improvements in AMS, MFI, BMI, and waist circumference than older quartiles. IIEF scores, however, did not differ significantly by age category. Conclusions: Substantial improvements in hypogonadal symptoms, quality of life, fatigue, erectile dysfunction, and libido/sexual desire were observed. Adverse drug reactions were experienced by 7.5% of the safety population over the 6-month study period. [ABSTRACT FROM AUTHOR]

Published
2014
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50. Registry of Hypogonadism in Men (RHYME): design of a multi-national longitudinal, observational registry of exogenous testosterone use in hypogonadal men.

Author

Rosen, Raymond C, Wu, Frederick C. W., Behre, Hermann M., Roehrborn, Claus G, Schröder, Fritz H., Siami, Flora S., Martha, Julia F., Finn, Joseph D., and Araujo, Andre B.

Subjects
HYPOGONADISM, TESTOSTERONE, HORMONES, GONADOTROPIN, ANDROGENS, CLINICAL trials
Abstract

Objective: Despite the prevalence of hypogonadism (HG) and widespread use of testosterone therapy, little is known about the safety/effectiveness of long-term testosterone use. The Registry of Hypogonadism in Men (RHYME) is a multi-national patient registry assessing prostate health and other outcomes associated with testosterone treatment in men. Design: Observational patient disease registry. Methods: RHYME is a non-interventional disease registry with longitudinal data collection on a large sample ( N = 999) of well-characterized, hypogonadal men aged 18 years or older. The Registry will prospectively evaluate male patients diagnosed with HG, who have not previously been treated with testosterone therapy. Key design features include: (1) broad inclusion/exclusion criteria, (2) standardized central laboratory hormone assays, (3) independent adjudication of prostate biopsies and mortalities, (4) standard of care treatment, (5) comprehensive medical record and questionnaire data at six months and annually post-enrollment and (6) adequate statistical power for assessing prostate endpoints at 36 months. Results: A total of 25 clinical sites in six European countries (Germany, Italy, the Netherlands, Spain, Sweden and the United Kingdom) have completed recruitment for the study. Recruitment was initiated in May 2009, and completed in December 2011. Data collection is ongoing with a minimum of two years of follow-up on all patients. [ABSTRACT FROM AUTHOR]

Published
2013
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