Pituitary regulation of plasma lipoprotein metabolism and intestinal cholesterol absorption /

Matasconi, Manuela,

January 2005

Diss. (sammanfattning) Stockholm : Karol. inst., 2005. / Härtill 4 uppsatser.

The role of the Rx homeobox gene in development of the eye and pituitary gland

Kozhemyakina, Elena A.

January 2005

Thesis (Ph. D.)--West Virginia University, 2005. / Title from document title page. Document formatted into pages; contains viii, 179 p. : ill. (some col.). Includes abstract. Includes bibliographical references (p. 156-179).

Estudo do gene LHX4 em pacientes com hipopituitarismo associado a neuro-hipófise ectópica / Molecular analysis of the LHX4 gene in hypopituitary patients with ectopic posterior pituitary lobe

Melo, Maria Edna de

12 December 2005

INTRODUÇÃO: O hipopituitarismo está associado, em cerca de 40% dos casos, à ectopia da neuro-hipófise observada em imagem por ressonância magnética (RM). Nestes pacientes a visualização da haste ocorre predominantemente nos que têm deficiência isolada de GH (DIGH), enquanto a não visualização da mesma está mais associada à deficiência hipofisária múltipla (DHM). A etiologia deste quadro, no entanto, permanece indeterminada na maioria dos pacientes. A elevada freqüência de parto pélvico e de complicações neonatais sugere uma causa traumática, enquanto que relatos de casos familiares, associação com outras patologias do SNC e descrição de mutações nos genes HESX1, LHX4 e SOX3 apontam para uma causa genética. O LHX4 é um fator de transcrição envolvido na embriogênese hipofisária fundamental para a formação da bolsa de Rathke definitiva. O LHX4 está localizado no cromossomo 1q 25, possui 6 éxons e estende-se por mais de 45 kb de DNA genômico. A única mutação publicada neste gene em humanos é a IVS4-1G>C, associada a um fenótipo caracterizado por baixa estatura, deficiências de GH, TSH e ACTH, neuro-hipófise ectópica e malformação Arnold-Chiari tipo I. O objetivo do estudo é analisar as regiões exônicas e éxon-íntron do LHX4 e caracterizar o perfil hormonal, correlacionando com os achados de RM, em 63 pacientes com hipopituitarismo associado a neurohipófise ectópica. MÉTODOS: Os pacientes foram submetidos à avaliação hormonal e por imagem através de ressonância magnética. A análise molecular incluiu amplificação do gene por PCR, seqüenciamento automático e uso de enzima de restrição. RESULTADOS: A visualização da haste ocorreu em 21 pacientes; destes, 10 (48%) apresentaram DIGH. A não visualização da haste foi mais associada a DHM, o que ocorreu em 40 (95%) dos 42 pacientes. Não encontramos diferença significativa quando comparamos pacientes com haste visualizada e não visualizada quanto à freqüência de partos vaginais em apresentação pélvica, à freqüência de malformações do SNC e à posição precisa da neuro-hipófise ectópica. Identificamos 6 variações alélicas no gene LHX4 em nossos pacientes: GGT>GGC, no códon 21; GAC>GAT, no códon 128; AAC>AAT, no códon 150; AGC>AGT, no códon 230; GGA>GGT, no códon 283 e AAT>AGT no códon 329 (N329S), esta já descrita como polimorfismo no GenBank. Nenhuma das outras variações determina troca de aminoácidos, altera o sítio de \"splice\" ou se correlaciona com um padrão de deficiência hormonal característico. As variações alélicas nos códons 21, 128 e 150 foram caracterizadas como polimorfismos. Não foi possível estabelecer uma relação entre as variações alélicas e o fenótipo dos pacientes. CONCLUSÃO: Mutações no LHX4 são causas raras de hipopituitarismo / INTRODUCTION: Ectopic posterior pituitary lobe (EPL) is observed using magnetic resonance imaging (MRI) scans in about 40% of patients with hypopituitarism. In these patients, the pituitary stalk is visualized mainly in patients with isolated GH deficiency (IGHD), whilst it is not visualized predominantly in patients with combined pituitary hormone deficiency (CPHD). Nevertheless, the etiology of EPL remains undetermined in most of the patients. A traumatic etiology is proposed for this figure, which presents a high frequency of breech delivery and perinatal damages. On the other hand, a genetic cause is suggested by associations to other CNS abnormalities and reports of gene mutations in HESX1, LHX4 and SOX3, as well as familial cases. LHX4 is a transcription factor implicated in pituitary embryogenesis which is essential to definitive Rathke\'s pouch development. It is located in chromosome 1q25, has 6 exons and is stretched out for more than 45 kb of genomic DNA. The only documented human mutation in this gene, IVS4-1G>C, is associated to a phenotype characterized by short stature, GH, TSH and ACTH deficiencies, EPL and Arnold-Chiari type I malformation. The aim of this study is to analyze exonic and exon-intron regions of LHX4 gene and characterize the hormonal deficiency profiles, establishing relationships to MRI findings in 63 patients with hypopituitarism associated to EPL. METHODS: All patients were submitted to hormonal evaluation and MRI scans. The molecular analysis included amplification of the gene using PCR, direct automatic sequencer and digestion with restriction enzymes. RESULTS: The pituitary stalk was visualized in 21 patients; of these, 10 (48%) exhibited IGHD. The stalk was not visualized in 42 patients, most of them with CPHD (95%). We did not find a statistical difference, when patients with and without visualized pituitary stalk were compared, regarding breech deliveries, CNS malformations and exact position of EPL. We identified 6 allelic variations in LHX4 gene: GGT>GGC in codon 21, GAC>GAT in codon 128, AAC>AAT in codon 150, AGC>AGT in codon 230, GGA>GGT in codon 283 and AAT>AGT in codon 329 (N329S), this already related as a polymorphism in GenBank. None of the former variations determine amino acid changes, nor splicing site changes, not even are related to a typical profile of hormonal deficiency. The allelic variations in codons 21, 128 and 150 were described as polymorphisms. It was not possible to establish a relationship between the allelic variations and the phenotype. CONCLUSION: LHX4 gene mutations are rare causes of hypopituitarism

Dwarfism pituitary

Fatores de transcrição

Glândula pituitária

Glândula pituitária posterior

Hipopituitarismo

Hypopituitarism

Nanismo hipofisário

Pituitary gland

Pituitary gland posterior

Pituitary gland posterior/abnormalities

Transcription factors

Estudo do gene LHX4 em pacientes com hipopituitarismo associado a neuro-hipófise ectópica / Molecular analysis of the LHX4 gene in hypopituitary patients with ectopic posterior pituitary lobe

Maria Edna de Melo

12 December 2005

INTRODUÇÃO: O hipopituitarismo está associado, em cerca de 40% dos casos, à ectopia da neuro-hipófise observada em imagem por ressonância magnética (RM). Nestes pacientes a visualização da haste ocorre predominantemente nos que têm deficiência isolada de GH (DIGH), enquanto a não visualização da mesma está mais associada à deficiência hipofisária múltipla (DHM). A etiologia deste quadro, no entanto, permanece indeterminada na maioria dos pacientes. A elevada freqüência de parto pélvico e de complicações neonatais sugere uma causa traumática, enquanto que relatos de casos familiares, associação com outras patologias do SNC e descrição de mutações nos genes HESX1, LHX4 e SOX3 apontam para uma causa genética. O LHX4 é um fator de transcrição envolvido na embriogênese hipofisária fundamental para a formação da bolsa de Rathke definitiva. O LHX4 está localizado no cromossomo 1q 25, possui 6 éxons e estende-se por mais de 45 kb de DNA genômico. A única mutação publicada neste gene em humanos é a IVS4-1G>C, associada a um fenótipo caracterizado por baixa estatura, deficiências de GH, TSH e ACTH, neuro-hipófise ectópica e malformação Arnold-Chiari tipo I. O objetivo do estudo é analisar as regiões exônicas e éxon-íntron do LHX4 e caracterizar o perfil hormonal, correlacionando com os achados de RM, em 63 pacientes com hipopituitarismo associado a neurohipófise ectópica. MÉTODOS: Os pacientes foram submetidos à avaliação hormonal e por imagem através de ressonância magnética. A análise molecular incluiu amplificação do gene por PCR, seqüenciamento automático e uso de enzima de restrição. RESULTADOS: A visualização da haste ocorreu em 21 pacientes; destes, 10 (48%) apresentaram DIGH. A não visualização da haste foi mais associada a DHM, o que ocorreu em 40 (95%) dos 42 pacientes. Não encontramos diferença significativa quando comparamos pacientes com haste visualizada e não visualizada quanto à freqüência de partos vaginais em apresentação pélvica, à freqüência de malformações do SNC e à posição precisa da neuro-hipófise ectópica. Identificamos 6 variações alélicas no gene LHX4 em nossos pacientes: GGT>GGC, no códon 21; GAC>GAT, no códon 128; AAC>AAT, no códon 150; AGC>AGT, no códon 230; GGA>GGT, no códon 283 e AAT>AGT no códon 329 (N329S), esta já descrita como polimorfismo no GenBank. Nenhuma das outras variações determina troca de aminoácidos, altera o sítio de \"splice\" ou se correlaciona com um padrão de deficiência hormonal característico. As variações alélicas nos códons 21, 128 e 150 foram caracterizadas como polimorfismos. Não foi possível estabelecer uma relação entre as variações alélicas e o fenótipo dos pacientes. CONCLUSÃO: Mutações no LHX4 são causas raras de hipopituitarismo / INTRODUCTION: Ectopic posterior pituitary lobe (EPL) is observed using magnetic resonance imaging (MRI) scans in about 40% of patients with hypopituitarism. In these patients, the pituitary stalk is visualized mainly in patients with isolated GH deficiency (IGHD), whilst it is not visualized predominantly in patients with combined pituitary hormone deficiency (CPHD). Nevertheless, the etiology of EPL remains undetermined in most of the patients. A traumatic etiology is proposed for this figure, which presents a high frequency of breech delivery and perinatal damages. On the other hand, a genetic cause is suggested by associations to other CNS abnormalities and reports of gene mutations in HESX1, LHX4 and SOX3, as well as familial cases. LHX4 is a transcription factor implicated in pituitary embryogenesis which is essential to definitive Rathke\'s pouch development. It is located in chromosome 1q25, has 6 exons and is stretched out for more than 45 kb of genomic DNA. The only documented human mutation in this gene, IVS4-1G>C, is associated to a phenotype characterized by short stature, GH, TSH and ACTH deficiencies, EPL and Arnold-Chiari type I malformation. The aim of this study is to analyze exonic and exon-intron regions of LHX4 gene and characterize the hormonal deficiency profiles, establishing relationships to MRI findings in 63 patients with hypopituitarism associated to EPL. METHODS: All patients were submitted to hormonal evaluation and MRI scans. The molecular analysis included amplification of the gene using PCR, direct automatic sequencer and digestion with restriction enzymes. RESULTS: The pituitary stalk was visualized in 21 patients; of these, 10 (48%) exhibited IGHD. The stalk was not visualized in 42 patients, most of them with CPHD (95%). We did not find a statistical difference, when patients with and without visualized pituitary stalk were compared, regarding breech deliveries, CNS malformations and exact position of EPL. We identified 6 allelic variations in LHX4 gene: GGT>GGC in codon 21, GAC>GAT in codon 128, AAC>AAT in codon 150, AGC>AGT in codon 230, GGA>GGT in codon 283 and AAT>AGT in codon 329 (N329S), this already related as a polymorphism in GenBank. None of the former variations determine amino acid changes, nor splicing site changes, not even are related to a typical profile of hormonal deficiency. The allelic variations in codons 21, 128 and 150 were described as polymorphisms. It was not possible to establish a relationship between the allelic variations and the phenotype. CONCLUSION: LHX4 gene mutations are rare causes of hypopituitarism

Fatores de transcrição

Glândula pituitária

Glândula pituitária posterior

Hipopituitarismo

Nanismo hipofisário

Dwarfism pituitary

Hypopituitarism

Pituitary gland

Pituitary gland posterior

Pituitary gland posterior/abnormalities

Transcription factors

DOPAMINE AS A DYNAMIC REGULATOR OF PROLACTIN SECRETION.

FINDELL, PAUL RICHARD.

January 1983

To test the hypothesis that the hypothalamic tuberoinfundibular dopaminergic neuronal system plays a role in the dynamic regulation of pituitary prolactin secretion, its activity was correlated with experimentally-induced prolactin secretory episodes in the male rat. Direct estimates of tuberoinfundibular neuronal activity were made by measuring its rates of dopamine and norepinephrine synthesis or release. Prolactin secretion was assessed in vivo by measuring radioimmunoassayable prolactin levels in peripheral blood and the pituitary and in vitro by measuring prolactin concentrations released into incubation media. The anesthetic urethane and a substance isolated from the pineal gland were both demonstrated to inhibit prolactin secretion. Significant elevations of newly synthesized tuberoinfundibular dopamine were observed concomitant with this decreased prolactin secretion suggesting that acute increases in tuberoinfundibular dopaminergic neuronal activity were perhaps causally related to acute decreases in prolactin secretion since these substances were without a direct effect on the pituitary in vitro. Conversely, acute decreases in tuberoinfundibular neuronal activity induced by dopamine biosynthesis inhibition or mimicked by pituitary receptor blockade induced acute increases in prolactin secretion. As another prerequisite for its involvement in the dynamic regulation of prolactin secretion, the tuberoinfundibular neuronal system was demonstrated to be involved in the negative feedback control of prolactin over its own secretion. Elevated circulating prolactin levels produced by pituitary homografts transplanted beneath the kidney capsule accelerated tuberoinfundibular dopaminergic neuronal activity. In two unrelated experimental conditions, rats rendered blind and anosmic or hyperprolactinemic, the chronic inhibition of prolactin secretion was not associated with the maintenance of an increased tuberoinfundibular neuronal activity, but rather with a supersensitivity of the anterior pituitary to the prolactin-release-inhibitory action of dopamine. Long-lasting alterations in tuberoinfundibular dopaminergic neuronal activity appeared to induce this pituitary supersensitivity to dopamine. The tuberoinfundibular neuronal system appears to have the capacity to modulate prolactin secretory episodes via the alteration of its dopaminergic activity. Long-lasting alterations in this activity may induce changes in anterior pituitary sensitivity to dopamine essential for the chronic inhibition of pituitary prolactin secretion.

Dopamine -- Receptors.

Prolactin.

Pituitary gland.

Pituitary hormone releasing factors.

PITUITARY-THYROID FUNCTION IN THE C57 BL/KSJ DB/DB DIABETIC MOUSE.

FEHN, RICHARD., FEHN, RICHARD.

January 1983

The C57 BL/KsJ db/db mouse is obese, hyperglycemic, hyperinsulinemic and serves as a model for noninsulin dependent diabetes mellitus (NIDDM). This study reports a dysfunction in the pituitary-thyroid axis and apparent peripheral resistence to thyroid hormones due to a reduction in T3 receptor binding. Diabetic mice have subnormal serum T4 concentrations and supranormal T3 concentrations which are most pronounced between 8 and 10 weeks of age. Thyroid glands of diabetic animals appear hypoactive histologically. Serum TSH concentrations approximate those found in normal mice. In vitro studies show that thryroid glands from diabetic animals are responsive to TSH. Pituitary glands from the same animals hypersecrete TSH and are responsive to TRH. Ultrastructural analysis of pituitary thyrotropes from diabetic mice indicate that these cells are hypersecretory and may be under chronic stimulation by TRH. Diet restriction maintains diabetic mice at a normal total body weight but these animals still possess abnormally large fat deposits. The thyroid hormone profile of these mice appears normal as does the histological appearance of the thyroid gland. Similarly, the blockade of peripheral deiodination by daily injection of iopanoic acid returns the thyroid hormone profile to normal.

Diabetes -- Research.

Mice -- Physiology.

Pituitary gland.

Thyroid gland.

Thyroid hormones.

Analyse intégrative génomique et épigénomique de tumeurs hypophysaires à prolactine / Genomics and epigenomics integrative analysis of prolactin pituitary tumors

Roche, Magali

19 December 2013

De nombreux modèles ont été proposés pour expliquer les mécanismes de développement et de progression tumorale, néanmoins certains aspects comme la nature et la hiérarchie des altérations primaires et secondaires sont encore discutés. Pour répondre à ces questions, nous nous sommes intéressés à la progression tumorale des tumeurs hypophysaires à prolactine humaines. Ces tumeurs d'origine monoclonale sont souvent bénignes mais certaines présentent un phénotype agressif voire malin. Afin d'identifier les mécanismes impliqués dans la progression vers le phénotype agressif nous avons utilisé des techniques de génomique intégrative (puces à ADN, séquençage haut débit) couplant l'étude du transcriptome, du génome (variation du nombre de copie chromosomique, polymorphismes) et du miRNome à partir des mêmes échantillons tumoraux. Par cette stratégie nous avons identifié et hierarchisé des altérations spécifiques des tumeurs agressives et / ou malignes dans un modèle expliquant la progression tumorale des tumeurs hypophysaires à prolactine humaines. Nous avons montré que la sous-expression des microARNs miR-183, miR-744 et miR-98 stimule la prolifération via la surexpression de leurs cibles KIAA0101, TGFB1 et E2F2 spécifiquement dans les tumeurs agressives. Ceci entraine l'acquisition d'altérations chromosomiques (perte du chromosome 11 et le gain du chromosome 1q) permettant l'activation de la dissémination métastatique. Enfin, ce travail montre que l'approche de génomique intégrative multidimensionnelle permet d'apporter de nouveaux éléments pour la caractérisation des phénotypes tumoraux, le diagnostic des tumeurs agressives et la prédiction du comportement tumoral / Numerous models have been proposed to explain the mechanisms of tumor development and progression. Nevertheless some aspects such as the nature and hierarchy of primary and secondary alterations are still debated. To answer these questions, we decided to focus on the tumoral progression of human prolactin pituitary tumors. These monoclonal tumors are usually benign but some present an aggressive or malignant phenotype. To identify the molecular events involved in tumoral progression of human PRL towards aggressive phenotype we used an integrative genomics approach (microarrays, high-throughput sequencing) coupling analysis of transcriptome, genome (variation in the number of chromosomal copy polymorphisms) and miRNome from the same human tumor. Using this strategy we identified and prioritized specific alterations of aggressive and / or malignant tumors in a model explaining the tumor progression of human prolactin pituitary tumors. We have shown that under-expression of micro-RNA miR-183, miR-744 and miR-98 stimulates proliferation through overexpression of their targets KIAA0101, TGFB1 and E2F2 specifically in aggressive tumors. This leads to the acquisition of chromosomal damage (loss of chromosome 11 and gain of chromosome 1q) which allowed the activation of the metastatic processes. Finally, this work shows that the integrative genomic multi-dimensional approach can provide new clues for the characterization of tumor phenotypes, diagnosis of aggressive tumors and prediction of tumor behavior

Hypophyse

Tumeur

Prolactinome

Génomique

Pituitary gland

Tumor

Prolactinoma

Genomics

612.015

Aspectos morfológicos da hipófise do macaco Cebus apella / Morphology Aspects of the Hipophisis of the monkey Cebus apella

Ribeiro, Adriana Rodrigues

29 June 2006

O conhecimento de diversos aspectos da Neuroanatomia de primatas não humanos - que atualmente é falho, pela falta de trabalhos a respeito - é importante não apenas pela importância intrínseca desse conhecimento como até pelo fato de contribuir para um melhor entendimento da própria evolução do grupo, o que representa um fator relevante para a sua preservação e proteção. O objetivo deste trabalho é efetuar estudos morfológicos da hipófise do macaco Cebus apella a fim de conhecer melhor esta estrutura, e oferecer subsídios para análises comparativas mais amplas. Utilizamos 11 animais sendo 7 deles constantes do acervo de pesquisa da Universidade Federal de Uberlândia e, os outros 4 exemplares, doados pelo IBAMA-MG. A preparação das peças anatômicas foi levada a efeito mediante cuidadosa dissecção dos espécimes, cujos encéfalos foram retirados das caixas cranianas, preservando-se ao máximo todas as suas estruturas. As hipófises, depois de registrada sua macroscopia, foram submetidas aos métodos histológicos de rotina para observações em microscopia de luz e eletrônica de transmissão. Dos resultados obtidos podemos citar que a hipófise, neste animal, é uma glândula intracraniana alojada na sela turcica, fixada à base do cérebro pelo infundíbulo, sendo este muito curto. Ela exibe forma odontóide, exibindo-se aparentemente, como uma massa única, pois macroscopicamente apenas é possível, a identificação de uma divisão discreta em um lobo anterior e outro posterior, além do infundíbulo. As análises histológicas mostram esta glândula dividida em três lobos: anterior (adenohipófise), intermédio e posterior (neurohipófise). À microscopia eletrônica de transmissão foi possível identificar e classificar 4 tipos celulares em relação á adenohipófise: células do tipo I, II, III e IV. O aspecto do núcleo dessas células, exibindo freqüentemente, invaginações profundas de sua membrana, confere à hipófise do macaco Cebus apella, características peculiares, o que nos instiga a realizar novas pesquisas sobre o assunto / The knowledge of many aspects of Neuroanatomy of non-human primates - which is currently poor due to the lack of studies on the subject - is very important not only for the intrinsic significance of the knowledge itself but also because it contributes for a better understanding of the evolution of the group, which represents a relevant factor for its preservation and protection. The objective of this study is to perform morphological researches on the hypophysis of the Cebus apella monkey in order to understand this structure better and to provide basis for wider comparative analyses. Eleven animals were used on this study. Seven of them were properties of the research collection of the Federal University of Uberlândia and the other four were donated by the IBAMA-MG. The preparation of the anatomical parts was carefully done through dissection of the specimens, whose encephalus were removed from their skulls preserving all their structures. The hypophysis, after having their macroscopy registered, were submitted to histological methods of routine for observation in light microscopy and electronic microscopy of transmission. We could conclude from the obtained results that the hypophysis, on this particular animal, is a intracranial gland lodged in the sela turcica fixed to the base of the brain by the infundibulum which is very short. It has in dens shape and it presents itself as a single mass, because, macroscopically, it is only possible the identification of a discrete division in an anterior lobe and another posterior one besides the infundibulum. The histological analyses show this gland divided in three lobes: anterior (adenohypophysis), intermediary and posterior (neurohypophysis). Through the electronic microscopy of transmission it was possible to identify and classify four cellular types related to the adenohypophysis: types I, II, III and IV. The aspect of the cores of these cells, frequently showing deep invaginations of their membranes, confers to hypophysis of the Cebus apella monkey, peculiar characteristics, which instigates us to carry on performing new studies on the subject

Cebus apella

Cebus apella

Glândula Pituitária

Neuroanatomia

Neuroanatomy

Pituitary gland

Effects of endocrine manipulation on the peptide levels and the gene expression of {221}-endorphin, met-enkephalin, somatostatin, substanceP and cholecystokinin in the rat hypothalamus and pituitary

張頌恩, Cheung, Chung-yan.

January 1998

published_or_final_version / Physiology / Master / Master of Philosophy

Endorphins.

Enkephalins.

Somatostatin.

Hypothalamus.

Cholecystokinin.

Pituitary gland.

Rats - Genetics.

EFFECT OF REDUCED ENERGY INTAKE ON PITUITARY RESPONSE TO GONADOTROPIN RELEASING HORMONE

Chipepa, Joseph Augustine Shangosa

January 1981

An experiment was conducted with Brangus cows to evaluate the effect of loss of body weight and condition on pituitary responsiveness to gonadotropin releasing hormone (GnRH) stimulation during late lactation. The treatment groups were lactating intact (LI), lactating ovariectomized (LO), nonlactating intact (NLI), and nonlactating ovariectomized (NLO). The study was carried out in two separate blocks, each one consisting of 3 periods. During period 1 the cows were fed a ration that supplied 90% and 88% of the NRC recommendations for TDN in lactating and nonlactating cows, respectively. This period lasted 170 in block 1 and 130 days in block 2. During period 2 the TDN was reduced to 55% or 52% for lactating and nonlactating cows, respectively. Period 2 lasted 100 days for cows in block 1 and 63 days for cows in block 2. At the beginning of period 3 TDN was further reduced to 25% or 27% for the lactating and nonlactating cows, respectively. Cows in block 1 were challenged with GnRH 40 days after the beginning of the 1st energy reduction, 30 days later and 7 days after the 2nd energy reduction. The cows in block 2 were challenged with GnRH 30 days after the 1st energy reduction, 30 days later and 25 days after the 2nd energy reduction. At the end of the study body composition parameters and organ gland weights were determined. No significant differences in the weights of the cows among the treatment groups were found. All cows were, however, losing weight through the course of this study. The nonlactating cows maintained higher body condition (P < .05) than lactating cows from 31 days after ovariectomies were performed until the end of the study. The pituitary glands were significantly heavier in the lactating ovariectomized (2.3 g vs. 1.7 g, P < .05) than the nonlactating intact cows. The weight of the adrenals per unit of body weight of LO cows was significantly higher (.057 g/kg vs. .040 g, P < .05) than among NLO cows. The percent of carcass lipid was significantly higher (P < .05) in nonlactating as compared to lactating cows. Percent moisture and protein were higher (P < .05) in lactating cows. Amount of LH released after GnRH stimulation tended to be higher in lactating than nonlactating cows. The magnitude of the LH peak did not differ significantly among the treatment groups at each of the dates GnRN was injected. Ovariectomized cows (LO and NLO) responded more rapidly (P < .05) to GnRH stimulation than intact cows (LI and NLI). Time on reduced TDN did not affect cow's response pattern after GnRH injection.

Dairy cattle -- Feeding and feeds.

Brangus cattle.

Gonadotropin.

Pituitary gland.