• 한국동물학회:뉴스레터
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• 제12권2호
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• pp.8-8
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• 1995

No Abstract, See Full Text

• 한국동물학회:학술대회논문집
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• 한국동물학회 1995년도 한국생물과학협회 학술발표대회
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• pp.74-74
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• 1995

No Abstract, See Full Text

• Fisheries and Aquatic Sciences
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• 제25권11호
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• pp.559-571
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• 2022

Galectins, a family of ß-galactoside-binding lectins, have emerged as soluble mediators in infected cells and pattern recognition receptors (PRRs) responsible for evoking and regulating innate immunity. The present study aimed to evaluate the role of galectin-1 in the host immune response of redlip mullet (Liza haematocheilia). We established a cDNA database for redlip mullet, and the cDNA sequence of galectin-1 (LhGal-1) was characterized. In silico analysis was performed, and the spatial and temporal expression patterns in gills and blood in response to lipopolysaccharide polyinosinic:polycytidylic acid, and Lactococcus garvieae were estimated via quantitative real-time PCR. Functional assays were conducted using recombinant protein to investigate carbohydrate binding, bacterial binding, and bacterial agglutination activity. LhGal-1 was composed of 135 amino acids. Conserved motifs (H-NPR, -N- and -W-E-R) within the carbohydrate recognition domain were found in LhGal-1. The tissue distribution revealed that the healthy stomach expressed high levels of LhGal-1. The temporal monitoring of LhGal-1 mRNA expression in the gill and blood showed its significant upregulation in response to immune challenges with different stimulants. rLhGal-1 exhibited binding activity in response to carbohydrates and bacteria. Moreover, the agglutination of rLhGal-1 against Escherichia coli was observed. Collectively, our findings suggest that LhGal-1 may function as a PRR in redlip mullet. Furthermore, LhGal-1 can be considered a significant gene to play a protective role in redlip mullet immune system.

• Asian-Australasian Journal of Animal Sciences
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• 제21권7호
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• pp.972-979
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• 2008

It has been recently shown that expression of the LH receptor (LHR) in cumulus cells is related with FSH-induced meiotic resumption of mouse cumulus enclosed oocytes (CEOs). However, to date, it is still unclear whether LHR expression in cumulus cells plays a key role during FSH-induced oocyte maturation. The purpose of this study was to characterize the functional role of LHRs in cumulus cells. CEOs were isolated from eCG-primed preovulatory follicles and cultured in hypoxanthine (HX) arrested medium. LHR protein expression in cumulus cells was time-dependent increasing during the process of FSH-induced oocyte maturation. While the sense oligodeoxynucleotide (ODN) had no effect, antisense ODN inhibited FSH-induced LHR expression and meiotic resumption. Moreover, this antisense ODN against LHR could inhibit FSH-induced mitogen-activated protein kinase (MAPK) phosphorylation. This study suggested that LHR expression in cumulus cells is involved in FSH-induced oocyte meiotic resumption, which process is possibly regulated by MAPK cascade.

• 한국발생생물학회지:발생과생식
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• 제11권1호
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• pp.13-20
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• 2007

암컷 포유동물의 노화 과정에서 생식계는 체내 여러 시스템 가운데 가장 먼저 기능 저하가 나타난다. 생식 노화(reproductive aging) 과정 중인 암컷 포유동물은 비록 종 특이성이 있지만 주기성(cyclicity)의 소실과 같은 생식 능력의 감소와 함께 여러 기능들의 변화가 동반되면서 궁극적으로 인간의 폐경 현상과 같은 생식 능력 상실이 나타난다. 본 증설은 암컷 포유동물의 생식호르몬 축, 특히 신경내분비 회로의 노화에 대한 정보들과 노화 연구에 유용한 설치류 모델들을 소개하고자 한다. 암컷 설치류의 중년(middle age, 생후 $8{\sim}12$개월)은 인간의 폐경기 진입 직전에 해당되는 시기로, 이 시기에 시상하부 GnRH 분비의 맥동성과 급등(surge)이 현저히 지연되기 시작하고, 곧 이어 뇌하수체 LH 분비의 맥동성과 급등이 역시 약화 내지 지연된다. 노화와 관련된 GnRH-LH 신경내분비 활성의 결손은 시상하부 GnRH 뉴런의 활성을 조절하는 여러 자극(예, glutamate)들의 변화와 밀접하게 연관되어 있다. 많은 연구자들이 이러한 '시상하부 결손(hypothalamic defects)'이 생식 노화의 주된 요인임을 지지하지만, inhibin과 같은 난소 요인의 변화 역시 생식 노화의 유도와 관련된 것으로 보인다. 생식 노화를 연구함에 유용한 몇몇 설치류 모델이 있다; FSH 수용체 녹아웃(follitropin receptor knockout; FORKO) 생쥐 모델의 경우는 homozygous(null) 뿐만 아니라 heterozygous(haploinsufficient) 상태도 노화에 따른 난자/난포의 고갈을 나타낸다. Dioxin/aryl hydrocarbon 수용체 녹아웃 (AhRKO) 생쥐 모델도 유사한 상태를 유발할 수 있다. 생식 노화의 기작에 관한 연구는 삶의 질을 높이기 위한 수단들, 예를 들어 호르몬 보충요법(HRT)의 장단점을 평가하고 안전성을 제고하는데 도움이 될 것이다.

• 한국발생생물학회지:발생과생식
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• 제5권2호
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• pp.175-180
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• 2001

태반이나 생식소 등 시상하부 이외의 조직에서도 gonadotropin releasing hormone(GnRH)과 그 수용체가 발현되어 조직 특이적인 기능을 담당함은 잘 알려진 사실이다. 최근 GnRH와 그 수용체 유전자가 흰쥐 유선에서도 발현됨이 증명되었고, LH $\alpha$-와 $\beta$-subunit와 LH 수용체에 대한 전사체 역시 흰쥐 유선에 존재함이 확인되었다 본 연구는 흰쥐 유선 LH의 발현과 유선의 분화과정 간의 상관관계를 조사하기 위해서 생식주기, 임신, 수유, 이유기에 걸쳐 얻은 유선을 재료로 LH 함량 변화를 방사면역측정법으로 측정하였다. 또한 동일한 실험동물에서 얻은 RNA를 사용한 reverse transcription-polymerase chain reaction(RT-PCR)과 Southern blot analysis를 통해 전사수준에서의 변화를 측정하였다. 난소 steroid에 의한 유선 LH의 발현조절 가능성을 조사하기 위해서 난소 제거(ovariectomy, OVX)후 steroid 처리 실험동물 모델을 사용하였다. 생식주기중인 흰쥐의 혈중 LH수준과 유선 내 LH 함량의 변화는 공히 proestrus 시기에 가장 높고 diestrus I 시기에 최저 수준을 보였다. 임신 17일 경으로부터 이유기까지 혈중 LH 수준은 등락을 보였으나, 유선 LH 함량은 수유기 중 현저히 감소한 후 이유기에 상승하였다. Southern blot analysis에서 흰쥐 유선 내 GnRH와 LH의 발현은 대체로 diestrus I 시기에 가장 낮고 이후 diestrus II, proestrus, estrus 시기를 거치며 증가하였고 임신 이후 수유기와 이유기까지 높은 수준으로 유지됨이 확인되었다. 한편 OVX 실험 동물모델에서 혈중 LH 수준은 예상한 바처럼 estrogen에 의한 negative feedback의 작용으로 OVX＋OIL 실험군(418.6$\pm$73.4 ng/ml)에 비해 OVX＋E$_2$ 실험군(125.9$\pm$45.4 ng/ml)에서 감소하였으며, 유선 내 LH 함량 역시 OVX+OIL 실험군(1.48$\pm$0.20 na/mg)에 비해 OVX+E$_2$ 실험군(1.07$\pm$0.13 ng/mg)에서 유의성 있게 감소하였다. 본 연구결과는 유선 LH가 생식주기, 임신, 수유, 이유 등의 생리적인 변화에 맞물려 조절되고, 특히 estrogen에 의해 유선 LH 합성이 조절될 수 있음을 시사하였다. 유선 LH의 기능으로는 모유의 생산ㆍ분비와 유선 상피세포의 분화와 같은 유선의 기능과 생리조절에 관여하는 것으로 추정된다.

• 대한약리학회지
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• 제23권2호
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• pp.57-75
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• 1987

Two modalities of gonadotropin secretion, pulsatile gonadotropin and preovulatory gonadotropin surge, have been identified in the mammals. Pulsatile gonadotropin secretion is modulated by the pulsatile pattern of GnRH release and complex ovarian steroid feedback actions. The neural mechansim that regulates the pulsatile release of GnRH in the hypothalamus is called "GnRH pulse generator". Ovarian steroids, estradiol and progesterone, appear to exert thier feedback effects both directly on the pituitary to modulate gonadotropin release and on a hypothalamic site to modulate GnRH release; estradiol primarily affects the amplitude while progesterone decreases the frequency of the pulsatile GnRH. Steroid hormones are known to affect catecholamine transmission in brain. MBH-POA is richly innervated by NE systems and close apposition of NE terminals and GnRH cell bodies occurs in the MBH as well as in the POA. NE normally facilitates pulsatile LH release by acting through ${\alpha}-receptor$ mechanism. However, precise nature of facilitative role of NE transmission in maintaining pulsatile LH has not been clearly understood. Close apposition of DA and GnRH terminals in ME might permit DA to influence GnRH release. Action of DA transmission probably is mediated by axo-axonic contacts between GnRH and DA fibers in the ME. Dopamine transmission does not normally regulate pulsatile LH release, but under certain conditions, increased DA transmission inhibit LH pulse. Endogenous opioid acts to suppress the secretion of GnRH into hypophysial portal circulation, thereby inhibiting gonadotropin secretion. However, an interaction between endogenenous opioid peptides and gonadotropin release is a complex one which involves ovarian hormones as well. LH secretion appears to be most suppressed by endogenenous opioids during the luteal phase, at a time of elevated progesterone secretion. The arcuate nucleus contains not only cell bodies for GnRH and ${\beta}-endorphin$ but also a dense aborization of fibers suggesting that GnRH release is changed by the interactions between GnRH and ${\beta}-endorphin$ cell bodies within the arcuate nucleus. The frequency and amplitude of pulsatile LH release seem to be increased during the preovulatory gonadotropin surge. Estradiol exerts positive feedback action on the hypothalamo-pituitary axis to trigger preovulatory LH surge. GnRH is also crucial hormonal stimulus for preovulatory LH surge. It is unlikely, however, that increased secretion of GnRH during the preovulatory gonadotropin surge represents an obligatory neural signal for generation of the LH discharge in primates including human. Modulation of preovulatory LH surge by catecholamines has been studied almost exclusively in rats. NE and E may be involved in distinct way to accumulate GnRH in the MBH and its release into the hypophysial portal system during the critical period for LH surge on proestrus in rats. However, the mechanisms whereby augmented adrenergic transmission may facilitate the formation and accumulation of GnRH in the ME-ARC nerve terminals before the LH surge have not been clearly understood.

• Environmental Analysis Health and Toxicology
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• 제18권2호
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• pp.95-100
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• 2003

본 연구는 환경호르몬(endocrine disruptors)으로 분류되었으며, 제초제로 널리 사용되었던 Dichlorodiphenyltrichloroethane(DDT)가 설치류의 생식세포 중 Leydig 세포의 testosterone(T)생성억제 및 그 관련 작용메카니즘을 규명코자 수행되었다. 먼저 흰쥐의 웅성 생식세포주인 R2C세포에 T의 양 및 aromatase 활성도를 radio immunoassay (RIA)방법을 이용하여 측정하였다. 그 결과 R2C 세포에 황체형성호르몬(LH)를 처리하여 testosterone생성을 증가시킨 후, DDT를 처리한 군들은 대조군에 비하여 농도 의존적으로 T의 양은 감소하였으며, aromatase 활성도는 증가하였다. 또한 DDT자체만 처리한 군에서도 대조군에 비하여 testosterone의 생성이 감소하였다. 이러한 aromatase활성 증가가 estradiol receptor(ER)와의 상호 관련성을 확인하기 위해 ER antagonist인 ICI 182.780를 처리한 후 T의 양 및 aromatase 활성도를 측정한 결과 DDT에 의해 증가된 aromatase활성도가 ICI 182.780에 의해 다시 감소됨을 확인하였다. 또한 DDT에 의해 감소된 T의 양도 ICI 182.780에 의해 다시 회복되었다. In vivo실험으로 흰쥐에 DDT를 직접 투여한 후 정소 내 성 호르몬들을 측정해 본 결과 T의 양은 유의성 있게 감소하였으며, estradiol(E$_2$)의 양은 증가하였으며, aromatase 활성도도 감소하였다. 이러한 결과를 종합해 볼 때 DDT는 aromatase를 감소시키고, 이렇게 감소된 aromatase에 의해 testosterone 생성량을 억제하고, 이러한 DDT의 aromatase의 감소는 ER을 경유하는 것으로 추정할 수 있다.

• 동의생리병리학회지
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• 제18권5호
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• pp.1463-1470
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• 2004

Paljinickmohwan(八珍益母丸) is used in female infertility. especially due to deficiency of qi and blood or Qihyulyanghe(氣血兩虛). An attempt was made to evaluate the influences of PJIMH on the serum concentrations of FSH, LH, and estradiol(E2), the histological changes of ovary and the immunohistochemical staining for AT2 receptor in ovary of rats. The results of the study were as follows : Blood FSH level significantly increased in experimental group as compared with control group. In blood LH level, experimental group as compared with control group showed no efficacy. Blood E2 level significantly increased in experimental group as compared with control group. In histological observations of ovary, ovulation increased in experimental group as compared control group, which showed no efficacy. In observations of immunohistochemical staining for AT2 receptor in ovary, there is no difference between control group and experimental group. According to these results, it can be concluded that PJIMH influences ovary to increase the ovulation of rats.

• 한국발생생물학회:학술대회논문집
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• 한국발생생물학회 2003년도 제3회 국제심포지움 및 학술대회
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• pp.83-83
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• 2003

The lutropin/choriogonadotropin receptor (LHR) is a member of the rhodopsin-like subfamily of G protein coupled receptor (GPCRs), that has been shown to mediate the internalization of its two naturally occurring agonist, lutropin and choriogonadotropin (CG). The clustered agonist-receptor complex is internalized by a dynamin-dependent pathway and traverses the endosomal compartment without agonist dissociation Dissociation of the agonist-receptor complex occurs in the lysosomes, where both the agonist and receptor are degrade. Recently, constitutively activating mutations of the receptor have been identified that are associated with familial male-precocious puberty (FMPP). A FMPP is a form of sexual precocious puberty in boys in which testosterone levels are elevated independent of changes in luteinizing hormone-releasing hormone and serum luteinizing hormone levels, We have now analyzed two naturally occurring, constitutively active mutants of the human LHR. These mutations were introduced into the rat LHR (rLHR) and are designated L435R and D556Y. Cells expressing rLHR-D556Y bind human choriogonadotropin (hCG) with normal affinity, exhibit a 25-fold increase in basal cAMP and respond to hCG with a normal increase in cAMP accumulation. Cells expressing rLHR-L435R also bind hCG with normal affinity, exhibit a 47-fold increase in basal cAMP, and do not respond to hCG with a further increase in cAMP accumulation. This mutation enhances the internalization of the free and agonist-occupied receptors ~2- and ~17- fold, respectively We conclude that the state of activation of the rLHR can modulate its basal and/or agonist-stimulated internalization. Since the internalization of hCG is involved in the termination of hCG actions, we suggest that the lack of responsiveness detected in cells expressing rLHR-L435R is due to the fast rate of internalization of the bound hCG. The finding that membranes expressing rLHR-L435R respond to hCG with an increase in adenylyl cyclase activity supports this suggestion. Autonomous Leydig cell activity in FMPP is caused by a constitutively activating LH/CGR.