Your search keyword '"PGRMC"' showing total 13 results

1. Effect of Steroid Hormones, Prostaglandins (E2 and F2α), Oxytocin, and Tumor Necrosis Factor Alpha on Membrane Progesterone (P4) Receptors Gene Expression in Bovine Myometrial Cells

Author

Magdalena K. Kowalik, Karolina Dobrzyn, Jaroslaw Mlynarczuk, and Robert Rekawiecki

Subjects

membrane progesterone receptors, non-genomic action, PGRMC, mPR, myometrium, uterus, Veterinary medicine, SF600-1100, Zoology, QL1-991

Abstract

Myometrium tissue shows the expression of non-genomic membrane progesterone (P4) receptors, such as progesterone receptor membrane components (PGRMC) 1 and 2 and membrane progestin receptors (mPR) alpha (mPRα), beta (mPRβ), and gamma (mPRγ). Their variable expression in the bovine uterus during the estrous cycle and early pregnancy suggests that ovarian steroids and luteotropic and/or luteolytic factors may regulate the expression of these receptors in the myometrium. Therefore, this study aimed to examine the effect of P4, estradiol (E2), P4 with E2, prostaglandins (PG) E2 and F2α, oxytocin (OT), and tumor necrosis factor α (TNFα) on the gene expression of PGRMC1, PGRMC2, serpine-1 mRNA-binding protein (SERBP1), and mPRα, mPRβ, and mPRγ in bovine myometrial cells from days 6 to 10 and 11 to 16 of the estrous cycle. The PGE2 concentration and mRNA expression were determined by EIA and real-time PCR, respectively. The data indicated that P4 and E2 can affect the mRNA expression of all studied receptors and SERPB1. However, PGE2, OT, and TNFα could only modulate the expression of PGRMC1, PGRMC2, and SERPB1, respectively. Steroids/factors changed the expression of PGRMC and mPR genes depending on the dose, the stage of the estrous cycle, and the types of receptors. This suggests that the local hormonal milieu may influence the activity of these receptors and P4 action in myometrial cells during the estrous cycle.

Published

2022

2. A novel progesterone receptor membrane component (PGRMC) in the human and swine parasite Taenia solium: implications to the host-parasite relationship

Author

Hugo Aguilar-Díaz, Karen E. Nava-Castro, Galileo Escobedo, Lenin Domínguez-Ramírez, Martín García-Varela, Víctor H. del Río-Araiza, Margarita I. Palacios-Arreola, and Jorge Morales-Montor

Subjects

Taenia solium, Cysticerci, Parasite, Helminth, PGRMC, Hormone receptors, Infectious and parasitic diseases, RC109-216

Abstract

Abstract Background We have previously reported that progesterone (P4) has a direct in vitro effect on the scolex evagination and growth of Taenia solium cysticerci. Here, we explored the hypothesis that the P4 direct effect on T. solium might be mediated by a novel steroid-binding parasite protein. Methods By way of using immunofluorescent confocal microscopy, flow cytometry analysis, double-dimension electrophoresis analysis, and sequencing the corresponding protein spot, we detected a novel PGRMC in T. solium. Molecular modeling studies accompanied by computer docking using the sequenced protein, together with phylogenetic analysis and sequence alignment clearly demonstrated that T. solium PGRMC is from parasite origin. Results Our results show that P4 in vitro increases parasite evagination and scolex size. Using immunofluorescent confocal microscopy, we detected that parasite cells showed expression of a P4-binding like protein exclusively located at the cysticercus subtegumental tissue. Presence of the P4-binding protein in cyst cells was also confirmed by flow cytometry. Double-dimension electrophoresis analysis, followed by sequencing the corresponding protein spot, revealed a protein that was previously reported in the T. solium genome belonging to a membrane-associated progesterone receptor component (PGRMC). Molecular modeling studies accompanied by computer docking using the sequenced protein showed that PGRMC is potentially able to bind steroid hormones such as progesterone, estradiol, testosterone and dihydrodrotestosterone with different affinities. Phylogenetic analysis and sequence alignment clearly demonstrated that T. solium PGRMC is related to a steroid-binding protein of Echinoccocus granulosus, both of them being nested within a cluster including similar proteins present in platyhelminths such as Schistocephalus solidus and Schistosoma haematobium. Conclusion Progesterone may directly act upon T. solium cysticerci probably by binding to PGRMC. This research has implications in the field of host-parasite co-evolution as well as the sex-associated susceptibility to this infection. In a more practical matter, present results may contribute to the molecular design of new drugs with anti-parasite actions.

Published

2018

3. Advances in the Understanding of Protein-Protein Interactions in Drug Metabolizing Enzymes through the Use of Biophysical Techniques.

Author

Lampe, Jed N.

Subjects

PROTEIN-protein interactions, DRUG metabolism, MONOAMINE oxidase

Abstract

In recent years, a growing appreciation has developed for the importance of protein-protein interactions to modulate the function of drug metabolizing enzymes. Accompanied with this appreciation, new methods and technologies have been designed for analyzing protein-protein interactions both in vitro and in vivo. These technologies have been applied to several classes of drug metabolizing enzymes, including: cytochrome P450's (CYPs), monoamine oxidases (MAOs), UDP-glucuronosyltransferases (UGTs), glutathione S-transferases (GSTs), and sulfotransferases (SULTs). In this review, we offer a brief description and assessment of the impact of many of these technologies to the study of protein-protein interactions in drug disposition. The still expanding list of these techniques and assays has the potential to revolutionize our understanding of how these enzymes carry out their important functions in vivo. [ABSTRACT FROM AUTHOR]

Published

2017

4. Molecular Characterization of Membrane Steroid Receptors in Hormone-Sensitive Cancers

Author

Erica Buoso, Emanuela Corsini, Marco Racchi, Mirco Masi, and Cristina Travelli

Subjects

TRPM8, Receptors, Steroid, OXER1, QH301-705.5, GPRC6A, Review, Biology, Models, Biological, breast cancer, Cell surface receptor, Neoplasms, Animals, Humans, Neoplastic transformation, Biology (General), Receptor, ZIP9, PGRMC, Tumor microenvironment, mPR, Cell Membrane, General Medicine, prostate cancer, GPER, Hormones, Cell biology, ovarian cancer, Nuclear receptor, endometrial cancer, Signal Transduction, Hormone

Abstract

Cancer is one of the most common causes of death worldwide, and its development is a result of the complex interaction of genetic factors, environmental cues, and aging. Hormone-sensitive cancers depend on the action of one or more hormones for their development and progression. Sex steroids and corticosteroids can regulate different physiological functions, including metabolism, growth, and proliferation, through their interaction with specific nuclear receptors, that can transcriptionally regulate target genes via their genomic actions. Therefore, interference with hormones’ activities, e.g., deregulation of their production and downstream pathways or the exposition to exogenous hormone-active substances such as endocrine-disrupting chemicals (EDCs), can affect the regulation of their correlated pathways and trigger the neoplastic transformation. Although nuclear receptors account for most hormone-related biologic effects and their slow genomic responses are well-studied, less-known membrane receptors are emerging for their ability to mediate steroid hormones effects through the activation of rapid non-genomic responses also involved in the development of hormone-sensitive cancers. This review aims to collect pre-clinical and clinical data on these extranuclear receptors not only to draw attention to their emerging role in cancer development and progression but also to highlight their dual role as tumor microenvironment players and potential candidate drug targets.

Published

2021

5. A novel progesterone receptor membrane component (PGRMC) in the human and swine parasite Taenia solium: implications to the host-parasite relationship

Author

Martín García-Varela, Galileo Escobedo, Jorge Morales-Montor, Karen Elizabeth Nava-Castro, Hugo Aguilar-Díaz, Lenin Domínguez-Ramírez, Víctor Hugo Del Río-Araiza, and Margarita Isabel Palacios-Arreola

Subjects

0301 basic medicine, Models, Molecular, Swine, Sequence alignment, Biology, Hormone receptors, Flow cytometry, Host-Parasite Interactions, lcsh:Infectious and parasitic diseases, 03 medical and health sciences, Taenia solium, Progesterone receptor, parasitic diseases, medicine, Helminth, Parasite hosting, Animals, Humans, Electrophoresis, Gel, Two-Dimensional, lcsh:RC109-216, Phylogeny, Progesterone, PGRMC, Microscopy, Confocal, medicine.diagnostic_test, Research, Sequence Analysis, DNA, Flow Cytometry, In vitro, Cell biology, Molecular Docking Simulation, Parasite, medicine.drug_formulation_ingredient, 030104 developmental biology, Infectious Diseases, Microscopy, Fluorescence, Docking (molecular), Hormone receptor, Parasitology, Cysticerci, Receptors, Progesterone, Sequence Alignment

Abstract

Background We have previously reported that progesterone (P4) has a direct in vitro effect on the scolex evagination and growth of Taenia solium cysticerci. Here, we explored the hypothesis that the P4 direct effect on T. solium might be mediated by a novel steroid-binding parasite protein. Methods By way of using immunofluorescent confocal microscopy, flow cytometry analysis, double-dimension electrophoresis analysis, and sequencing the corresponding protein spot, we detected a novel PGRMC in T. solium. Molecular modeling studies accompanied by computer docking using the sequenced protein, together with phylogenetic analysis and sequence alignment clearly demonstrated that T. solium PGRMC is from parasite origin. Results Our results show that P4 in vitro increases parasite evagination and scolex size. Using immunofluorescent confocal microscopy, we detected that parasite cells showed expression of a P4-binding like protein exclusively located at the cysticercus subtegumental tissue. Presence of the P4-binding protein in cyst cells was also confirmed by flow cytometry. Double-dimension electrophoresis analysis, followed by sequencing the corresponding protein spot, revealed a protein that was previously reported in the T. solium genome belonging to a membrane-associated progesterone receptor component (PGRMC). Molecular modeling studies accompanied by computer docking using the sequenced protein showed that PGRMC is potentially able to bind steroid hormones such as progesterone, estradiol, testosterone and dihydrodrotestosterone with different affinities. Phylogenetic analysis and sequence alignment clearly demonstrated that T. solium PGRMC is related to a steroid-binding protein of Echinoccocus granulosus, both of them being nested within a cluster including similar proteins present in platyhelminths such as Schistocephalus solidus and Schistosoma haematobium. Conclusion Progesterone may directly act upon T. solium cysticerci probably by binding to PGRMC. This research has implications in the field of host-parasite co-evolution as well as the sex-associated susceptibility to this infection. In a more practical matter, present results may contribute to the molecular design of new drugs with anti-parasite actions. Electronic supplementary material The online version of this article (10.1186/s13071-018-2703-1) contains supplementary material, which is available to authorized users.

Published

2018

6. Effect of Steroid Hormones, Prostaglandins (E2 and F2α), Oxytocin, and Tumor Necrosis Factor Alpha on Membrane Progesterone (P4) Receptors Gene Expression in Bovine Myometrial Cells.

Author

Kowalik, Magdalena K., Dobrzyn, Karolina, Mlynarczuk, Jaroslaw, and Rekawiecki, Robert

Subjects

*PROSTAGLANDIN receptors, *TUMOR necrosis factors, *STEROID receptors, *GENE expression, *STEROID hormones, *ESTRUS, *PROGESTERONE

Abstract

Simple Summary: The myometrium is one of the layers of the uterus. It consists of smooth muscle and can therefore stretch during pregnancy and contract during parturition. Thus, it can assist oocyte fertilization and its transport in the fallopian tube as well as the blastocyst implantation process. Myometrial function is regulated by the activation of several signal transduction pathways and the expression of many genes. Among them are non-genomic membrane progesterone (P4) receptors such as progesterone receptor membrane components (PGRMC) 1 and 2 and membrane progestin receptors (mPR) alpha (mPRα), beta (mPRβ), and gamma (mPRγ). Their improper action may cause disturbances in fertilization and the correct course of the estrous cycle and pregnancy. The results of this study indicate the possible role of P4, estradiol (E2), prostaglandins (PG) E2 and F2α, oxytocin (OT), and tumor necrosis factor alpha (TNFα) in the regulation of membrane P4 receptor gene expression. This suggests that the local hormonal milieu may influence the activity of these receptors and P4 action in myometrial cells during the estrous cycle. Therefore, elucidation of the mechanisms by which the action of membrane P4 receptors in the myometrium is regulated may be an important element in understanding the proper functioning of the uterus and can help to reduce abnormalities in the course of pregnancy in cows. Myometrium tissue shows the expression of non-genomic membrane progesterone (P4) receptors, such as progesterone receptor membrane components (PGRMC) 1 and 2 and membrane progestin receptors (mPR) alpha (mPRα), beta (mPRβ), and gamma (mPRγ). Their variable expression in the bovine uterus during the estrous cycle and early pregnancy suggests that ovarian steroids and luteotropic and/or luteolytic factors may regulate the expression of these receptors in the myometrium. Therefore, this study aimed to examine the effect of P4, estradiol (E2), P4 with E2, prostaglandins (PG) E2 and F2α, oxytocin (OT), and tumor necrosis factor α (TNFα) on the gene expression of PGRMC1, PGRMC2, serpine-1 mRNA-binding protein (SERBP1), and mPRα, mPRβ, and mPRγ in bovine myometrial cells from days 6 to 10 and 11 to 16 of the estrous cycle. The PGE2 concentration and mRNA expression were determined by EIA and real-time PCR, respectively. The data indicated that P4 and E2 can affect the mRNA expression of all studied receptors and SERPB1. However, PGE2, OT, and TNFα could only modulate the expression of PGRMC1, PGRMC2, and SERPB1, respectively. Steroids/factors changed the expression of PGRMC and mPR genes depending on the dose, the stage of the estrous cycle, and the types of receptors. This suggests that the local hormonal milieu may influence the activity of these receptors and P4 action in myometrial cells during the estrous cycle. [ABSTRACT FROM AUTHOR]

Published

2022

7. Transcriptional Analysis of Novel Hormone Receptors PGRMC1 and PGRMC2 as Potential Biomarkers of Breast Adenocarcinoma Staging

Author

Causey, Marlin Wayne, Huston, Laurel J., Harold, Dawn M., Charaba, Cameron J., Ippolito, Danielle L., Hoffer, Zachary S., Brown, Tommy A., and Stallings, Jonathan D.

Subjects

*BREAST cancer, *TUMOR classification, *TUMOR markers, *PROGESTERONE receptors, *GENE expression, *CARCINOGENESIS, *CARCINOMA in situ

Abstract

Background: The expression of progesterone receptor membrane component 1 (PGRMC1) in breast cancer has generated interest in this recently discovered protein because of its role in tumorigenesis. However, correlations between patient age, PGRMC1 gene expression, breast cancer morphology, and breast cancer stage have not been adequately studied. Furthermore, very little is known about possible roles for other PGRMC isoforms in breast cancer, like PGRMC2. Thus, we examined the expression of PGRMC1 and PGRMC2 mRNA by relative quantitative PCR (RelqPCR) and determined whether transcript levels correlate with age, breast cancer staging, estrogen receptor alpha (ERα) status, and other morphometric features routinely used during the pathological examination of breast ductal adenocarcinomas. Methods: Twenty-eight frozen or paraffin embedded breast cancer samples (ductal carcinoma in situ and stages I thru IV invasive ductal adenocarcinoma) and 10 control benign breast tissue samples were randomly selected and interrogated by RelqPCR to determine PGRMC1, 2, and ERα mRNA transcript levels. To control for slight variations in sample preparation, receptor transcript was normalized to the housekeeping gene phosphoglycerate kinase 1 (PGK1). Descriptive statistics and ANOVA of multiparametric datasets were used to correlate transcript levels with pathological staging parameters. Results: PGRMC1 mRNA levels decreased significantly with patient age (Pearson''s correlation –0.369; P = 0.035), whereas PGRMC2 levels did not. Although the mean relative expression of PGRMC1 significantly decreased in stage II breast cancer compared with controls (P = 0.050), it was no longer significant when age was considered a covariance (P = 0.371). On the other hand, PGRMC2 mRNA transcript was significantly decreased in stage II breast cancer when compared to stage III cancer (P = 0.028) in a manner independent of age (corrected model Bonferroni pair wise comparison, P = 0.036). Furthermore, PGRMC2 levels positively correlated with ERα mRNA transcripts in patients with ER positive tumors (Pearson''s correlation 0.503, P = 0.096). Conclusions: Decreases in PGRMC1 mRNA are partially explained by increasing patient age. On the other hand, compared to stage III, PCRMC2 mRNA was significantly decreased in stage II adenocarcinoma of the breast in an age-independent manner. Additionally, PGRMC2 mRNA levels displayed a positive correlation with ERα transcripts. Thus, in addition to morphometric pathologic staging criteria, measurements of PGRMC2 mRNA may be useful for distinguishing low stage tumors from higher stages that require more aggressive clinical management, and may be a useful test when tumor ER IHC results are equivocal. [ABSTRACT FROM AUTHOR]

Published

2011

8. Molecular identification of a PGRMC-2 receptor in maturing oocytes of the zoonotic nematode parasite Trichinella spiralis.

Author

Morales-Montor, Jorge, Colin-Oviedo, Álvaro, González, Gloria M., Palma-Nicolás, José Prisco, Sánchez-González, Alejandro, Nava-Castro, Karen Elizabeth, Domínguez-Ramírez, Lenin, García-Varela, Martín, Del Río-Araiza, Víctor Hugo, and Hernández-Bello, Romel

Subjects

*TRICHINELLA spiralis, *PROGESTERONE receptors, *OVUM, *PARASITES, *PARASITE life cycles, *RECOMBINANT proteins, *GERM cells

Abstract

[Display omitted] • We confirm and extend the presence of a Trichinella spiralis PGRMC2. • The recombinant protein produced proved to be efficient for the immunization of mice. • The membrane receptor Ts-PGRMC2 is located in the membrane of the germ cells of the parasite. • Ts-PGRMC2 probably confers a relevance on the development, as well as the differentiation and development of their offspring. • This new molecule it is important to the host-parasite relationship. We previously reported that the Trichinella nematode showed higher parasite loads in one gender than another, but also the parasite molting rate decreased when it was cultivated in the presence of progesterone. In this study we explored the hypothesis that the direct effect of progesterone on Trichinella spiralis could be mediated by a steroid-binding parasite protein. We sequenced, cloned and amplified the Cyt-domain of the progesterone receptor membrane component-2 of Trichinella spiralis (PGRMC2-Ts). Furthermore, we expressed the protein and developed an antibody to perform confocal microscopy and flow cytometry. The expression of the PGRMC2-Ts protein was exclusively detected at the oocyte and the parasite's cuticle in cross-sections of the parasite, and this expression was confirmed by western blot and flow cytometry. Molecular modeling studies and computer docking for the PGRMC2-Ts protein showed that it is potentially able to bind to progesterone, estradiol, testosterone, and dihydrotestosterone with different affinities. Furthermore, phylogenetic analysis demonstrated that T. spiralis PGRMC2 is related to a steroid-binding protein of another platyhelminth. Progesterone probably acts upon Trichinella spiralis oocytes by binding to PGRMC2-Ts. Our data showed that the PGRMC2-Ts protein is present in the parasite's oocytes, a development step that is crucial for the life cycle of the parasite. Indeed, this research might have implications in the field of host-parasite co-evolution and the sex-associated susceptibility to this infection. In a more practical matter, these results may contribute to the design of new drugs with anti-parasite effects. [ABSTRACT FROM AUTHOR]

Published

2022

9. Candidates for membrane progestin receptors—Past approaches and future challenges

Author

Zhu, Yong, Hanna, Richard N., Schaaf, Marcel J.M., Spaink, Herman P., and Thomas, Peter

Subjects

*HORMONE receptors, *PROGESTATIONAL hormones, *OVUM, *ZEBRA danio, *STEROIDS, *CELL membranes, *REPRODUCTION

Abstract

Abstract: Progestins have a broad range of functions in reproductive biology. Many rapid nongenomic actions of progestins have been identified, including induction of oocyte maturation, modulation of reproductive signaling in the brain, rapid activation of breast cancer cell signaling, induction of the acrosomal reaction and hypermotility in mammalian sperm. Currently, there are three receptor candidates for mediating rapid progestin actions: (1) membrane progestin receptors (mPRs); (2) progestin receptor membrane components (PGRMCs); and (3) nuclear progestin receptors (nPRs). The recently-described mPR family of proteins has seven integral transmembrane domains and mediates signaling via G-protein coupled pathways. The PGRMCs have a single transmembrane with putative Src homology domains for potential activation of second messengers. The classical nPRs, in addition to having well defined transcriptional activity, can also mediate rapid activation of intracellular signaling pathways. However, details of the mechanisms by which these three classes of progestin receptors mediate rapid intracellular signaling and their subcellular localization remain unclear. In addition, mPRs, nPRs and PGRMCs exhibit overlapping expression and functions in multiple tissues, implying potential interactions during oocyte maturation, parturition, and breast cancer signaling in individual cells. However, the overwhelming majority of studies to date have focused on the functions of one of these groups of receptors in isolation. This review will summarize recent findings on the three major progestin receptor candidates, emphasizing the different approaches used, some experimental pitfalls, and current controversies. We will also review evidence for the involvement of mPRs and nPRs in one of the most well-characterized nongenomic steroid actions in basal vertebrates, oocyte maturation, and conclude by suggesting some future areas of research. Clarification of the controversies surrounding the identities and localization of membrane progestin receptors may help direct future research that could advance our understanding of rapid actions of steroids. [Copyright &y& Elsevier]

Published

2008

10. Molecular Characterization of Membrane Steroid Receptors in Hormone-Sensitive Cancers.

Author

Masi, Mirco, Racchi, Marco, Travelli, Cristina, Corsini, Emanuela, and Buoso, Erica

Subjects

*STEROID receptors, *CARCINOGENESIS, *DRUG target, *STEROID hormones, *TUMOR microenvironment, *ENDOCRINE disruptors

Abstract

Cancer is one of the most common causes of death worldwide, and its development is a result of the complex interaction of genetic factors, environmental cues, and aging. Hormone-sensitive cancers depend on the action of one or more hormones for their development and progression. Sex steroids and corticosteroids can regulate different physiological functions, including metabolism, growth, and proliferation, through their interaction with specific nuclear receptors, that can transcriptionally regulate target genes via their genomic actions. Therefore, interference with hormones' activities, e.g., deregulation of their production and downstream pathways or the exposition to exogenous hormone-active substances such as endocrine-disrupting chemicals (EDCs), can affect the regulation of their correlated pathways and trigger the neoplastic transformation. Although nuclear receptors account for most hormone-related biologic effects and their slow genomic responses are well-studied, less-known membrane receptors are emerging for their ability to mediate steroid hormones effects through the activation of rapid non-genomic responses also involved in the development of hormone-sensitive cancers. This review aims to collect pre-clinical and clinical data on these extranuclear receptors not only to draw attention to their emerging role in cancer development and progression but also to highlight their dual role as tumor microenvironment players and potential candidate drug targets. [ABSTRACT FROM AUTHOR]

Published

2021

11. A novel progesterone receptor membrane component (PGRMC) in the human and swine parasite Taenia solium: implications to the host-parasite relationship

Author

Aguilar-Díaz, Hugo, Nava-Castro, Karen E., Escobedo, Galileo, Domínguez-Ramírez, Lenin, García-Varela, Martín, del Río-Araiza, Víctor H., Palacios-Arreola, Margarita I., and Morales-Montor, Jorge

Published

2018

12. Advances in the Understanding of Protein-Protein Interactions in Drug Metabolizing Enzymes through the Use of Biophysical Techniques

Author

Jed N. Lampe

Subjects

0301 basic medicine, cytochrome P450, homodimer, Review, Biology, Protein–protein interaction, protein-protein interaction, 03 medical and health sciences, In vivo, cytochrome b5, heterodimer, Pharmacology (medical), PGRMC, allosterism, Pharmacology, chemistry.chemical_classification, cytochrome P450 reductase, 030102 biochemistry & molecular biology, Drug disposition, lcsh:RM1-950, Cytochrome P450, Cytochrome P450 reductase, 3. Good health, Drug metabolizing enzymes, 030104 developmental biology, Enzyme, lcsh:Therapeutics. Pharmacology, chemistry, Biochemistry, biology.protein, Function (biology)

Abstract

In recent years, a growing appreciation has developed for the importance of protein-protein interactions to modulate the function of drug metabolizing enzymes. Accompanied with this appreciation, new methods and technologies have been designed for analyzing protein-protein interactions both in vitro and in vivo. These technologies have been applied to several classes of drug metabolizing enzymes, including: cytochrome P450’s (CYPs), monoamine oxidases (MAO’s), UDP-glucuronosyltransferases (UGTs), glutathione S-transferases (GSTs), and sulfotransferases (SULTs). In this review, we offer a brief description and assessment of the impact of many of these technologies to the study of protein-protein interactions in drug disposition. The still expanding list of these techniques and assays has the potential to revolutionize our understanding of how these enzymes carry out their important functions in vivo.

Published

2017

13. A novel progesterone receptor membrane component (PGRMC) in the human and swine parasite <italic>Taenia solium</italic>: implications to the host-parasite relationship.

Author

Aguilar-Díaz, Hugo, Nava-Castro, Karen E., Escobedo, Galileo, Domínguez-Ramírez, Lenin, García-Varela, Martín, del Río-Araiza, Víctor H., Palacios-Arreola, Margarita I., and Morales-Montor, Jorge

Subjects

PROGESTERONE receptors, CARRIER proteins, PHYLOGENY, POLYMERASE chain reaction, SCHISTOSOMA haematobium

Abstract

Background: We have previously reported that progesterone (P4) has a direct in vitro effect on the scolex evagination and growth of Taenia solium cysticerci. Here, we explored the hypothesis that the P4 direct effect on T. solium might be mediated by a novel steroid-binding parasite protein. Methods: By way of using immunofluorescent confocal microscopy, flow cytometry analysis, double-dimension electrophoresis analysis, and sequencing the corresponding protein spot, we detected a novel PGRMC in T. solium. Molecular modeling studies accompanied by computer docking using the sequenced protein, together with phylogenetic analysis and sequence alignment clearly demonstrated that T. solium PGRMC is from parasite origin. Results: Our results show that P4 in vitro increases parasite evagination and scolex size. Using immunofluorescent confocal microscopy, we detected that parasite cells showed expression of a P4-binding like protein exclusively located at the cysticercus subtegumental tissue. Presence of the P4-binding protein in cyst cells was also confirmed by flow cytometry. Double-dimension electrophoresis analysis, followed by sequencing the corresponding protein spot, revealed a protein that was previously reported in the T. solium genome belonging to a membrane-associated progesterone receptor component (PGRMC). Molecular modeling studies accompanied by computer docking using the sequenced protein showed that PGRMC is potentially able to bind steroid hormones such as progesterone, estradiol, testosterone and dihydrodrotestosterone with different affinities. Phylogenetic analysis and sequence alignment clearly demonstrated that T. solium PGRMC is related to a steroid-binding protein of Echinoccocus granulosus, both of them being nested within a cluster including similar proteins present in platyhelminths such as Schistocephalus solidus and Schistosoma haematobium. Conclusion: Progesterone may directly act upon T. solium cysticerci probably by binding to PGRMC. This research has implications in the field of host-parasite co-evolution as well as the sex-associated susceptibility to this infection. In a more practical matter, present results may contribute to the molecular design of new drugs with anti-parasite actions. [ABSTRACT FROM AUTHOR]

Published

2018