Your search keyword '"GLYCOSYLPHOSPHATIDYLINOSITOL"' showing total 1,919 results

1. Biallelic PIGM Coding Variant Causes Intractable Epilepsy and Intellectual Disability Without Thrombotic Events.

Author

Heimer, Gali, Pode‐Shakked, Ben, Marek‐Yagel, Dina, Vernitsky, Helly, Tzadok, Michal, Barel, Ortal, Eyal, Eran, Ben‐Zeev, Bruria, Atzmon, Gil, and Anikster, Yair

Subjects

*GLYCOSYLPHOSPHATIDYLINOSITOL, *CEREBRAL embolism & thrombosis, *ERYTHROCYTES, *CEREBRAL veins, *MISSENSE mutation

Abstract

ABSTRACT During the past two decades, an emerging group of genes coding for proteins involved in glycosylphosphatidylinositol (GPI) anchor biosynthesis are being implicated in early‐infantile epileptic encephalopathy. Amongst these, a hypomorphic promoter mutation in the mannosyltransferase‐encoding PIGM gene was described in seven patients to date, exhibiting intractable absence epilepsy, portal and cerebral vein thrombosis and intellectual disability (ID). We describe here three siblings exhibiting intractable epilepsy and ID, found to harbor a homozygous c.224G>A p.(Arg75His) missense variant in PIGM, which segregated with the disease in the family. The variant is evolutionary conserved, extremely rare in general population databases and predicted to be deleterious. Structural modeling of the PIGM protein and the p.(Arg75His) variant indicates that it is located in a short luminal region of the protein, predicted to be hydrophilic. Functional prediction suggests that the entire local region is sensitive to mutations, with the p.(Arg75His) variant in particular. This is the first report of a PIGM coding variant, and the second variant altogether to be described affecting this gene. This phenotype differs from that of patients with the shared PIGM promoter mutation by lack of thrombotic events and no decrease in PIGM cDNA levels or CD59 expression on red blood cells. [ABSTRACT FROM AUTHOR]

Published

2024

2. Genetically predicted metabolites mediate the association between lipidome and malignant melanoma of skin.

Author

Yuzhou Wu, Hang Ma, and Zhenyu Liu

Subjects

GENOME-wide association studies, MELANOMA, LIPID analysis, GLYCOSYLPHOSPHATIDYLINOSITOL, METABOLITES

Abstract

Objective: To investigate the causal relationship between lipidome and malignant melanoma of skin (MMOS), while identifying and quantifying the role of metabolites as potential mediators. Methods: A two-sample Mendelian randomization (MR) analysis of lipid species (n=7174) and MMOS was performed using pooled data from genome-wide association studies (GWAS). In addition, we quantified the proportion of metabolite-mediated lipidome effects on MMOS by two-step MR. Results: This study identified potential causal relationships between 11 lipids and MMOS, and 40 metabolites and MMOS, respectively. Phosphatidylethanolamine (18:0_18:2) levels mined from 179 lipids by MR Analysis increased the risk of MMOS (OR: 1.962; 95%CI:1.298,2.964; P=0.001). There is no strong evidence for a relationship between genetically predicted MMOS and phosphatidylethanolamine (18:0_18:2) levels (P=0.628). The proportion of gene predictions for phosphatidylethanolamine (18:0_18:2) levels mediated by 1-stearoyl-(glycosylphosphatidylinositol) GPI (18:0) levels was 12.40%. Conclusion: This study identifies 1-stearoyl-GPI (18:0) levels as a potentialmediator that may mediate the causal relationship between phosphatidylethanolamine (18:0_18:2) levels and MMOS, This provides direction for the investigation of MMOS, but further research of other possible potential mediators is still needed. [ABSTRACT FROM AUTHOR]

Published

2024

3. Variant surface protein GP60 contributes to host infectivity of Cryptosporidium parvum.

Author

Li, Muxiao, Yang, Fuxian, Hou, Tianyi, Gong, Xiaoqing, Li, Na, Sibley, L. David, Feng, Yaoyu, Xiao, Lihua, and Guo, Yaqiong

Subjects

*GLYCOSYLPHOSPHATIDYLINOSITOL, *SPERMATOZOA, *CRYPTOSPORIDIUM parvum, *CELL surface antigens, *PEPTIDES

Abstract

Biological studies of the determinants of Cryptosporidium infectivity are lacking despite the fact that cryptosporidiosis is a major public health problem. Recently, the 60-kDa glycoprotein (GP60) has received attention because of its high sequence polymorphism and association with host infectivity of isolates and protection against reinfection. However, studies of GP60 function have been hampered by its heavy O-linked glycosylation. Here, we used advanced genetic tools to investigate the processing, fate, and function of GP60. Endogenous gene tagging showed that the GP60 cleavage products, GP40 and GP15, are both highly expressed on the surface of sporozoites, merozoites and male gametes. During invasion, GP40 translocates to the apical end of the zoites and remains detectable at the parasite-host interface. Deletion of the signal peptide, GPI anchor, and GP15 sequences affects the membrane localization of GP40. Deletion of the GP60 gene significantly reduces parasite growth and severity of infection, and replacement of the GP60 gene with sequence from an avirulent isolate reduces the pathogenicity of a highly infective isolate. These results have revealed dynamic changes in GP60 expression during parasite development. They further suggest that GP60 is a key protein mediating host infectivity and pathogenicity. The immunodominant surface antigen GP60 undergoes dynamic changes in expression profile and localization during parasite invasion and development and is a key molecule mediating host infectivity and pathogenicity. [ABSTRACT FROM AUTHOR]

Published

2024

4. The cellular prion protein does not affect tau seeding and spreading of sarkosyl-insoluble fractions from Alzheimer's disease.

Author

Sala-Jarque, Julia, Gil, Vanessa, Andrés-Benito, Pol, Martínez-Soria, Inés, Picón-Pagès, Pol, Hernández, Félix, Ávila, Jesús, Lanciego, José Luis, Nuvolone, Mario, Aguzzi, Adriano, Gavín, Rosalina, Ferrer, Isidro, and del Río, José Antonio

Subjects

*GLYCOSYLPHOSPHATIDYLINOSITOL, *ALZHEIMER'S disease, *TAU proteins, *AMYLOID, *PRIONS

Abstract

The cellular prion protein (PrPC) plays many roles in the developing and adult brain. In addition, PrPC binds to several amyloids in oligomeric and prefibrillar forms and may act as a putative receptor of abnormal misfolded protein species. The role of PrPC in tau seeding and spreading is not known. In the present study, we have inoculated well-characterized sarkosyl-insoluble fractions of sporadic Alzheimer's disease (sAD) into the brain of adult wild-type mice (Prnp+/+), Prnp0/0 (ZH3 strain) mice, and mice over-expressing the secreted form of PrPC lacking their GPI anchor (Tg44 strain). Phospho-tau (ptau) seeding and spreading involving neurons and oligodendrocytes were observed three and six months after inoculation. 3Rtau and 4Rtau deposits from the host tau, as revealed by inoculating Mapt0/0 mice and by using specific anti-mouse and anti-human tau antibodies suggest modulation of exon 10 splicing of the host mouse Mapt gene elicited by exogenous sAD-tau. However, no tau seeding and spreading differences were observed among Prnp genotypes. Our results show that PrPC does not affect tau seeding and spreading in vivo. [ABSTRACT FROM AUTHOR]

Published

2024

5. Evolutionary rate covariation is pervasive between glycosylation pathways and points to potential disease modifiers.

Author

Thorpe, Holly J., Partha, Raghavendran, Little, Jordan, Clark, Nathan L., and Chow, Clement Y.

Subjects

*GLYCOSYLPHOSPHATIDYLINOSITOL, *PROTEIN synthesis, *DNA repair, *PATHOLOGICAL physiology, *PROTEIN analysis

Abstract

Mutations in glycosylation pathways, such as N-linked glycosylation, O-linked glycosylation, and GPI anchor synthesis, lead to Congenital Disorders of Glycosylation (CDG). CDG typically present with seizures, hypotonia, and developmental delay but display large clinical variability with symptoms affecting every system in the body. This variability suggests modifier genes might influence the phenotypes. Because of the similar physiology and clinical symptoms, there are likely common genetic modifiers between CDG. Here, we use evolution as a tool to identify common modifiers between CDG and glycosylation genes. Protein glycosylation is evolutionarily conserved from yeast to mammals. Evolutionary rate covariation (ERC) identifies proteins with similar evolutionary rates that indicate shared biological functions and pathways. Using ERC, we identified strong evolutionary rate signatures between proteins in the same and different glycosylation pathways. Genome-wide analysis of proteins showing significant ERC with GPI anchor synthesis proteins revealed strong signatures with ncRNA modification proteins and DNA repair proteins. We also identified strong patterns of ERC based on cellular sub-localization of the GPI anchor synthesis enzymes. Functional testing of the highest scoring candidates validated genetic interactions and identified novel genetic modifiers of CDG genes. ERC analysis of disease genes and biological pathways allows for rapid prioritization of potential genetic modifiers, which can provide a better understanding of disease pathophysiology and novel therapeutic targets. Author summary: Congenital Disorders of Glycosylation (CDG) are a group of rare disorders resulting from impaired protein glycosylation. Glycosylation is the addition of sugar chains onto proteins and is required for proper protein function. CDG patients typically present with seizures and hypotonia. However, they can have a large amount of clinical variability, which is likely influenced by modifier genes. Modifier genes are genes that affect a phenotype without causing the disease. Using an evolutionary method that examines proteins that evolve at similar rates, we identified proteins within glycosylation pathways and among other unexpected pathways, such as ncRNA modification and DNA repair, that could be potential genetic modifiers of CDG genes. We also tested top protein pairs using the Drosophila eye as a model and identified novel genetic modifiers of CDG genes. Broadening our understanding of CDG modifiers can help us to better understand why loss of glycosylation results in specific patient symptoms and could provide new treatment targets. [ABSTRACT FROM AUTHOR]

Published

2024

6. Apicoplast-derived isoprenoids are essential for biosynthesis of GPI protein anchors, and consequently for egress and invasion in Plasmodium falciparum.

Author

Bulloch, Michaela S., Huynh, Long K., Kennedy, Kit, Ralton, Julie E., McConville, Malcolm J., and Ralph, Stuart A.

Subjects

*GLYCOSYLPHOSPHATIDYLINOSITOL, *ERYTHROCYTES, *BIOLOGICAL membranes, *PLASMODIUM falciparum, *PLASMODIUM

Abstract

Glycophosphatidylinositol (GPI) anchors are the predominant glycoconjugate in Plasmodium parasites, enabling modified proteins to associate with biological membranes. GPI biosynthesis commences with donation of a mannose residue held by dolichol-phosphate at the endoplasmic reticulum membrane. In Plasmodium dolichols are derived from isoprenoid precursors synthesised in the Plasmodium apicoplast, a relict plastid organelle of prokaryotic origin. We found that treatment of Plasmodium parasites with apicoplast inhibitors decreases the synthesis of isoprenoid and GPI intermediates resulting in GPI-anchored proteins becoming untethered from their normal membrane association. Even when other isoprenoids were chemically rescued, GPI depletion led to an arrest in schizont stage parasites, which had defects in segmentation and egress. In those daughter parasites (merozoites) that did form, proteins that would normally be GPI-anchored were mislocalised, and when these merozoites were artificially released they were able to attach to but not invade new red blood cells. Our data provides further evidence for the importance of GPI biosynthesis during the asexual cycle of P. falciparum, and indicates that GPI biosynthesis, and by extension egress and invasion, is dependent on isoprenoids synthesised in the apicoplast. Author summary: The plastid apicoplast organelle of the malaria parasite Plasmodium falciparum has long been recognised as a drug target. However, the downstream metabolic pathways have not been fully elucidated. In this study we inhibited apicoplast function in blood-stage P. falciparum and, following the depletion of essential apicoplast-derived isoprenoids, we observed that levels of the polyisoprenoid alcohol, dolichol-phosphate, were also depleted. This led to a block in the synthesis of glycophosphatidylinositols (GPIs), which are abundant plasma membrane glycolipids and serve as membrane anchors for major surface proteins. Severe parasite impairments followed with incomplete membrane segmentation of their daughter merozoites, which could subsequently neither egress nor reinvade host red blood cells. Our data implicates dolichol as an essential parasite metabolite, dependent on normal apicoplast function, and reveals novel roles for GPI anchored proteins. The widespread phenotype following disrupted dolichol synthesis supports aspects of GPI biosynthesis as potential future drug targets. [ABSTRACT FROM AUTHOR]

Published

2024

7. JAGGER localization and function are dependent on GPI anchor addition.

Author

Figueiredo, Raquel, Costa, Mónica, Moreira, Diana, Moreira, Miguel, Noble, Jennifer, Pereira, Luís Gustavo, Melo, Paula, Palanivelu, Ravishankar, Coimbra, Sílvia, and Pereira, Ana Marta

Subjects

*GLYCOSYLPHOSPHATIDYLINOSITOL, *POLLEN tube, *FLUORESCENT proteins, *ARABIDOPSIS proteins, *CELL membranes, *OVULES

Abstract

Key message: GPI anchor addition is important for JAGGER localization and in vivo function. Loss of correct GPI anchor addition in JAGGER, negatively affects its localization and function. In flowering plants, successful double fertilization requires the correct delivery of two sperm cells to the female gametophyte inside the ovule. The delivery of a single pair of sperm cells is achieved by the entrance of a single pollen tube into one female gametophyte. To prevent polyspermy, Arabidopsis ovules avoid the attraction of multiple pollen tubes to one ovule–polytubey block. In Arabidopsisjagger mutants, a significant number of ovules attract more than one pollen tube to an ovule due to an impairment in synergid degeneration. JAGGER encodes a putative arabinogalactan protein which is predicted to be anchored to the plasma membrane by a glycosylphosphatidylinositol (GPI) anchor. Here, we show that JAGGER fused to citrine yellow fluorescent protein (JAGGER-cYFP) is functional and localizes mostly to the periphery of ovule integuments and transmitting tract cells. We further investigated the importance of GPI-anchor addition domains for JAGGER localization and function. Different JAGGER proteins with deletions in predicted ω-site regions and GPI attachment signal domain, expected to compromise the addition of the GPI anchor, led to disruption of JAGGER localization in the cell periphery. All JAGGER proteins with disrupted localization were also not able to rescue the polytubey phenotype, pointing to the importance of GPI-anchor addition to in vivo function of the JAGGER protein. [ABSTRACT FROM AUTHOR]

Published

2024

8. 鱼源荧光假单胞菌分泌蛋白的全基因组预测与功能分析.

Author

李秋莹, 张雪婷, 崔方超, 檀茜倩, 孙 彤, and 励建荣

Subjects

GLYCOSYLPHOSPHATIDYLINOSITOL, FISH spoilage, MARINE fishes, SIGNAL peptides, PSEUDOMONAS fluorescens, BIOINFORMATICS software

Abstract

Copyright of Journal of Chinese Institute of Food Science & Technology is the property of Journal of Chinese Institute of Food Science & Technology Periodical Office and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2024

9. Inherited glycosylphosphatidylinositol deficiency: a review from molecular and clinical perspectives

Author

Li Shan, Tang Qi, Jiang Yuwu, and Chen Xing

Subjects

glycosylation, glycosylphosphatidylinositol, inherited GPI deficiency, Biochemistry, QD415-436, Genetics, QH426-470

Abstract

Glycosylphosphatidylinositol (GPI) is a highly conserved post-translational modification in eukaryotes, which is essential for anchoring various proteins to the cell surface. Dysfunction of GPI biogenesis leads to human diseases, such as inherited GPI deficiency (IGD) caused by germline mutations in GPI-related genes. With accumulating reports on individuals with IGD, there has been increasing interest and studies on disease mechanism, diagnosis, and therapy. This review outlines the biosynthetic pathway of GPI-anchored proteins (GPI-APs) and summarizes clinical IGD cases from a molecular perspective. We also review current diagnostic and therapeutic approaches for IGD. Finally, we discuss future research directions to facilitate the understanding and treatment of GPI-related disorders.

Published

2024

10. The major surface protein of malaria sporozoites is GPI-anchored to the plasma membrane.

Author

Nagar, Rupa, Garcia Castillo, Stefano S., Pinzon-Ortiz, Maria, Patray, Sharon, Coppi, Alida, Kanatani, Sachie, Moritz, Robert L., Swearingen, Kristian E., Ferguson, Michael A. J., and Sinnis, Photini

Subjects

*GLYCOSYLPHOSPHATIDYLINOSITOL, *CIRCUMSPOROZOITE protein, *PLASMODIUM falciparum, *CELL membranes, *PLASMODIUM

Abstract

Glycosylphosphatidylinositol (GPI) anchor protein modification in Plasmodium species is well known and represents the principal form of glycosylation in these organisms. The structure and biosynthesis of GPI anchors of Plasmodium spp. has been primarily studied in the asexual blood stage of Plasmodium falciparum and is known to contain the typical conserved GPI structure of EtN-P-Man3GlcN-PI. Here, we have investigated the circumsporozoite protein (CSP) for the presence of a GPI anchor. CSP is the major surface protein of Plasmodium sporozoites, the infective stage of the malaria parasite. While it is widely assumed that CSP is a GPI-anchored cell surface protein, compelling biochemical evidence for this supposition is absent. Here, we employed metabolic labeling and mass-spectrometry-based approaches to confirm the presence of a GPI anchor in CSP. Biosynthetic radiolabeling of CSP with [ ³H]-palmitic acid and [³H]-ethanolamine, with the former being base-labile and therefore ester-linked, provided strong evidence for the presence of a GPI anchor on CSP, but these data alone were not definitive. To provide further evidence, immunoprecipitated CSP was analyzed for the presence of myo-inositol (a characteristic component of GPI anchor) using strong acid hydrolysis and GC-MS for highly sensitive and quantitative detection. The single ion monitoring (SIM) method for GC-MS analysis confirmed the presence of the myo-inositol component in CSP. Taken together, these data provide confidence that the long-assumed presence of a GPI anchor on this important parasite protein is correct. [ABSTRACT FROM AUTHOR]

Published

2024

11. Glycosylphosphatidylinositol anchor biosynthesis pathway-based biomarker identification with machine learning for prognosis and T cell exhaustion status prediction in breast cancer.

Author

Haodong Wu, Zhixuan Wu, Hongfeng Li, Ziqiong Wang, Yao Chen, Jingxia Bao, Buran Chen, Shuning Xu, Erjie Xia, Daijiao Ye, and Xuanxuan Dai

Subjects

T-cell exhaustion, GLYCOSYLPHOSPHATIDYLINOSITOL, BIOSYNTHESIS, BREAST cancer, MACHINE learning

Abstract

As the primary component of anti-tumor immunity, T cells are prone to exhaustion and dysfunction in the tumor microenvironment (TME). A thorough understanding of T cell exhaustion (TEX) in the TME is crucial for effectively addressing TEX in clinical settings and promoting the efficacy of immune checkpoint blockade therapies. In eukaryotes, numerous cell surface proteins are tethered to the plasma membrane via Glycosylphosphatidylinositol (GPI) anchors, which play a crucial role in facilitating the proper translocation of membrane proteins. However, the available evidence is insufficient to support any additional functional involvement of GPI anchors. Here, we investigate the signature of GPI-anchor biosynthesis in the TME of breast cancer (BC)patients, particularly its correlation with TEX. GPI-anchor biosynthesis should be considered as a prognostic risk factor for BC. Patients with high GPI-anchor biosynthesis showed more severe TEX. And the levels of GPI-anchor biosynthesis in exhausted CD8 T cells was higher than normal CD8 T cells, which was not observed between malignant epithelial cells and normal mammary epithelial cells. In addition, we also found that GPI -anchor biosynthesis related genes can be used to diagnose TEX status and predict prognosis in BC patients, both the TEX diagnostic model and the prognostic model showed good AUC values. Finally, we confirmed our findings in cells and clinical samples. Knockdown of PIGU gene expression significantly reduced the proliferation rate of MDA-MB-231 and MCF-7 cell lines. Immunofluorescence results from clinical samples showed reduced aggregation of CD8 T cells in tissues with high expression of GPAA1 and PIGU. [ABSTRACT FROM AUTHOR]

Published

2024

12. A case of inherited glycosylphosphatidylinositol deficiency caused by PGAP3 variant with uniparental isodisomy on chromosome 17.

Author

Mukai, Takeo, Kato, Shota, Tanaka, Hiroyuki, Kuroda, Yukiko, Kitaoka, Hiroki, Ito, Atsushi, Shitara, Yoshihiko, Kashima, Kohei, Takami, Hirokazu, Takahashi, Naoto, and Kato, Motohiro

Subjects

*GLYCOSYLPHOSPHATIDYLINOSITOL, *MAGNETIC resonance imaging, *ALKALINE phosphatase, *CHROMOSOMES, *SOFT palate, *MAGNETIC recording heads

Abstract

Background: Inherited glycosylphosphatidylinositol (GPI) deficiency is an autosomal recessive disease and a set of syndromes caused by different genes involved in the biosynthesis of phosphatidylinositol characterized by severe cognitive disability, elevated serum alkaline phosphatase (ALP) levels, and distinct facial features. This report presents a patient with inherited GPI deficiency caused by a homozygous frameshift variant of PGAP3 due to uniparental isodisomy (UPiD) on chromosome 17. Method: Clinical characteristics of the patient were collected. Microarray analysis followed by adaptive sampling sequencing targeting chromosome 17 was used for the identification of variants. Sanger sequencing was used to confirm the variant in the target region. Results: The patient was born at 38 weeks of gestation with a birthweight of 3893 g. He had a distinctive facial appearance with hypertelorism, wide nasal bridge, and cleft soft palate. Postnatal head magnetic resonance imaging revealed a Blake's pouch cyst. The serum ALP level was 940 IU/L at birth and increased to 1781 IU/L at 28 days of age. Microarray analysis revealed region of homozygosity in nearly the entire region of chromosome 17, leading to the diagnosis of UPiD. Adaptive sampling sequencing targeting chromosome 17 confirmed the homozygous variant NM_033419:c.778dupG (p.Val260Glyfs*14) in the PGAP3 gene, resulting in a diagnosis of inherited GPI deficiency. Conclusion: This is the first report of inherited GPI deficiency caused by UPiD. Inherited GPI deficiency must be considered in patients with unexplained hyperphosphatasemia. [ABSTRACT FROM AUTHOR]

Published

2024

13. Production of CA125 with Tn antigens using a glycosylphosphatidylinositol anchoring system.

Author

Tang, Yu-He, Leng, Ji-Xiong, Yang, Ganglong, Gao, Xiao-Dong, Liu, Yi-Shi, and Fujita, Morihisa

Subjects

*THREONINE, *GLYCANS, *GLYCOSYLPHOSPHATIDYLINOSITOL, *BIOMARKERS, *ANTIGENS, *CANCER diagnosis

Abstract

Cancer antigen 125 (CA125) is a serum marker associated with ovarian cancer. Despite its widespread use, CA125 levels can also be elevated in benign conditions. Recent reports suggest that detecting serum CA125 that carries the Tn antigen, a truncated O -glycan containing only N -acetylgalactosamine on serine or threonine residues, can improve the specificity of ovarian cancer diagnosis. In this study, we engineered cells to express CA125 with a Tn antigen. To achieve this, we knocked out C1GALT1 and SLC35A1 , genes encoding Core1 synthase and a transporter for cytidine-5′-monophospho-sialic acid respectively, in human embryonic kidney 293 (HEK293) cells. In ClGALT1-SLC35A1-knockout (KO) cells, the expression of the Tn antigen showed a significant increase, whereas the expression of the T antigen (galactose-β1,3- N -acetylgalactosamine on serine or threonine residues) was decreased. Due to the inefficient secretion of soluble CA125, we employed a glycosylphosphatidylinositol (GPI) anchoring system. This allowed for the expression of GPI-anchored CA125 on the cell surface of ClGALT1-SLC35A1-KO cells. Cells expressing high levels of GPI-anchored CA125 were then enriched through cell sorting. By knocking out the PGAP2 gene, the GPI-anchored form of CA125 was converted to a secretory form. Through the engineering of O -glycans and the use of a GPI-anchoring system, we successfully produced CA125 with Tn antigen modification. [ABSTRACT FROM AUTHOR]

Published

2024

14. MDGAs perform activity-dependent synapse type-specific suppression via distinct extracellular mechanisms.

Author

Seungjoon Kim, Gyubin Jang, Hyeonho Kim, Dongseok Lim, Kyung Ah Han, Ji Won Um, and Jaewon Ko

Subjects

*SYNAPSES, *NEURAL transmission, *GLYCOSYLPHOSPHATIDYLINOSITOL, *NEURAL circuitry, *NEURONS

Abstract

MDGA (MAM domain containing glycosylphosphatidylinositol anchor) family proteins were previously identified as synaptic suppressive factors. However, various genetic manipulations have yielded often irreconcilable results, precluding precise evaluation of MDGA functions. Here, we found that, in cultured hippocampal neurons, conditional deletion of MDGA1 and MDGA2 causes specific alterations in synapse numbers, basal synaptic transmission, and synaptic strength at GABAergic and glutamatergic synapses, respectively. Moreover, MDGA2 deletion enhanced both N-methyl-D-aspartate (NMDA) receptor- and a-amino-3-hydroxy-5-methylisoxazole-4-propionic acid (AMPA) receptor-mediated postsynaptic responses. Strikingly, ablation of both MDGA1 and MDGA2 abolished the effect of deleting individual MDGAs that is abrogated by chronic blockade of synaptic activity. Molecular replacement experiments further showed that MDGA1 requires the meprin/ A5 protein/PTPmu (MAM) domain, whereas MDGA2 acts via neuroligin-dependent and/or MAM domain-dependent pathways to regulate distinct postsynaptic properties. Together, our data demonstrate that MDGA paralogs act as unique negative regulators of activity-dependent postsynaptic organization at distinct synapse types, and cooperatively contribute to adjustment of excitation--inhibition balance. [ABSTRACT FROM AUTHOR]

Published

2024

15. Multiple Congenital Anomalies-Hypotonia-Seizures Syndrome 2 Caused by a Novel PIGA Variant Not Associated with a Skewed X-Inactivation Pattern.

Author

Gabaldon-Albero, Alba, Cordon, Lourdes, Sempere, Amparo, Pedrola, Laia, Martin-Grau, Carla, Oltra, Silvestre, Monfort, Sandra, Caro-Llopis, Alfonso, Dominguez-Martinez, Marta, Hernandez-Muela, Sara, Rosello, Monica, Orellana, Carmen, and Martinez, Francisco

Subjects

*GENETIC variation, *SYNDROMES, *GLYCOSYLPHOSPHATIDYLINOSITOL, *GERM cells, *BIOSYNTHESIS

Abstract

Germline variants in the phosphatidylinositol glycan class A (PIGA) gene, which is involved in glycosylphosphatidylinositol (GPI) biosynthesis, cause multiple congenital anomalies-hypotonia-seizures syndrome 2 (MCAHS2) with X-linked recessive inheritance. The available literature has described a pattern of almost 100% X-chromosome inactivation in mothers carrying PIGA variants. Here, we report a male infant with MCAHS2 caused by a novel PIGA variant inherited from his mother, who has a non-skewed pattern of X inactivation. Phenotypic evidence supporting the pathogenicity of the variant was obtained by flow-cytometry tests. We propose that the assessment in neutrophils of the expression of GPI-anchored proteins (GPI-APs), especially CD16, should be considered in cases with variants of unknown significance with random X-inactivation in carrier mothers in order to clarify the pathogenic role of PIGA or other gene variants linked to the synthesis of GPI-APs. [ABSTRACT FROM AUTHOR]

Published

2024

16. PIGW-related glycosylphosphatidylinositol deficiency: A case report and literature review.

Author

Fang, Zhixu, Hu, Chaoping, Zhou, Shuizhen, and Yu, Lifei

Subjects

*LITERATURE reviews, *GLYCOSYLPHOSPHATIDYLINOSITOL, *EPILEPSY, *DISABILITIES, *ALKALINE phosphatase, *GENETIC variation

Abstract

Introduction: PIGW-related glycosylphosphatidylinositol deficiency is a rare disease that manifests heterogeneous clinical phenotypes. Methods: We describe a patient with PIGW deficiency and summarize the clinical characteristics of the case. In addition, we conducted a literature review of previously reported patients with pathogenic variants of PIGW. Results: A Chinese girl presented with refractory epilepsy, severe intellectual disability, recurrent respiratory infections, and hyperphosphatasia. Seizures worsened during fever and infections, making her more susceptible to epileptic status. She was found to carry a heterozygous variant of PIGW and a deletion of chromosome 17q12 containing PIGW. Only six patients with homozygous or compound heterozygous pathogenic variants of PIGW have been identified in the literature thus far. Epileptic seizures were reported in all patients, and the most common types of seizures were epileptic spasms. Distinctive facial and physical features and recurrent respiratory infections are common in these patients with developmental delays. Serum alkaline phosphatase (ALP) levels were elevated in four of the six patients. Conclusions: PIGW-related glycosylphosphatidylinositol deficiency is characterized by developmental delay, epilepsy, distinctive facial features, and multiple organ anomalies. Genetic testing is an important method for diagnosing this disease, and flow cytometry and serum ALP level detection are crucial complements for genetic testing. [ABSTRACT FROM AUTHOR]

Published

2024

17. Protein sorting upon exit from the endoplasmic reticulum dominates Golgi biogenesis in budding yeast.

Author

Sasaki, Saku, Schlarmann, Philipp, Hanaoka, Kazuki, Nishii, Hinako, Moriya, Hisao, Muñiz, Manuel, and Funato, Kouichi

Subjects

*ENDOPLASMIC reticulum, *MEMBRANE lipids, *GLYCOSYLPHOSPHATIDYLINOSITOL, *PROTEINS, *YEAST, *CERAMIDES

Abstract

Cells sense and control the number and quality of their organelles, but the underlying mechanisms of this regulation are not understood. Our recent research in the yeast Saccharomyces cerevisiae has shown that long acyl chain ceramides in the endoplasmic reticulum (ER) membrane and the lipid moiety of glycosylphosphatidylinositol (GPI) anchor determine the sorting of GPI‐anchored proteins in the ER. Here, we show that a mutant strain, which produces shorter ceramides than the wild‐type strain, displays a different count of Golgi cisternae. Moreover, deletions of proteins that remodel the lipid portion of GPI anchors resulted in an abnormal number of Golgi cisternae. Thus, our study reveals that protein sorting in the ER plays a critical role in maintaining Golgi biogenesis. [ABSTRACT FROM AUTHOR]

Published

2024

18. Drosophila models of phosphatidylinositol glycan biosynthesis class A congenital disorder of glycosylation (PIGA-CDG) mirror patient phenotypes.

Author

Thorpe, Holly J, Owings, Katie G, Aziz, Miriam C, Haller, Madelyn, Coelho, Emily, and Chow, Clement Y

Subjects

*CONGENITAL disorders, *DROSOPHILA, *GLYCOSYLPHOSPHATIDYLINOSITOL, *BIOSYNTHESIS, *GLYCANS, *GLYCOSYLATION, *RECESSIVE genes

Abstract

Mutations in the phosphatidylinositol glycan biosynthesis class A (PIGA) gene cause a rare, X-linked recessive congenital disorder of glycosylation. Phosphatidylinositol glycan biosynthesis class A congenital disorder of glycosylation (PIGA-CDG) is characterized by seizures, intellectual and developmental delay, and congenital malformations. The PIGA gene encodes an enzyme involved in the first step of glycosylphosphatidylinositol (GPI) anchor biosynthesis. There are over 100 GPI-anchored proteins that attach to the cell surface and are involved in cell signaling, immunity, and adhesion. Little is known about the pathophysiology of PIGA-CDG. Here, we describe the first Drosophila model of PIGA-CDG and demonstrate that loss of PIG-A function in Drosophila accurately models the human disease. As expected, complete loss of PIG-A function is larval lethal. Heterozygous null animals appear healthy but, when challenged, have a seizure phenotype similar to what is observed in patients. To identify the cell-type specific contributions to disease, we generated neuron- and glia-specific knockdown of PIG-A. Neuron-specific knockdown resulted in reduced lifespan and a number of neurological phenotypes but no seizure phenotype. Glia-knockdown also reduced lifespan and, notably, resulted in a very strong seizure phenotype. RNA sequencing analyses demonstrated that there are fundamentally different molecular processes that are disrupted when PIG-A function is eliminated in different cell types. In particular, loss of PIG-A in neurons resulted in upregulation of glycolysis, but loss of PIG-A in glia resulted in upregulation of protein translation machinery. Here, we demonstrate that Drosophila is a good model of PIGA-CDG and provide new data resources for future study of PIGA-CDG and other GPI anchor disorders. [ABSTRACT FROM AUTHOR]

Published

2024

19. GPI-anchored Gas1 protein regulates cytosolic proteostasis in budding yeast.

Author

Wang, Yuhao, Ruan, Linhao, and Li, Rong

Subjects

*GLYCOSYLPHOSPHATIDYLINOSITOL, *PROTEOLYSIS, *FUNGAL cell walls, *CELLULAR aging, *PROTEIN synthesis, *YEAST, *MITOCHONDRIAL proteins

Abstract

The decline in protein homeostasis (proteostasis) is a hallmark of cellular aging and aging-related diseases. Maintaining a balanced proteostasis requires a complex network of molecular machineries that govern protein synthesis, folding, localization, and degradation. Under proteotoxic stress, misfolded proteins that accumulate in cytosol can be imported into mitochondria for degradation through the "mitochondrial as guardian in cytosol" (MAGIC) pathway. Here, we report an unexpected role of Gas1, a cell wall-bound glycosylphosphatidylinositol (GPI)-anchored β-1,3-glucanosyltransferase in the budding yeast, in differentially regulating MAGIC and ubiquitin-proteasome system (UPS). Deletion of GAS1 inhibits MAGIC but elevates protein ubiquitination and UPS-mediated protein degradation. Interestingly, we found that the Gas1 protein exhibits mitochondrial localization attributed to its C-terminal GPI anchor signal. But this mitochondria-associated GPI anchor signal is not required for mitochondrial import and degradation of misfolded proteins through MAGIC. By contrast, catalytic inactivation of Gas1 via the gas1-E161Q mutation inhibits MAGIC but not its mitochondrial localization. These data suggest that the glucanosyltransferase activity of Gas1 is important for regulating cytosolic proteostasis. [ABSTRACT FROM AUTHOR]

Published

2024

20. Stable expression of mucin glycoproteins GP40 and GP15 of Cryptosporidium parvum in Toxoplasma gondii.

Author

Li, Muxiao, Sun, Xiaohua, Chen, Haoyu, Li, Na, Feng, Yaoyu, Xiao, Lihua, and Guo, Yaqiong

Subjects

*CRYPTOSPORIDIUM, *CRYPTOSPORIDIUM parvum, *TOXOPLASMA gondii, *GLYCOPROTEINS, *MUCINS, *GLYCOSYLPHOSPHATIDYLINOSITOL

Abstract

Background: Cryptosporidium spp. are common protozoa causing diarrhea in humans and animals. There are currently only one FDA-approved drug and no vaccines for cryptosporidiosis, largely due to the limited knowledge of the molecular mechanisms involved in the invasion of the pathogens. Previous studies have shown that GP60, which is cleaved into GP40 and GP15 after expression, is an immunodominant mucin protein involved in the invasion of Cryptosporidium. The protein is highly O-glycosylated, and recombinant proteins expressed in prokaryotic systems are non-functional. Therefore, few studies have investigated the function of GP40 and GP15. Methods: To obtain recombinant GP40 with correct post-translational modifications, we used CRISPR/Cas9 technology to insert GP40 and GP15 into the UPRT locus of Toxoplasma gondii, allowing heterologous expression of Cryptosporidium proteins. In addition, the Twin-Strep tag was inserted after GP40 for efficient purification of GP40. Results: Western blotting and immunofluorescent microscopic analyses both indicated that GP40 and GP15 were stably expressed in T. gondii mutants. GP40 localized not only in the cytoplasm of tachyzoites but also in the parasitophorous vacuoles, while GP15 without the GPI anchor was expressed only in the cytoplasm. In addition, a large amount of recTgGP40 was purified using Strep-TactinXT supported by a visible band of ~ 50 kDa in SDS-PAGE. Conclusions: The establishment of a robust and efficient heterologous expression system of GP40 in T. gondii represents a novel approach and concept for investigating Cryptosporidium mucins, overcoming the limitations of previous studies that relied on unstable transient transfection, which involved complex steps and high costs. [ABSTRACT FROM AUTHOR]

Published

2024

21. Investigation of Glycosylphosphatidylinositol (GPI)‐Plasma Membrane Interaction in Live Cells and the Influence of GPI Glycan Structure on the Interaction.

Author

Kundu, Sayan, Jaiswal, Mohit, Babu Mullapudi, Venkanna, Guo, Jiatong, Kamat, Manasi, Basso, Kari B., and Guo, Zhongwu

Subjects

*GLYCAN structure, *GLYCOSYLPHOSPHATIDYLINOSITOL, *MEMBRANE proteins, *PROTEIN crosslinking, *CELLULAR signal transduction, *CELL membranes

Abstract

Glycosylphosphatidylinositols (GPIs) need to interact with other components in the cell membrane to transduce transmembrane signals. A bifunctional GPI probe was employed for photoaffinity‐based proximity labelling and identification of GPI‐interacting proteins in the cell membrane. This probe contained the entire core structure of GPIs and was functionalized with photoreactive diazirine and clickable alkyne to facilitate its crosslinking with proteins and attachment of an affinity tag. It was disclosed that this probe was more selective than our previously reported probe containing only a part structure of the GPI core for cell membrane incorporation and an improved probe for studying GPI‐cell membrane interaction. Eighty‐eight unique membrane proteins, many of which are related to GPIs/GPI‐anchored proteins, were identified utilizing this probe. The proteomics dataset is a valuable resource for further analyses and data mining to find new GPI‐related proteins and signalling pathways. A comparison of these results with those of our previous probe provided direct evidence for the profound impact of GPI glycan structure on its interaction with the cell membrane. [ABSTRACT FROM AUTHOR]

Published

2024

22. Climate change: approach to intervention using expression vector for carbonic anhydrase via glycosylphosphatidylinositol.

Author

Huili, Zhang, Li, Kefeng, and Nguyen, Khue Vu

Subjects

*CARBONIC anhydrase, *CLIMATE change, *GLYCOSYLPHOSPHATIDYLINOSITOL, *GREENHOUSE gases, *ATMOSPHERE, *MEDICAL climatology, *NATURAL disasters

Abstract

Climate change is a change in the usual weather found in a place. The climate change has a major impact not only on natural disasters of the Earth but also on human health. The climate crisis is then no longer a future concern. It includes both the global warming driven by human emissions of greenhouse gases (GHG), and the resulting large-scale shifts in weather patterns. Global warming can occur from a variety of causes, both natural and human induced. The primary GHG in Earth's atmosphere, listed in decreasing order of average global mole fraction, are: water vapor (H2O), carbon dioxide (CO2), methane (CH4), nitrous oxide (N2O), and ozone (O3). Today, scientists around the world continue to try and solve the puzzle of climate change. It is clear that to address climate change, the amount of CO2 released into the atmosphere by industrial process has to be reduced because once it is added to the atmosphere, it can continue to affect climate for thousands of years. For such a purpose, an approach to intervention using expression vectors for any protein targeting to the cell plasma membrane via the glycosylphosphatidylinositol, GPI, anchor is suggested. The resulting GPI-anchored proteins would be useful for studying intermolecular interactions, especially gene-environment interactions, in investigating the potential impact of any chemical compounds on any genes of interest and could be used for carbonic anhydrase (CA)-based CO2-capture (environmental application). This approach would be crucial not only for capturing CO2via GPI and CA but also for the production of CA enzyme as well as its stabilization and therefore useful for combating the global warming of climate change. [ABSTRACT FROM AUTHOR]

Published

2024

23. mRNA vaccines expressing malaria transmission-blocking antigens Pfs25 and Pfs230D1 induce a functional immune response.

Author

Scaria, Puthupparampil V., Roth, Nicole, Schwendt, Kim, Muratova, Olga V., Alani, Nada, Lambert, Lynn E., Barnafo, Emma K., Rowe, Christopher G., Zaidi, Irfan U., Rausch, Kelly M., Narum, David L., Petsch, Benjamin, and Duffy, Patrick E.

Subjects

MALARIA, MALARIA vaccines, GLYCOSYLPHOSPHATIDYLINOSITOL, CELL surface antigens, MESSENGER RNA, INSECTICIDE resistance, IMMUNE response

Abstract

Malaria transmission-blocking vaccines (TBV) are designed to inhibit the sexual stage development of the parasite in the mosquito host and can play a significant role in achieving the goal of malaria elimination. Preclinical and clinical studies using protein–protein conjugates of leading TBV antigens Pfs25 and Pfs230 domain 1 (Pfs230D1) have demonstrated the feasibility of TBV. Nevertheless, other promising vaccine platforms for TBV remain underexplored. The recent success of mRNA vaccines revealed the potential of this technology for infectious diseases. We explored the mRNA platform for TBV development. mRNA constructs of Pfs25 and Pfs230D1 variously incorporating signal peptides (SP), GPI anchor, and Trans Membrane (TM) domain were assessed in vitro for antigen expression, and selected constructs were evaluated in mice. Only mRNA constructs with GPI anchor or TM domain that resulted in high cell surface expression of the antigens yielded strong immune responses in mice. These mRNA constructs generated higher transmission-reducing functional activity versus the corresponding alum-adjuvanted protein-protein conjugates used as comparators. Pfs25 mRNA with GPI anchor or TM maintained >99% transmission reducing activity through 126 days, the duration of the study, demonstrating the potential of mRNA platform for TBV. [ABSTRACT FROM AUTHOR]

Published

2024

24. Synthesis of glycosylphosphatidylinositol analogues with an unnatural β-D-glucosamine-(1→6)-myo-inositol motif.

Author

Yan, Xin and Guo, Zhongwu

Subjects

*CLICK chemistry, *GLYCOSYLPHOSPHATIDYLINOSITOL, *INOSITOL, *MOIETIES (Chemistry), *GLYCOSYLATION

Abstract

Glycosylphosphatidylinositol (GPI) anchors contain a unique α-D-glucosamine-(1→6)-myo-inositol [αGlcN(1,6)Ins] motif in their conserved core structure. To facilitate investigations of the functional roles of this structural motif, two GPI analogues containing unnatural βGlcN(1,6)Ins, instead of αGlcN(1,6)Ins, and an alkyne group at different positions of the GPI core were designed and synthesized. To this end, an orthogonally protected pseudopentasaccharide derivative of GPIs with the βGlcN(1,6)Ins motif was convergently constructed via [3 + 2] glycosylation and used as the common intermediate to prepare both GPI analogues by streamlined synthetic protocols. The pseudopentasaccharide intermediate and developed protocols can be widely applicable to access various GPI analogues with the βGlcN(1,6)Ins motif. The target GPI analogues contain an alkyne, which allows their further modification to introduce various molecular labels via click chemistry, making them useful probes for the study of GPI anchorage. The differences in reactivity and NMR behavior of the two GPI analogues, as well as the differences of these analogues from previously reported GPI derivatives of similar structure containing an αGlcN(1,6)Ins motif, suggest that the 2-O-phosphoethanolamine moiety on mannose-I and the linkage form of GlcN in GPIs can have a decisive impact on the structure, which is likely relevant to biology. [ABSTRACT FROM AUTHOR]

Published

2024

25. 血清 GPAA1, SF, OPN 与儿童急性淋巴细胞白血病危险度的关系 及对血栓发生风险的评估效能研究.

Author

刘 静, 刘翠云, 马金海, 卫雪利, and 汤长超

Subjects

*LYMPHOBLASTIC leukemia, *ACUTE leukemia, *GLYCOSYLPHOSPHATIDYLINOSITOL, *OSTEOPONTIN, *FERRITIN

Abstract

Objective: To analyze the relationship between serum glycosylphosphatidylinositol anchor attachment protein 1 (GPAA1), ferritin (SF), osteopontin (OPN) and the risk of acute lymphoblastic leukemia in children and evaluate the risk of thrombosis.Methods: 112 children with acute lymphoblastic leukemia admitted to our hospital from January 2017 to December 2022 were selected as the observation group, and 112 healthy children matching the gender and age of the observation group were selected as the control group.The expression levels of serum GPAA1, SF and OPN in the two groups were detected, the differences in the expression levels of serum GPAA1, SF and OPN in children with acute lymphoblastic leukemia with different risk levels were analyzed, and the occurrence of thrombosis in children with acute lymphoblastic leukemia was observed.The area under receiver operating characteristic curve (ROC) (AUC) was used to evaluate the efficacy of serum GPAA1, SF and OPN in predicting thrombus occurrence in children with acute lymphoblastic leukemia. Results: The expression levels of serum GPAA1, SF and OPN in observation group were higher than those in control group (P＜0.05) . The expression levels of serum GPAA1,SF and OPN in children with low-risk,medium-risk and high-risk acute lymphoblastic leukemia were significant (P＜0.05) . The expression levels of serum GPAA1, SF and OPN were positively correlated with the risk of childhood acute lymphoblastic leukemia by Spearman correlation analysis (P＜0.05) . Among 112 children with acute lymphoblastic leukemia, thrombosis occurred in 12 cases (10.71%) . Multivariate Logistic regression analysis showed that serum GPAA1,SF and OPN were independent predictors of thrombosis in children with acute lymphoblastic leukemia (P＜0.05) . According to ROC curve analysis, the AUC of serum GPAA1 and SF combined with OPN to predict thrombus occurrence in children with acute lymphoblastic leukemia was 0.901. Conclusion: Serum GPAA1, SF and OPN are closely related to the risk of acute lymphoblastic leukemia in children, and the combination of GPAA1, SF and OPN is effective in predicting thrombus occurrence in children, which has important guiding significance in the diagnosis and treatment of this disease. [ABSTRACT FROM AUTHOR]

Published

2023

26. 罕见病研究：GPAA1 基因突变导致糖基 磷脂酰肌醇生物合成缺陷15型.

Author

陈秋蓉, 张朕杰, 卢一岫, 袁孙碧歆, and 李冀

Subjects

GLYCOSYLPHOSPHATIDYLINOSITOL, BIOSYNTHESIS, EPILEPSY, FEVER, GENES

Abstract

Copyright of Chinese Journal of Contemporary Pediatrics is the property of Xiangya Medical Periodical Press and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2023

27. GPI‐anchoring disorders and the heart: Is cardiomyopathy an overlooked feature?

Author

Bayat, Allan, Lindau, Tobias, Aledo‐Serrano, Angel, Gil‐Nagel, Antonio, Barić, Ivo, Bartoniček, Dorotea, Mateševac, Josipa, Ramadža, Danijela Petković, Žigman, Tamara, Pušeljić, Silvija, Dorner, Sanja, Bupp, Caleb, Devries, Seth, and Møller, Rikke Steensbjerre

Subjects

*HEART, *CARDIOMYOPATHIES, *CONSCIOUSNESS raising, *CONGENITAL disorders, *EARLY death, *GLYCOSYLPHOSPHATIDYLINOSITOL

Abstract

Glycosylphosphatidylinositol anchoring disorders (GPI‐ADs) are a subgroup of congenital disorders of glycosylation. GPI biosynthesis requires proteins encoded by over 30 genes of which 24 genes are linked to neurodevelopmental disorders. Patients, especially those with PIGA‐encephalopathy, have a high risk of premature mortality which sometimes is attributed to cardiomyopathy. We aimed to explore the occurrence of cardiomyopathy among patients with GPI‐ADs and to raise awareness about this potentially lethal feature. Unpublished patients with genetically proven GPI‐ADs and cardiomyopathy were identified through an international collaboration and recruited through the respective clinicians. We also reviewed the literature for published patients with cardiomyopathy and GPI‐AD and contacted the corresponding authors for additional information. We identified four novel and unrelated patients with GPI‐AD and cardiomyopathy. Cardiomyopathy was diagnosed before adulthood and was the cause of early demise in two patients. Only one patients underwent cardiac workup after being diagnosed with a GPI‐AD. All were diagnosed with PIGA‐encephalopathy and three had a disease‐causing variant at the same residue. The literature reports five additional children with GPI‐AD related cardiomyopathy, three of which died before adulthood. We have shown that patients with GPI‐ADs are at risk of developing cardiomyopathy and that regular cardiac workup with echocardiography is necessary. [ABSTRACT FROM AUTHOR]

Published

2023

28. The PIG‐A gene mutation assay in human biomonitoring and disease.

Author

Lawrence, Rachel, Munn, Kathryn, Naser, Hamsa, Thomas, Laura, Haboubi, Hasan, Williams, Lisa, Doak, Shareen, and Jenkins, Gareth

Subjects

GENETIC mutation, GLYCOSYLPHOSPHATIDYLINOSITOL, BIOLOGICAL monitoring, SOMATIC mutation, MUTAGENICITY testing, ERYTHROCYTE deformability

Abstract

The blood cell phosphatidylinositol glycan class A (PIG‐A) gene mutation assay has been extensively researched in rodents for in vivo mutagenicity testing and is now being investigated in humans. The PIG‐A gene is involved in glycosyl phosphatidylinositol (GPI)‐anchor biosynthesis. A single mutation in this X‐linked gene can lead to loss of membrane‐bound GPI anchors, which can be enumerated via corresponding GPI‐anchored proteins (e.g., CD55) using flow cytometry. The studies published to date by different research groups demonstrate a remarkable consistency in PIG‐A mutant frequencies. Moreover, with the low background level of mutant erythrocytes in healthy subjects (2.9–5.56 × 10−6 mutants), induction of mutation post genotoxic exposure can be detected. Cigarette smoking, radiotherapy, and occupational exposures, including lead, have been shown to increase mutant levels. Future applications of this test include identifying new harmful agents and establishing new exposure limits. This mutational monitoring approach may also identify individuals at higher risk of cancer development. In addition, identifying protective agents that could mitigate these effects may reduce baseline somatic mutation levels and such behaviors can be encouraged. Further technological progress is required including establishing underlying mechanisms of GPI anchor loss, protocol standardization, and the development of cryopreservation methods to improve GPI‐anchor stability over time. If successful, this assay has the potential be widely employed, for example, in rural and low‐income countries. Here, we review the current literature on PIG‐A mutation in humans and discuss the potential role of this assay in human biomonitoring and disease detection. [ABSTRACT FROM AUTHOR]

Published

2023

29. Structures of liganded glycosylphosphatidylinositol transamidase illuminate GPI-AP biogenesis.

Author

Xu, Yidan, Li, Tingting, Zhou, Zixuan, Hong, Jingjing, Chao, Yulin, Zhu, Zhini, Zhang, Ying, Qu, Qianhui, and Li, Dianfan

Subjects

GLYCOSYLPHOSPHATIDYLINOSITOL, TRANSMEMBRANE domains, PEPTIDES, PROTEINS, AMIDASES, ENZYMES

Abstract

Many eukaryotic receptors and enzymes rely on glycosylphosphatidylinositol (GPI) anchors for membrane localization and function. The transmembrane complex GPI-T recognizes diverse proproteins at a signal peptide region that lacks consensus sequence and replaces it with GPI via a transamidation reaction. How GPI-T maintains broad specificity while preventing unintentional cleavage is unclear. Here, substrates- and products-bound human GPI-T structures identify subsite features that enable broad proprotein specificity, inform catalytic mechanism, and reveal a multilevel safeguard mechanism against its promiscuity. In the absence of proproteins, the catalytic site is invaded by a locally stabilized loop. Activation requires energetically unfavorable rearrangements that transform the autoinhibitory loop into crucial catalytic cleft elements. Enzyme-proprotein binding in the transmembrane and luminal domains respectively powers the conformational rearrangement and induces a competent cleft. GPI-T thus integrates various weak specificity regions to form strong selectivity and prevent accidental activation. These findings provide important mechanistic insights into GPI-anchored protein biogenesis. GPI-T adds GPI to proteins faithfully despite the sequence variance. Here, the authors reveal structural features underpinning this broad specificity, and a fidelity mechanism where unlocking autoinhibition necessitates the synergistic binding of substrate regions with individually weak specificity. [ABSTRACT FROM AUTHOR]

Published

2023

30. Phospholipid cofactor solubilization inhibits formation of native prions.

Author

Schwind, Abigail M., Walsh, Daniel J., Burke, Cassandra M., and Supattapone, Surachai

Subjects

*PRIONS, *SOLUBILIZATION, *TRITON X-100, *POST-translational modification, *GLYCOSYLPHOSPHATIDYLINOSITOL, *BRAIN banks

Abstract

Cofactor molecules are required to generate infectious mammalian prions in vitro. Mouse and hamster prions appear to have different cofactor preferences: Whereas both mouse and hamster prions can use phosphatidylethanolamine (PE) as a prion cofactor, only hamster prions can also use single‐stranded RNA as an alternative cofactor. Here, we investigated the effect of detergent solubilization on rodent prion formation in vitro. We discovered that detergents that can solubilize PE (n‐octylglucoside, n‐octylgalactoside, and CHAPS) inhibit mouse prion formation in serial protein misfolding cyclic amplification (sPMCA) reactions using bank vole brain homogenate substrate, whereas detergents that are unable to solubilize PE (Triton X‐100 and IPEGAL) have no effect. For all three PE‐solubilizing detergents, inhibition of RML mouse prion formation was only observed above the critical micellar concentration (CMC). Two other mouse prion strains, Me7 and 301C, were also inhibited by the three PE‐solubilizing detergents but not by Triton X‐100 or IPEGAL. In contrast, none of the detergents inhibited hamster prion formation in parallel sPMCA reactions using the same bank vole brain homogenate substrate. In reconstituted sPMCA reactions using purified substrates, n‐octylglucoside inhibited hamster prion formation when immunopurified bank vole PrPC substrate was supplemented with brain phospholipid but not with RNA. Interestingly, phospholipid cofactor solubilization had no effect in sPMCA reactions using bacterially expressed recombinant PrP substrate, indicating that the inhibitory effect of solubilization requires PrPC post‐translational modifications. Overall, these in vitro results show that the ability of PE to facilitate the formation of native but not recombinant prions requires phospholipid bilayer integrity, suggesting that membrane structure may play an important role in prion formation in vivo. [ABSTRACT FROM AUTHOR]

Published

2023

31. A lipid scramblase TMEM41B is involved in the processing and transport of GPI-anchored proteins.

Author

Cao, Shu-Ya, Liu, Yi-Shi, Gao, Xiao-Dong, Kinoshita, Taroh, and Fujita, Morihisa

Subjects

*CARRIER proteins, *MEMBRANE proteins, *PROTEIN transport, *PHOSPHOLIPASE C, *LIPIDS, *SELENOPROTEINS

Abstract

Protein modification by glycosylphosphatidylinositol (GPI) takes place in the endoplasmic reticulum (ER). GPI-anchored proteins (GPI-APs) formed in the ER are transported to the cell surface through the Golgi apparatus. During transport, the GPI-anchor structure is processed. In most cells, an acyl chain modified to the inositol of GPI is removed by a GPI-inositol deacylase, PGAP1, in the ER. Inositol-deacylated GPI-APs become sensitive to bacterial phosphatidylinositol-specific phospholipase C (PI-PLC). We previously reported that GPI-APs are partially resistant to PI-PLC when PGAP1 activity is weakened by the deletion of selenoprotein T (SELT) or cleft lip and palate transmembrane protein 1 (CLPTM1). In this study, we found that the loss of TMEM41B, an ER-localized lipid scramblase, restored PI-PLC sensitivity of GPI-APs in SELT-knockout (KO) and CLPTM1-KO cells. In TMEM41B-KO cells, the transport of GPI-APs as well as transmembrane proteins from the ER to the Golgi was delayed. Furthermore, the turnover of PGAP1, which is mediated by ER-associated degradation, was slowed in TMEM41B-KO cells. Taken together, these findings indicate that inhibition of TMEM41B-dependent lipid scrambling promotes GPI-AP processing in the ER through PGAP1 stabilization and slowed protein trafficking. [ABSTRACT FROM AUTHOR]

Published

2023

32. Identification of the glycosylphosphatidylinositol-specific phospholipase A2 (GPI-PLA2) that mediates GPI fatty acid remodeling in Trypanosoma brucei.

Author

Zhe Ji, Nagar, Rupa, Duncan, Samuel M., Sampaio Guther, Maria Lucia, and Ferguson, Michael A. J.

Subjects

*PHOSPHOLIPASE A2, *TRYPANOSOMA brucei, *FATTY acids, *PROTEIN precursors, *GLYCOSYLPHOSPHATIDYLINOSITOL, *PHOSPHOLIPASES, *AMIDASES

Abstract

The biosynthesis of glycosylphosphatidylinositol (GPI)anchored proteins (GPI-APs) in the parasitic protozoan Trypanosoma brucei involves fatty acid remodeling of the GPI precursor molecules before they are transferred to protein in the endoplasmic reticulum. The genes encoding the requisite phospholipase A2 and A1 activities for this remodeling have thus far been elusive. Here, we identify a gene, Tb927.7.6110, that encodes a protein that is both necessary and sufficient for GPI-phospholipase A2 (GPI-PLA2) activity in the procyclic form of the parasite. The predicted protein product belongs to the alkaline ceramidase, PAQR receptor, Per1, SID-1, and TMEM8 (CREST) superfamily of transmembrane hydrolase proteins and shows sequence similarity to Post-GPIAttachment to Protein 6 (PGAP6), a GPI-PLA2 that acts after transfer of GPI precursors to protein in mammalian cells. We show the trypanosome Tb927.7.6110 GPI-PLA2 gene resides in a locus with two closely related genes Tb927.7.6150 and Tb927.7.6170, one of which (Tb927.7.6150) most likely encodes a catalytically inactive protein. The absence of GPI-PLA2 in the null mutant procyclic cells not only affected fatty acid remodeling but also reduced GPI anchor sidechain size on mature GPI-anchored procyclin glycoproteins. This reduction in GPI anchor sidechain size was reversed upon the re-addition of Tb927.7.6110 and of Tb927.7.6170, despite the latter not encoding GPI precursor GPI-PLA2 activity. Taken together, we conclude that Tb927.7.6110 encodes the GPI-PLA2 of GPI precursor fatty acid remodeling and that more work is required to assess the roles and essentiality of Tb927.7.6170 and the presumably enzymatically inactive Tb927.7.6150. [ABSTRACT FROM AUTHOR]

Published

2023

33. Persistent ER stress causes GPI anchor deficit to convert a GPI-anchored prion protein into pro-PrP via the ATF6–miR449c-5p–PIGV axis.

Author

JingFeng Li, SaSa Li, ShuPei Yu, Jie Yang, JingRu Ke, Huan Li, Heng Chen, MingJian Lu, Man-Sun Sy, ZhenXing Gao, and Chaoyang Li

Subjects

*GLYCOSYLPHOSPHATIDYLINOSITOL, *UNFOLDED protein response, *CANCER cell migration, *HEAT shock proteins, *T helper cells, *PRIONS, *SCRAPIE

Abstract

Endoplasmic reticulum (ER) stress and unfolded protein response are cells’ survival strategies to thwart disruption of proteostasis. Tumor cells are continuously being challenged by ER stress. The prion protein, PrP, normally a glycosylphosphatidylinositol (GPI)-anchored protein exists as a proPrP retaining its GPI-peptide signal sequence in human pancreatic ductal cell adenocarcinoma (PDAC). Higher abundance of pro-PrP indicates poorer prognosis in PDAC patients. The reason why PDAC cells express pro-PrP is unknown. Here, we report that persistent ER stress causes conversion of GPIanchored PrP to pro-PrP via a conserved ATF6–miRNA449c5p–PIGV axis. Mouse neurons and AsPC-1, a PDAC cell line, express GPI-anchored PrP. However, continuous culture of these cells with the ER stress inducers thapsigargin or brefeldin A results in the conversion of a GPI-anchored PrP to pro-PrP. Such a conversion is reversible; removal of the inducers allows the cells to re-express a GPI-anchored PrP. Mechanistically, persistent ER stress increases the abundance of an active ATF6, which increases the level of miRNA449c-5p (miR449c-5p). By binding the mRNA of PIGV at its 30 -UTRs, miR449c-5p suppresses the level of PIGV, a mannosyltransferase pivotal in the synthesis of the GPI anchor. Reduction of PIGV leads to disruption of the GPI anchor assembly, causing pro-PrP accumulation and enhancing cancer cell migration and invasion. The importance of ATF6–miR449c-5p–PIGV axis is recapitulated in PDAC biopsies as the higher levels of ATF6 and miR449c-5p and lower levels of PIGV are markers of poorer outcome for patients with PDAC. Drugs targeting this axis may prevent PDAC progression [ABSTRACT FROM AUTHOR]

Published

2023

34. A Novel Homozygous GPAA1 Variant in a Patient with a Glycosylphosphatidylinositol Biosynthesis Defect.

Author

Fontana, Paolo, Budillon, Alberto, Simeone, Domenico, Del Vecchio Blanco, Francesca, Caiazza, Martina, D'Amico, Alessandra, Lonardo, Fortunato, Nigro, Vincenzo, Limongelli, Giuseppe, and Scarano, Gioacchino

Subjects

*GLYCOSYLPHOSPHATIDYLINOSITOL, *BIOSYNTHESIS, *MAGNETIC resonance imaging, *GENETIC variation, *DEVELOPMENTAL delay, *INTELLECTUAL disabilities

Abstract

Glycosylphosphatidylinositol biosynthesis defect 15 is a rare autosomal recessive disorder due to biallelic loss of function of GPAA1. At the moment, less than twenty patients have been reported, usually compound heterozygous for GPAA1 variants. The main clinical features are intellectual disability, hypotonia, seizures, and cerebellar atrophy. We describe a 4-year-old male with a novel, homozygous variant. The patient presents with typical features, such as developmental delay, hypotonia, seizures, and atypical features, such as macrocephaly, preauricular, and cheek appendages. When he was 15 months, the cerebellum was normal. When he was 33 months old, after the molecular diagnosis, magnetic resonance imaging was repeated, showing cerebellar atrophy. This case extends the clinical spectrum of the GPAA1-related disorder and helps to delineate phenotypic differences with defects of other subunits of the transamidase complex. [ABSTRACT FROM AUTHOR]

Published

2023

35. The biological roles of CD24 in ovarian cancer: old story, but new tales.

Author

Yuanyuan Gu, Guannan Zhou, Xue Tang, Fang Shen, Jingxin Ding, and Keqin Hua

Subjects

OVARIAN cancer, CANCER cells, GLYCOSYLPHOSPHATIDYLINOSITOL, STEM cells, CELLULAR signal transduction, CANCER treatment

Abstract

CD24 is a glycosylphosphatidylinositol linked molecular which expressed in diverse malignant tumor cells, particular in ovarian carcinoma cells and ovarian carcinoma stem cells. The CD24 expression is associated with increased metastatic potential and poor prognosis of malignancies. CD24 on the surface of tumor cells could interact with Siglec-10 on the surface of immune cells, to mediate the immune escape of tumor cells. Nowadays, CD24 has been identified as a promising focus for targeting therapy of ovarian cancer. However, the roles of CD24 in tumorigenesis, metastasis, and immune escape are still not clearly demonstrated systematically. In this review, we i) summarized the existing studies on CD24 in diverse cancers including ovarian cancer, ii) illustrated the role of CD24-siglec10 signaling pathway in immune escape, iii) reviewed the existing immunotherapeutic strategies (targeting the CD24 to restore the phagocytic effect of Siglec-10 expressing immune cells) based on the above mechanisms and evaluated the priorities in the future research. These results might provide support for guiding the CD24 immunotherapy as the intervention upon solid tumors. [ABSTRACT FROM AUTHOR]

Published

2023

36. (Patho)Physiology of Glycosylphosphatidylinositol-Anchored Proteins II: Intercellular Transfer of Matter (Inheritance?) That Matters.

Author

Müller, Günter A. and Müller, Timo D.

Subjects

*PHYSIOLOGY, *GLYCOSYLPHOSPHATIDYLINOSITOL, *BLOOD proteins, *PLURIPOTENT stem cells, *SOMATIC cells, *INSULIN, *CELL communication, *ADIPOGENESIS

Abstract

Glycosylphosphatidylinositol (GPI)-anchored proteins (APs) are anchored at the outer leaflet of the plasma membrane (PM) bilayer by covalent linkage to a typical glycolipid and expressed in all eukaryotic organisms so far studied. Lipolytic release from PMs into extracellular compartments and intercellular transfer are regarded as the main (patho)physiological roles exerted by GPI-APs. The intercellular transfer of GPI-APs relies on the complete GPI anchor and is mediated by extracellular vesicles such as microvesicles and exosomes and lipid-free homo- or heteromeric aggregates, and lipoprotein-like particles such as prostasomes and surfactant-like particles, or lipid-containing micelle-like complexes. In mammalian organisms, non-vesicular transfer is controlled by the distance between donor and acceptor cells/tissues; intrinsic conditions such as age, metabolic state, and stress; extrinsic factors such as GPI-binding proteins; hormones such as insulin; and drugs such as anti-diabetic sulfonylureas. It proceeds either "directly" upon close neighborhood or contact of donor and acceptor cells or "indirectly" as a consequence of the induced lipolytic release of GPI-APs from PMs. Those displace from the serum GPI-binding proteins GPI-APs, which have retained the complete anchor, and become assembled in aggregates or micelle-like complexes. Importantly, intercellular transfer of GPI-APs has been shown to induce specific phenotypes such as stimulation of lipid and glycogen synthesis, in cultured human adipocytes, blood cells, and induced pluripotent stem cells. As a consequence, intercellular transfer of GPI-APs should be regarded as non-genetic inheritance of (acquired) features between somatic cells which is based on the biogenesis and transmission of matter such as GPI-APs and "membrane landscapes", rather than the replication and transmission of information such as DNA. Its operation in mammalian organisms remains to be clarified. [ABSTRACT FROM AUTHOR]

Published

2023

37. Intersection of Coagulation and Fibrinolysis by the Glycosylphosphatidylinositol (GPI)-Anchored Serine Protease Testisin.

Author

Buzza, Marguerite S., Pawar, Nisha R., Strong, Amando A., and Antalis, Toni M.

Subjects

*FIBRINOLYSIS, *GLYCOSYLPHOSPHATIDYLINOSITOL, *PLASMINOGEN, *PLASMINOGEN activators, *PLASMIN, *SERINE, *BLOOD coagulation

Abstract

Hemostasis is a delicate balance between coagulation and fibrinolysis that regulates the formation and removal of fibrin, respectively. Positive and negative feedback loops and crosstalk between coagulation and fibrinolytic serine proteases maintain the hemostatic balance to prevent both excessive bleeding and thrombosis. Here, we identify a novel role for the glycosylphosphatidylinositol (GPI)-anchored serine protease testisin in the regulation of pericellular hemostasis. Using in vitro cell-based fibrin generation assays, we found that the expression of catalytically active testisin on the cell surface accelerates thrombin-dependent fibrin polymerization, and intriguingly, that it subsequently promotes accelerated fibrinolysis. We find that the testisin-dependent fibrin formation is inhibited by rivaroxaban, a specific inhibitor of the central prothrombin-activating serine protease factor Xa (FXa), demonstrating that cell-surface testisin acts upstream of factor X (FX) to promote fibrin formation at the cell surface. Unexpectedly, testisin was also found to accelerate fibrinolysis by stimulating the plasmin-dependent degradation of fibrin and enhancing plasmin-dependent cell invasion through polymerized fibrin. Testisin was not a direct activator of plasminogen, but it is able to induce zymogen cleavage and the activation of pro-urokinase plasminogen activator (pro-uPA), which converts plasminogen to plasmin. These data identify a new proteolytic component that can regulate pericellular hemostatic cascades at the cell surface, which has implications for angiogenesis, cancer biology, and male fertility. [ABSTRACT FROM AUTHOR]

Published

2023

38. A point mutation in GPI-attachment signal peptide accelerates the development of prion disease.

Author

Kobayashi, Atsushi, Hirata, Tetsuya, Shimazaki, Taishi, Munesue, Yoshiko, Aoshima, Keisuke, Kimura, Takashi, Nio-Kobayashi, Junko, Hasebe, Rie, Takeuchi, Atsuko, Matsuura, Yuichi, Kusumi, Satoshi, Koga, Daisuke, Iwasaki, Yasushi, Kinoshita, Taroh, Mohri, Shirou, and Kitamoto, Tetsuyuki

Subjects

*PRION diseases, *PEPTIDES, *PRIONS, *CREUTZFELDT-Jakob disease, *MISSENSE mutation, *JAPANESE people

Abstract

A missense variant from methionine to arginine at codon 232 (M232R) of the prion protein gene accounts for ~ 15% of Japanese patients with genetic prion diseases. However, pathogenic roles of the M232R substitution for the induction of prion disease have remained elusive because family history is usually absent in patients with M232R. In addition, the clinicopathologic phenotypes of patients with M232R are indistinguishable from those of sporadic Creutzfeldt-Jakob disease patients. Furthermore, the M232R substitution is located in the glycosylphosphatidylinositol (GPI)-attachment signal peptide that is cleaved off during the maturation of prion proteins. Therefore, there has been an argument that the M232R substitution might be an uncommon polymorphism rather than a pathogenic mutation. To unveil the role of the M232R substitution in the GPI-attachment signal peptide of prion protein in the pathogenesis of prion disease, here we generated a mouse model expressing human prion proteins with M232R and investigated the susceptibility to prion disease. The M232R substitution accelerates the development of prion disease in a prion strain-dependent manner, without affecting prion strain-specific histopathologic and biochemical features. The M232R substitution did not alter the attachment of GPI nor GPI-attachment site. Instead, the substitution altered endoplasmic reticulum translocation pathway of prion proteins by reducing the hydrophobicity of the GPI-attachment signal peptide, resulting in the reduction of N-linked glycosylation and GPI glycosylation of prion proteins. To the best of our knowledge, this is the first time to show a direct relationship between a point mutation in the GPI-attachment signal peptide and the development of disease. [ABSTRACT FROM AUTHOR]

Published

2023

39. (Patho)Physiology of Glycosylphosphatidylinositol-Anchored Proteins I: Localization at Plasma Membranes and Extracellular Compartments.

Author

Müller, Günter A. and Müller, Timo D.

Subjects

*CELL membranes, *GLYCOSYLPHOSPHATIDYLINOSITOL, *PHOSPHOLIPASE D, *TRANSMEMBRANE domains, *LIVER cells, *PHOSPHOLIPASES

Abstract

Glycosylphosphatidylinositol (GPI)-anchored proteins (APs) are anchored at the outer leaflet of plasma membranes (PMs) of all eukaryotic organisms studied so far by covalent linkage to a highly conserved glycolipid rather than a transmembrane domain. Since their first description, experimental data have been accumulating for the capability of GPI-APs to be released from PMs into the surrounding milieu. It became evident that this release results in distinct arrangements of GPI-APs which are compatible with the aqueous milieu upon loss of their GPI anchor by (proteolytic or lipolytic) cleavage or in the course of shielding of the full-length GPI anchor by incorporation into extracellular vesicles, lipoprotein-like particles and (lyso)phospholipid- and cholesterol-harboring micelle-like complexes or by association with GPI-binding proteins or/and other full-length GPI-APs. In mammalian organisms, the (patho)physiological roles of the released GPI-APs in the extracellular environment, such as blood and tissue cells, depend on the molecular mechanisms of their release as well as the cell types and tissues involved, and are controlled by their removal from circulation. This is accomplished by endocytic uptake by liver cells and/or degradation by GPI-specific phospholipase D in order to bypass potential unwanted effects of the released GPI-APs or their transfer from the releasing donor to acceptor cells (which will be reviewed in a forthcoming manuscript). [ABSTRACT FROM AUTHOR]

Published

2023

40. Genome-Wide Analysis and Abiotic Stress-Responsive Patterns of COBRA-like Gene Family in Liriodendron chinense.

Author

Qiu, Chen, Chen, Jinhui, Wu, Weihuang, Liao, Bojun, Zheng, Xueyan, Li, Yong, Huang, Jing, Shi, Jisen, and Hao, Zhaodong

Subjects

LIRIODENDRON chinense, GENE families, GENE expression, ABIOTIC stress, GLYCOSYLPHOSPHATIDYLINOSITOL, PHYSIOLOGICAL effects of cold temperatures

Abstract

The COBRA gene encodes a plant-specific glycosylphosphatidylinositol (GPI)-anchored protein (GAP), which plays an important role in cell wall cellulose deposition. In this study, a total of 7 COBRA-like (COBL) genes were identified in the genome of the rare and endangered woody plant Liriodendron chinense (L. chinense). Phylogenetic analysis showed that these LcCOBL genes can be divided into two subfamilies, i.e., SF I and II. In the conserved motif analysis of two subfamilies, SF I contained 10 predicted motifs, while SF II contained 4–6 motifs. The tissue-specific expression patterns showed that LcCOBL5 was highly expressed in the phloem and xylem, indicating its potential role in cellulose biosynthesis. In addition, the cis-element analysis and abiotic stress transcriptomes showed that three LcCOBLs, LcCOBL3, LcCOBL4 and LcCOBL5, transcriptionally responded to abiotic stresses, including cold, drought and heat stress. In particular, the quantitative reverse-transcription PCR (qRT-PCR) analysis further confirmed that the LcCOBL3 gene was significantly upregulated in response to cold stress and peaked at 24–48 h, hinting at its potential role in the mechanism of cold resistance in L. chinense. Moreover, GFP-fused LcCOBL2, LcCOBL4 and LcCOBL5 were found to be localized in the cytomembrane. In summary, we expect these results to be beneficial for research on both the functions of LcCOBL genes and resistance breeding in L. chinense. [ABSTRACT FROM AUTHOR]

Published

2023

41. Designer molecules of the synaptic organizer MDGA1 reveal 3D conformational control of biological function.

Author

Lee, Hubert, Chofflet, Nicolas, Jianfang Liu, Shanghua Fan, Zhuoyang Lu, Rojas, Martin Resua, Penndorf, Patrick, Bailey, Aaron O., Russell, William K., Machius, Mischa, Gang Ren, Hideto Takahashi, and Rudenko, Gabby

Subjects

*MOLECULES, *ELBOW, *NEUREXINS, *GLYCOSYLPHOSPHATIDYLINOSITOL, *DESIGNERS, *FIBRONECTINS

Abstract

MDGAs (MAM domain-containing glycosylphosphatidylinositol anchors) are synaptic cell surface molecules that regulate the formation of trans-synaptic bridges between neurexins (NRXNs) and neuroligins (NLGNs), which promote synaptic development. Mutations in MDGAs are implicated in various neuropsychiatric diseases. MDGAs bind NLGNs in cis on the postsynaptic membrane and physically block NLGNs from binding to NRXNs. In crystal structures, the six immunoglobulin (Ig) and single fibronectin III domains of MDGA1 reveal a striking compact, triangular shape, both alone and in complex with NLGNs. Whether this unusual domain arrangement is required for biological function or other arrangements occur with different functional outcomes is unknown. Here, we show that WT MDGA1 can adopt both compact and extended 3D conformations that bind NLGN2. Designer mutants targeting strategic molecular elbows in MDGA1 alter the distribution of 3D conformations while leaving the binding affinity between soluble ectodomains of MDGA1 and NLGN2 intact. In contrast, in a cellular context, these mutants result in unique combinations of functional consequences, including altered binding to NLGN2, decreased capacity to conceal NLGN2 from NRXN1ß, and/or suppressed NLGN2-mediated inhibitory presynaptic differentiation, despite the mutations being located far from the MDGA1-NLGN2 interaction site. Thus, the 3D conformation of the entire MDGA1 ectodomain appears critical for its function, and its NLGN-binding site on Ig1-Ig2 is not independent of the rest of the molecule. As a result, global 3D conformational changes to the MDGA1 ectodomain via strategic elbows may form a molecular mechanism to regulate MDGA1 action within the synaptic cleft. [ABSTRACT FROM AUTHOR]

Published

2023

42. Synthesis of a Bifunctionalized Glycosylphosphatidylinositol (GPI) Anchor Useful for the Study of GPI Biology.

Author

Mullapudi, Venkanna Babu, Craig, Kendall C., and Guo, Zhongwu

Subjects

*GLYCOSYLPHOSPHATIDYLINOSITOL, *GLYCANS, *MEMBRANE proteins, *PHOTOACTIVATION, *DIAZOMETHANE, *FUNCTIONAL groups

Abstract

A new, bifunctional glycosylphosphatidylinositol (GPI) derivative containing the highly conserved core structure of all natural GPI anchors with a photoactivable diazirine in the lipid chain and clickable alkynes in the glycan was synthesized by a convergent [3+2] glycosylation strategy with late stage protecting group manipulation and regioselective phosphorylation. The challenges of this synthesis were due to the presence of several distinctive functional groups in the synthetic target, which complicated the protection tactics, in addition to the inherent difficulties associated with GPI synthesis. This bifunctional GPI derivative can cross‐react with molecules in proximity upon photoactivation and be subsequently labeled with other molecular tags via click reaction. Therefore, it should be a valuable probe for biological studies of GPIs, such as analysis of GPI‐interacting membrane proteins, and gaining insights into their functional mechanisms. [ABSTRACT FROM AUTHOR]

Published

2023

43. Labeling cell surface glycosylphosphatidylinositol-anchored proteins through metabolic engineering using an azide-modified phosphatidylinositol.

Author

Kundu, Sayan, Jaiswal, Mohit, Craig, Kendall C., Guo, Jiatong, and Guo, Zhongwu

Subjects

*CELL membranes, *FLUORESCENT proteins, *AZIDO group, *BLOOD proteins, *PROTEINS

Abstract

Glycosylphosphatidylinositol (GPI) anchorage is one of the most common mechanisms to attach proteins to the plasma membrane of eukaryotic cells. GPI-anchored proteins (GPI-APs) play a critical role in many biological processes but are difficult to study. Here, a new method was developed for the effective and selective metabolic engineering and labeling of cell surface GPI-APs with an azide-modified phosphatidylinositol (PI) as the biosynthetic precursor of GPIs. It was demonstrated that this azido-PI derivative was taken up by HeLa cells and incorporated into the biosynthetic pathway of GPIs to present azide-labeled GPI-APs on the live cell surface. The azido group was used as a molecular handle to install other labels through a biocompatible click reaction to enable various biological studies, e.g., fluorescent imaging and protein pull-down, which can help explore the functions of GPI-APs and discover new GPI-APs. [Display omitted] • A new method for metabolic engineering of GPI-anchored proteins (GPI-APs). • Labeling GPI-APs on live cells with an azide to enable further functionalization. • Labeling GPI-APs on cells with fluorophores to enable fluorescence-based studies. • Labeling GPI-APs on cells with an affinity tag to facilitate proteomics analysis. [ABSTRACT FROM AUTHOR]

Published

2023

44. Role and mechanism of CD90+ fibroblasts in inflammatory diseases and malignant tumors.

Author

Zeng, Feng, Gao, Mengxiang, Liao, Shan, Zhou, Zihua, Luo, Gengqiu, and Zhou, Yanhong

Subjects

*HYPERTROPHIC scars, *FIBROBLASTS, *INFLAMMATION, *PULMONARY fibrosis, *TUMOR markers, *MYOFIBROBLASTS, *STROMAL cells, *GLYCOSYLPHOSPHATIDYLINOSITOL

Abstract

Fibroblasts are highly heterogeneous mesenchymal stromal cells, and different fibroblast subpopulations play different roles. A subpopulation of fibroblasts expressing CD90, a 25–37 kDa glycosylphosphatidylinositol anchored protein, plays a dominant role in the fibrotic and pro-inflammatory state. In this review, we focused on CD90+ fibroblasts, and their roles and possible mechanisms in disease processes. First, the main biological functions of CD90+ fibroblasts in inducing angiogenesis and maintaining tissue homeostasis are described. Second, the role and possible mechanism of CD90+ fibroblasts in inducing pulmonary fibrosis, inflammatory arthritis, inflammatory skin diseases, and scar formation are introduced, and we discuss how CD90+ cancer-associated fibroblasts might serve as promising cancer biomarkers. Finally, we propose future research directions related to CD90+ fibroblasts. This review will provide a theoretical basis for the diagnosis and treatment CD90+ fibroblast-related disease. [ABSTRACT FROM AUTHOR]

Published

2023

45. FT-GPI, a highly sensitive and accurate predictor of GPI-anchored proteins, reveals the composition and evolution of the GPI proteome in Plasmodium species.

Author

Sauer, Lena M., Canovas, Rodrigo, Roche, Daniel, Shams-Eldin, Hosam, Ravel, Patrice, Colinge, Jacques, Schwarz, Ralph T., Ben Mamoun, Choukri, Rivals, Eric, and Cornillot, Emmanuel

Subjects

*GLYCOSYLPHOSPHATIDYLINOSITOL, *CHROMOSOME duplication, *PLASMODIUM, *BLOOD proteins, *PEPTIDES, *MALARIA vaccines, *TRYPANOSOMA

Abstract

Background: Protozoan parasites are known to attach specific and diverse group of proteins to their plasma membrane via a GPI anchor. In malaria parasites, GPI-anchored proteins (GPI-APs) have been shown to play an important role in host–pathogen interactions and a key function in host cell invasion and immune evasion. Because of their immunogenic properties, some of these proteins have been considered as malaria vaccine candidates. However, identification of all possible GPI-APs encoded by these parasites remains challenging due to their sequence diversity and limitations of the tools used for their characterization. Methods: The FT-GPI software was developed to detect GPI-APs based on the presence of a hydrophobic helix at both ends of the premature peptide. FT-GPI was implemented in C ++and applied to study the GPI-proteome of 46 isolates of the order Haemosporida. Using the GPI proteome of Plasmodium falciparum strain 3D7 and Plasmodium vivax strain Sal-1, a heuristic method was defined to select the most sensitive and specific FT-GPI software parameters. Results: FT-GPI enabled revision of the GPI-proteome of P. falciparum and P. vivax, including the identification of novel GPI-APs. Orthology- and synteny-based analyses showed that 19 of the 37 GPI-APs found in the order Haemosporida are conserved among Plasmodium species. Our analyses suggest that gene duplication and deletion events may have contributed significantly to the evolution of the GPI proteome, and its composition correlates with speciation. Conclusion: FT-GPI-based prediction is a useful tool for mining GPI-APs and gaining further insights into their evolution and sequence diversity. This resource may also help identify new protein candidates for the development of vaccines for malaria and other parasitic diseases. [ABSTRACT FROM AUTHOR]

Published

2023

46. Molecular Characterization and Function of the Nogo-66 Receptor (NgR1) Gene in the Chinese Tree Shrew.

Author

Caixia Lu, Xiuying Kui, Xiaofei Li, Wenguang Wang, Xiaomei Sun, Na Li, Pinfen Tong, and Jiejie Dai

Subjects

*GLYCOSYLPHOSPHATIDYLINOSITOL, *NOGO receptors, *REOVIRUSES, *CELL receptors, *NORTHERN tree shrew

Abstract

Background: Nogo-66 receptor (NgR1) is a glycosylphosphatidylinositol-linked cell surface receptor with high affinity for Nogo-66. The binding of Nogo-66 to NgR1 plays a key role in inhibiting neurite growth, limiting synaptic plasticity and mediating Mammalian Reovirus (MRV) infection. The Chinese tree shrew (Tupaia belangeri chinensis) is, a new and valuable experimental animal that is widely used in biomedical research. Although susceptible to MRV, little is known about tree shrew NgR1 and its role in MRV infection. Methods: In this study, we cloned NgR1 form the Chinese tree shrew by RACE technology and analyzed its characteristics, spatial structure and its tissue expression. We also examined the expression pattern of NgR1 in the response of tree shrew primary nerve cells (tNC) to MRV1/TS/2011 infection. Results: Tree shrew NgR1 was found to have a closer relationship to human NgR1 (90.34%) than to mouse NgR1. Similar to the protein structure of human NgR1, the tree shrew NgR1 has the same leucine-rich repeat (LRR) domain structure that is capped by C-terminal and N-terminal cysteine-rich modules. The tree shrew NgR1 mRNAs were predominantly detected in the central nervous system (CNS), and tree shrew NgR1 can mediate infection by MRV1/TS/2011. Conclusions: Taken together, these results help to elucidate the function of NgR1 and provide a basis for using the tree shrew as an animal model for studies of the nervous system and infectious diseases. [ABSTRACT FROM AUTHOR]

Published

2023

47. Glycosylphosphatidylinositol anchor lipid remodeling directs proteins to the plasma membrane and governs cell wall mechanics.

Author

Xu, Zuopeng, Gao, Yihong, Gao, Chengxu, Mei, Jiasong, Wang, Shaogan, Ma, Jiaxin, Yang, Hanlei, Cao, Shaoxue, Wang, Yan, Zhang, Fengxia, Liu, Xiangling, Liu, Qiaoquan, Zhou, Yihua, and Zhang, Baocai

Subjects

*BLOOD proteins, *CELLULAR mechanics, *CELL membranes, *GLYCOSYLPHOSPHATIDYLINOSITOL, *MEMBRANE proteins, *ACYLTRANSFERASES, *CELLULOSE synthase, *MEMBRANE lipids

Abstract

Glycosylphosphatidylinositol (GPI) anchoring is a common protein modification that targets proteins to the plasma membrane (PM). Knowledge about the GPI lipid tail, which guides the secretion of GPI-anchored proteins (GPI-APs), is limited in plants. Here, we report that rice (Oryza sativa) BRITTLE CULM16 (BC16), a membrane-bound O -acyltransferase (MBOAT) remodels GPI lipid tails and governs cell wall biomechanics. The bc16 mutant exhibits fragile internodes, resulting from reduced cell wall thickness and cellulose content. BC16 is the only MBOAT in rice and is located in the endoplasmic reticulum and Golgi apparatus. Yeast gup1 Δ mutant restoring assay and GPI lipid composition analysis demonstrated BC16 as a GPI lipid remodelase. Loss of BC16 alters GPI lipid structure and disturbs the targeting of BC1, a GPI-AP for cellulose biosynthesis, to the PM lipid nanodomains. Atomic force microscopy revealed compromised deposition of cellulosic nanofibers in bc16 , leading to an increased Young's modulus and abnormal mechanical properties. Therefore, BC16-mediated lipid remodeling directs the GPI-APs, such as BC1, to the cell surface to fulfill multiple functions, including cellulose organization. Our work unravels a mechanism by which GPI lipids are remodeled in plants and provides insights into the control of cell wall biomechanics, offering a tool for breeding elite crops with improved support strength. [ABSTRACT FROM AUTHOR]

Published

2022

48. Mutations in PIGS, Encoding a GPI Transamidase, Cause a Neurological Syndrome Ranging from Fetal Akinesia to Epileptic Encephalopathy

Author

Nguyen, Thi Tuyet Mai, Murakami, Yoshiko, Wigby, Kristen M, Baratang, Nissan V, Rousseau, Justine, St-Denis, Anik, Rosenfeld, Jill A, Laniewski, Stephanie C, Jones, Julie, Iglesias, Alejandro D, Jones, Marilyn C, Masser-Frye, Diane, Scheuerle, Angela E, Perry, Denise L, Taft, Ryan J, Le Deist, Françoise, Thompson, Miles, Kinoshita, Taroh, and Campeau, Philippe M

Subjects

Neurodegenerative, Congenital Structural Anomalies, Pediatric, Brain Disorders, Rare Diseases, Genetics, Human Genome, Neurosciences, 2.1 Biological and endogenous factors, Aetiology, Abnormalities, Multiple, Acyltransferases, Arthrogryposis, Cell Line, Cerebellar Ataxia, Child, Child, Preschool, Developmental Disabilities, Epilepsy, Generalized, Female, HEK293 Cells, Humans, Intellectual Disability, Male, Muscle Hypotonia, Mutation, Nervous System Malformations, Pedigree, Seizures, Syndrome, Whole Exome Sequencing, Exome Sequencing, PIGS, epilepsy, glycosylphosphatidylinositol, glycosylphosphatidylinositol biosynthesis defect, inherited GPI deficiency, seizures, Biological Sciences, Medical and Health Sciences, Genetics & Heredity

Abstract

Inherited GPI deficiencies (IGDs) are a subset of congenital disorders of glycosylation that are increasingly recognized as a result of advances in whole-exome sequencing (WES) and whole-genome sequencing (WGS). IGDs cause a series of overlapping phenotypes consisting of seizures, dysmorphic features, multiple congenital malformations, and severe intellectual disability. We present a study of six individuals from three unrelated families in which WES or WGS identified bi-allelic phosphatidylinositol glycan class S (PIGS) biosynthesis mutations. Phenotypes included severe global developmental delay, seizures (partly responding to pyridoxine), hypotonia, weakness, ataxia, and dysmorphic facial features. Two of them had compound-heterozygous variants c.108G>A (p.Trp36∗) and c.101T>C (p.Leu34Pro), and two siblings of another family were homozygous for a deletion and insertion leading to p.Thr439_Lys451delinsArgLeuLeu. The third family had two fetuses with multiple joint contractures consistent with fetal akinesia. They were compound heterozygous for c.923A>G (p.Glu308Gly) and c.468+1G>C, a splicing mutation. Flow-cytometry analyses demonstrated that the individuals with PIGS mutations show a GPI-AP deficiency profile. Expression of the p.Trp36∗ variant in PIGS-deficient HEK293 cells revealed only partial restoration of cell-surface GPI-APs. In terms of both biochemistry and phenotype, loss of function of PIGS shares features with PIGT deficiency and other IGDs. This study contributes to the understanding of the GPI-AP biosynthesis pathway by describing the consequences of PIGS disruption in humans and extending the family of IGDs.

Published

2018

49. importance of side branches of glycosylphosphatidylinositol anchors: a molecular dynamics perspective.

Author

Banerjee, Pallavi, Silva, Daniel Varon, Lipowsky, Reinhard, and Santer, Mark

Subjects

*MOLECULAR dynamics, *GLYCOSYLPHOSPHATIDYLINOSITOL, *GREEN fluorescent protein, *CELLULAR signal transduction, *BILAYER lipid membranes, *GLYCOLIPIDS

Abstract

Many proteins are anchored to the cell surface of eukaryotes using a unique family of glycolipids called glycosylphosphatidylinositol (GPI) anchors. These glycolipids also exist without a covalently bound protein, in particular on the cell surfaces of protozoan parasites where they are densely populated. GPIs and GPI-anchored proteins participate in multiple cellular processes such as signal transduction, cell adhesion, protein trafficking and pathogenesis of Malaria, Toxoplasmosis, Trypanosomiasis and prion diseases, among others. All GPIs share a common conserved glycan core modified in a cell-dependent manner with additional side glycans or phosphoethanolamine residues. Here, we use atomistic molecular dynamic simulations and perform a systematic study to evaluate the structural properties of GPIs with different side chains inserted in lipid bilayers. Our results show a flop-down orientation of GPIs with respect to the membrane surface and the presentation of the side chain residues to the solvent. This finding agrees well with experiments showing the role of the side residues as active epitopes for recognition of GPIs by macrophages and induction of GPI-glycan-specific immune responses. Protein-GPI interactions were investigated by attaching parasitic GPIs to Green Fluorescent Protein. GPIs are observed to recline on the membrane surface and pull down the attached protein close to the membrane facilitating mutual contacts between protein, GPI and the lipid bilayer. This model is efficient in evaluating the interaction of GPIs and GPI-anchored proteins with membranes and can be extended to study other parasitic GPIs and proteins and develop GPI-based immunoprophylaxis to treat infectious diseases. [ABSTRACT FROM AUTHOR]

Published

2022

50. Case report: Functional characterization of a de novo c.145G>A p.Val49Met pathogenic variant in a case of PIGA-CDG with megacolon.

Author

Salinas-Marín, Roberta, Yoshiko Murakami, Alberto González-Domínguez, Carlos, Cruz-Muñoz, Mario Ernesto, Manuel Mora-Montes, Héctor, Morava, Eva, Kinoshita, Taroh, Monroy-Santoyo, Susana, and Martínez-Duncker, Iván

Subjects

CONGENITAL disorders, GLYCOSYLPHOSPHATIDYLINOSITOL, FLOW cytometry, GLYCOSYLATION

Abstract

A subgroup of congenital disorders of glycosylation (CDGs) includes inherited GPI-anchor deficiencies (IGDs) that affect the biosynthesis of glycosylphosphatidylinositol (GPI) anchors, including the first reaction catalyzed by the X-linked PIGA. Here, we show the first PIGA-CDG case reported in Mexico in a male child with a moderate-to-severe phenotype characterized by neurological and gastrointestinal symptoms, including megacolon. Exome sequencing identified the hemizygous variant PIGA c.145G>A (p.Val49Met), confirmed by Sanger sequencing and characterized as de novo. The pathogenicity of this variant was characterized by flow cytometry and complementation assays in PIGA knockout (KO) cells. [ABSTRACT FROM AUTHOR]

Published

2022