Your search keyword '"Goodfellow P"' showing total 27 results

1. Characterization of the Homeodomain Gene EMX2: Sequence Conservation, Expression Analysis, and a Search for Mutations in Endometrial Cancers

Author

Noonan, Ferrin C, Mutch, David G, Ann Mallon, Mary, and Goodfellow, Paul J

Abstract

Previous loss-of-heterozygosity studies in endometrial carcinoma mapped a putative tumor suppressor gene to 10q25.3–26.1. An analysis of genomic sequences for the deletion interval showed several expressed sequence tags and the homeodomain gene EMX2, a homologue of Drosophila melanogaster empty spiracles. Expression studies showed that EMX2transcripts are abundant in the adult uterus and that message levels seem to be inversely correlated with endometrial proliferation. EMX2RNA was more abundant in quiescent postmenopausal endometrium than in premenopausal endometrium. We found decreased EMX2expression in a subset of primary endometrial tumors, and four of six endometrial cancer cell lines investigated failed to express EMX2. The predicted protein showed extensive amino acid conservation with EMX2sequences from several vertebrates. There was also considerable evolutionary conservation in the 3′ untranslated region. To examine the potential function of EMX2in endometrial tumorigenesis, we investigated 20 primary tumors and 6 endometrial cancer cell lines for mutations. Two primary tumors had mutations. Inactivation or reduced expression of EMX2in cancers, coupled with increased expression in the quiescent endometrium, indicate that this homeodomain gene is involved in maintenance of the differentiated state.

Published

2001

2. A 1-Mb Bacterial Clone Contig Spanning the Endometrial Cancer Deletion Region at 1p32–p33

Author

Arlt, Martin F., Li, Muhua, Herzog, Thomas J., and Goodfellow, Paul J.

Abstract

Our laboratory previously reported a high frequency of loss of heterozygosity (LOH) at 1p32–p33 in endometrial cancers. LOH at 1p32–p33 is a specific feature of one of the most aggressive forms of endometrial carcinoma, uterine papillary serous cancer (UPSC). The minimum region of allelic loss in UPSC is defined by D1S190 and D1S447, an interval corresponding to less than 1 cM. Here we describe the construction and characterization of a sequence-ready clone contig that spans the deletion region. The contig consists of 24 bacterial artificial chromosome clones and 18 P1 artificial chromosome clones and spans approximately 1050 kb. The consensus region of allelic loss between D1S190 and D1S447 represents approximately 792 kb. Eight previously described ESTs have been positioned within the contig.

Published

1999

3. Construction of a Mouse Whole-Genome Radiation Hybrid Panel and Application to MMU11

Author

Schmitt, K., Foster, J.W., Feakes, R.W., Knights, C., Davis, M.E., Spillett, D.J., and Goodfellow, P.N.

Abstract

Whole-genome radiation hybrids have been used to construct human genome maps that integrate different types of markers. To investigate this methodology in mammalian species other than humans, a panel of 164 mouse × hamster whole-genome radiation hybrids was constructed. This set of hybrids was used to produce a high-resolution map of a region on MMU11 that included microsatellite markers and cDNA sequences. The mouse homologue of the human SRY-related geneSOX9was mapped to an interval of approximately 1.1 cM flanked by the microsatellite markers D11Mit11 and D11Mit291. This interval includes the region containing the mouseTail-shortmutation, a possible homologue of the human syndrome campomelic dysplasia, which is caused by mutations inSOX9.Our results suggest that whole-genome radiation hybrid technology will be a useful adjunct to mapping the genomes of nonhuman mammalian species.

Published

1996

4. Mapping an Endometrial Cancer Tumor Suppressor Gene at 10q25 and Development of a Bacterial Clone Contig for the Consensus Deletion Interval

Author

Peiffer-Schneider, Stacia, Noonan, Ferrin C., Mutch, David G., Simpkins, Sally B., Herzog, T., Rader, Janet, Elbendary, Alaa, Gersell, Deborah J., Call, Katherine, and Goodfellow, Paul J.

Abstract

Frequent loss of chromosome 10q sequences in endometrial cancers suggests the involvement of a tumorsuppressor gene. Previous loss-of-heterozygosity (LOH)studies have pointed to the 10q25–q26 region as the likely site of a tumor suppressor involved in endometrial tumorigenesis (S. L. Peifferet al.,1995,Cancer Res.55: 1922–1926; S. Nagaseet al.,1996,Br. J. Cancer74: 1979–1983; S. Nagaseet al.,1997,Cancer Res.57: 1630–1633). In an attempt to define further the localization of a tumor suppressor gene at 10q25, we screened a panel of 123 endometrioid adenocarcinomas for loss of heterozygosity of 10q25.3 sequences. Forty-three (35%) revealed LOH at one or more loci. The observed patterns of allelic loss define a minimum consensus region of deletion between D10S221 and D10S610. A sequence-ready bacterial clone contig and a long-range restriction map for a 1-Mb interval spanning the deletion region were developed as the first step in experiments directed toward the discovery the 10q25 tumor suppressor.

Published

1998

5. A High-Resolution Whole Genome Radiation Hybrid Map of Human Chromosome 17q22–q25.3 across the Genes forGHandTK

Author

Foster, Jamie W., Schafer, Alan J., Critcher, Ricky, Spillett, Dominique J., Feakes, Robert W., Walter, Michael A., Dominguez-Steglich, Marina, Guioli, Silvana, Brook, J.David, and Goodfellow, Peter N.

Abstract

We have constructed a whole genome radiation hybrid (WG-RH) map across a region of human chromosome 17q, from growth hormone (GH) to thymidine kinase (TK). A panel of 128 WG-RH hybrid cell lines generated by X-irradiation and fusion has been tested for the retention of 39 sequence-tagged site (STS) markers by the polymerase chain reaction. This genome mapping technique has allowed the integration of existing VNTR and microsatellite markers with additional new markers and existing STS markers previously mapped to this region by other means. The WG-RH map includes eight expressed sequence tag (EST) and three anonymous markers developed for this study, together with 23 anonymous microsatellites and five existing ESTs. Analysis of these data resulted in a high-density comprehensive map across this region of the genome. A subset of these markers has been used to produce a framework map consisting of 20 loci ordered with odds greater than 1000:1. The markers are of sufficient density to build a YAC contig across this region based on marker content. We have developed sequence tags for both ends of a 2.1-Mb YAC and mapped these using the WG-RH panel, allowing a direct comparison of cRay6000to physical distance.

Published

1996

6. Cloning and Characterization ofSOX5,a New Member of the HumanSOXGene Family

Author

Wunderle, Véronique M., Critcher, R., Ashworth, A., and Goodfellow, Peter N.

Abstract

The mammalian Y-linked testis determining gene,SRY,encodes a protein with a DNA binding motif known as the HMG box. A large family of genes sharing a high similarity with theSRYHMG box and namedSox(Sry-related HMG box) in mouse andSOXin human has been identified from various organisms. We have clonedSOX5,a new member of the humanSOXgene family.SOX5cDNAs isolated from a human adult testis cDNA library show a high similarity with the mouseSox5transcript over a large region identical in all the human cDNAs. However, comparison of the 5′ unique sequences of the cDNAs suggests that theSOX5gene is subject to alternative splicing. Genomic analysis identified aSOX5pseudogene located on 8q21.1, whereas theSOX5gene itself, which contains a minimum of five introns, maps to 12p12.1. In contrast to the mouse gene, the humanSOX5gene is expressed in a variety of human tissues, and different size transcripts are observed in adult testis and fetal brain.

Published

1996

7. 41 Kilobases of Analyzed Sequence from the Pseudoautosomal and Sex-Determining Regions of the Short Arm of the Human Y Chromosome

Author

Whitfield, L.Simon, Hawkin, Trevor L., Goodfellow, Peter N., and Sulston, John

Abstract

Determination of 41.2 kb of Y chromosome genomic sequence has been made from a cosmid that spans the Yp pseudoautosomal boundary and includes 18.5 kb of sequence from the patient-defined sex-determining region of the Y chromosome. An AceDB database of the sequence and the analysis data have been produced as a resource for studies of the evolution and population genetics of the Y chromosome. Comparison of the 18.5 kb from the sex determining region to the sex determining region of mouse does not locate any areas of similarity outside SRY/Sry.Indeed, no coding regions other than those previously reported can be detected anywhere in the 41 kb. The Y-specific and pseudoautosomal portions of this sequence have different repeat sequence and GC contents: this may have relevance both to the events defining the pseudoautosomal boundary and to the course of sequence evolution in the absence of recombination.

Published

1995

8. Physical and Genetic Maps for Chromosome 10

Author

Lichter, Jay B., Difilippantonio, Michael J., Pakstis, Andrew J., Goodfellow, Paul J., Ward, David C., and Kidd, Kenneth K.

Abstract

A fluorescence in situ hybridization (FISH) physical map of 14 polymorphic loci on chromosome 10 covers over 62% of the fractional length of chromosome 10. The positions of three previously mapped loci are confirmed, nine more are refined, and two new loci are cytogenetically mapped. The order of loci determined by FISH agrees with that obtained by genetic linkage studies. When the distance estimates for the physical map are compared to the distance estimates of our existing linkage map, the sex average ratio of the fractional length (FL) per centimorgan (cM) for this portion of chromosome 10 is 0.004 (or 0.4% FL/cM). However, the average ratios for male- and female-specific genetic distances are quite different, in agreement with an overall higher rate of recombination in females (0.008 FL/cM and 0.003 FL/cM, respectively). Moreover, the ratio across the centromere is larger for both the male (0.031 FL/cM) and the female (0.009 FL/cM) than the ratio encompassing the q arm (0.006 FL/cM for males and (0.002 FL/cM for females), suggesting that there is reduced recombination at the centromere in both the male and the female maps when compared to the physical distance generated from FISH on metaphase chromosomes. Copyright 1993, 1999 Academic Press

Published

1993

9. Physical Mapping of the Bloom Syndrome Region by the Identification of YAC and P1 Clones from Human Chromosome 15 Band q26.1

Author

Straughen, Joel, Ciocci, Susan, Ye, Tian-Zhang, Lennon, David N., Proytcheva, Maria, Alhadeff, Becky, Goodfellow, Peter, German, James, Ellis, Nathan A., and Groden, Joanna

Abstract

The gene for Bloom syndrome (BLM) has been mapped to human chromosome 15 band q26.1 by homozygosity mapping. Further refinement of the location ofBLMhas relied upon linkage-disequilibrium mapping and somatic intragenic recombination. In combination with these mapping approaches and to identify novel DNA markers and probes for theBLMcandidate region, a contiguous representation of the 2-Mb region that contains theBLMgene was generated and is presented here. YAC and P1 clones from the region have been identified and ordered by using previously available genetic markers in the region along with newly developed sequence-tagged sites from radiation-reduced hybrids, polymorphic dinucleotide repeat loci, and end sequences of YACs and P1s. A long-range restriction map of the 2-Mb region that allowed estimation of the distance between polymorphic microsatellite loci is also reported. This map and the DNA markers derived from it were instrumental in the recent identification of theBLMgene.

Published

1996

10. Construction of a Radiation Hybrid Map of Chromosome 9p

Author

Bouzyk, Mark, Bryant, Stephen P., Schmitt, Karin, Goodfellow, Peter N., Ekong, Rosemary, and Spurr, Nigel K.

Abstract

A radiation hybrid panel has been constructed for chromosome 9 using the somatic cell hybrid GM10611 as the donor cell line fused to the hamster cell line A23. The hybrid GM10611 was characterized by fluorescencein situhybridization and reverse painting onto spreads of normal human metaphase chromosomes; it contains human chromosome 9 as the only cytogenetically detectable human material. GM10611 was irradiated with 6000 rads of X rays prior to fusion, a total of 93 independent clones were selected, and frozen stocks and DNA were prepared from each clone. These clones were screened by PCR amplification with oligonucleotide primers for sequence-tagged sites specific for 50 single-copy loci mapping to the short arm of chromosome 9. The average retention frequency of these hybrids was approximately 23%. The markers were ordered into a framework map by analyzing coretention patterns, minimizing the number of obligatory chromosome breaks, and finally confirming the order by maximum likelihood methods. A framework map ordering 27 markers with odds greater than 1000:1 was constructed. A further 16 markers that could not be uniquely placed on the map with the required support were positioned within a range of adjacent intervals.

Published

1996

11. Genomic and Yeast Artificial Chromosome Long-Range Regular Article Linking Six Loci in 10q11.2 and Spanning the Multiple Endocrine Neoplasia Type 2A (MEN2A) Region

Author

Brooks-Wilson, Angela R., Lichter, Jay B., Ward, David C., Kidd, Kenneth K., and Goodfellow, Paul J.

Abstract

Multiple endocrine neoplasia types 2A and 2B (MEN 2A and MEN 2B) and familial medullary thyroid carcinoma (FMTC) are dominantly inherited cancers that have in common the clinical feature of medullary thyroid carcinoma (MTC). We have performed both genomic long-range restriction mapping and yeast artificial chromosome (YAC) contig assembly and restriction mapping to establish physical linkage, order, and distances between six loci in 10q11.2 near the genes responsible for these hereditary cancers. RET, D10S94, D10S182,and D10S102have been mapped in genomic DNA. RET, D10S94, D10S182, D10F3853, and the 10q11.2 sequences detected by DNA marker DM124 are encompassed by a 1-Mb YAC contig. Six physically linked loci are within 1.4 Mb and have an order and orientation of 10cen, D10F38S3, DM124, RET, D10S94, D10S182, D10S102, 10qter. Mutations in the RETproto-oncogene have recently been demonstrated to be associated with MEN 2A and FMTC. RETis located within a genetically defined MEN2Acandidate interval between D10S141and D10S94; MEN2Bhas been mapped to a larger, overlapping region between D10S141and a more distal locus, RBP3. Both our genomic physical map and our YAC contig span the entire MEN2Acandidate region and overlap with that of MEN2B. These maps will facilitate the identification of genes that can be considered candidates for MEN2Band the identification of tumor-specific alterations important in sporadic MTC.

Published

1993

12. Cloning and characterization of SOX5, a new member of the human SOX gene family.

Author

Wunderle VM, Critcher R, Ashworth A, and Goodfellow PN

Subjects

Adult, Amino Acid Sequence, Animals, Base Sequence, Cloning, Molecular, DNA, Complementary, Humans, Male, Mice, Molecular Sequence Data, SOXD Transcription Factors, Transcription Factors, Chromosomes, Human, Pair 12, DNA-Binding Proteins genetics, Nuclear Proteins genetics

Abstract

The mammalian Y-linked testis determining gene, SRY, encodes a protein with a DNA binding motif known as the HMG box. A large family of genes sharing a high similarity with the SRY HMG box and named Sox (Sry-related HMG box) in mouse and SOX in human has been identified from various organisms. We have cloned SOX5, a new member of the human SOX gene family. SOX5 cDNAs isolated from a human adult testis cDNA library show a high similarity with the mouse Sox5 transcript over a large region identical in all the human cDNAs. However, comparison of the 5' unique sequences of the cDNAs suggests that the SOX5 gene is subject to alternative splicing. Genomic analysis identified a SOX5 pseudogene located on 8q21.1, whereas the SOX5 gene itself, which contains a minimum of five introns, maps to 12p12.1. In contrast to the mouse gene, the human SOX5 gene is expressed in a variety of human tissues, and different size transcripts are observed in adult testis and fetal brain.

Published

1996

13. Genomic and yeast artificial chromosome long-range physical maps linking six loci in 10q11.2 and spanning the multiple endocrine neoplasia type 2A (MEN2A) region.

Author

Brooks-Wilson AR, Lichter JB, Ward DC, Kidd KK, and Goodfellow PJ

Subjects

Base Sequence, Carcinoma, Medullary genetics, Chromosome Mapping, DNA genetics, DNA Primers, Genetic Markers, Humans, Molecular Sequence Data, Proto-Oncogene Mas, Proto-Oncogenes, Restriction Mapping, Thyroid Neoplasms genetics, Chromosomes, Artificial, Yeast, Chromosomes, Human, Pair 10, Multiple Endocrine Neoplasia genetics

Abstract

Multiple endocrine neoplasia types 2A and 2B (MEN 2A and MEN 2B) and familial medullary thyroid carcinoma (FMTC) are dominantly inherited cancers that have in common the clinical feature of medullary thyroid carcinoma (MTC). We have performed both genomic long-range restriction mapping and yeast artificial chromosome (YAC) contig assembly and restriction mapping to establish physical linkage, order, and distances between six loci in 10q11.2 near the genes responsible for these hereditary cancers. RET, D10S94, D10S182, and D10S102 have been mapped in genomic DNA. RET, D10S94, D10S182, D10F38S3, and the 10q11.2 sequences detected by DNA marker DM124 are encompassed by a 1-Mb YAC contig. Six physically linked loci are within 1.4 Mb and have an order and orientation of 10cen, D10F38S3, DM124, RET, D10S94, D10S182, D10S102, 10qter. Mutations in the RET proto-oncogene have recently been demonstrated to be associated with MEN 2A and FMTC. RET is located within a genetically defined MEN2A candidate interval between D10S141 and D10S94; MEN2B has been mapped to a larger, overlapping region between D10S141 and a more distal locus, RBP3. Both our genomic physical map and our YAC contig span the entire MEN2A candidate region and overlap with that of MEN2B. These maps will facilitate the identification of genes that can be considered candidates for MEN2B and the identification of tumor-specific alterations important in sporadic MTC.

Published

1993

14. Isolation of DNA markers from a region between incontinentia pigmenti 1 (IP1) X-chromosomal translocation breakpoints by a comparative PCR analysis of a radiation hybrid subclone mapping panel.

Author

Gorski JL, Burright EN, Reyner EL, Goodfellow PN, and Burgess DL

Subjects

Animals, Blotting, Southern, Chromosome Mapping, Cloning, Molecular, Cricetinae, DNA, Electrophoresis, Gel, Pulsed-Field, Humans, Hybrid Cells, Mice, Molecular Sequence Data, Polymerase Chain Reaction, Radiation Genetics, Repetitive Sequences, Nucleic Acid, Genetic Markers, Incontinentia Pigmenti genetics, Translocation, Genetic, X Chromosome

Abstract

A strategy based on the use of human-specific interspersed repetitive sequence (IRS)-PCR amplification was used to isolate regional DNA markers in the vicinity of the incontinentia pigmenti 1 (IP1) locus. A radiation hybrid (RH) resulting from a fusion of an irradiated X-only somatic cell hybrid (C12D) and a thymidine kinase deficient (TK-) hamster cell line (a23) was identified as containing multiple X chromosome fragments, including DNA markers spanning IP1 X-chromosomal translocation breakpoints within region Xp11.21. From this RH, a panel of subclones was constructed and analyzed by IRS-PCR amplification to (a) identify subclones containing a reduced number of X chromosome fragments spanning the IP1 breakpoints and (b) construct a mapping panel to assist in identifying regional DNA markers in the vicinity of the IP1 locus. By using this strategy, we have isolated three different IRS-PCR amplification products that map to a region between IP1 X chromosome translocation breakpoints. A total of nine DNA sequences have now been mapped to this region; using these DNA markers for PFGE analyses, we obtained a probe order DXS14-DXS422-MTHFDL1-DXS705. These DNA markers provide a starting point for identifying overlapping genomic sequences spanning the IP1 translocation breakpoints; the availability of IP1 translocation breakpoints should assist the molecular analysis of this locus.

Published

1992

15. A high-resolution meiotic mapping panel for the pericentromeric region of chromosome 10.

Author

Lichter JB, Wu J, Miller D, Goodfellow PJ, and Kidd KK

Subjects

Centromere, Crossing Over, Genetic, Female, Genetic Linkage, Genetic Markers, Humans, Male, Meiosis genetics, Multiple Endocrine Neoplasia genetics, Pedigree, Chromosome Mapping methods, Chromosomes, Human, Pair 10 ultrastructure

Abstract

Familial multiple endocrine neoplasia type 2A (MEN 2A) is a dominantly inherited cancer syndrome characterized by tumors in tissues derived from the neural crest. The disease manifests as medullary carcinoma of the thyroid, pheochromocytoma, and hyperparathyroidism. The MEN2A locus has been mapped near the centromere of chromosome 10 by linkage analysis. Statistical analyses have not resolved the location of MEN2A among several close markers. We have used our family material to refine the positions of 36 identified and confirmed crossovers among the markers most closely linked to MEN2A. This high-resolution meiotic mapping panel will help order loci in this pericentromeric region and narrow the region in which MEN2A maps.

Published

1992

16. Isolation and high-resolution mapping of new DNA markers from the pericentromeric region of chromosome 10.

Author

Miller DL, Dill FJ, Lichter JB, Kidd KK, and Goodfellow PJ

Subjects

Centromere, Chromosome Mapping, DNA Probes, Humans, Hybrid Cells, Multiple Endocrine Neoplasia genetics, Chromosomes, Human, Pair 10 ultrastructure, DNA genetics, Genetic Markers

Abstract

The gene responsible for multiple endocrine neoplasia type 2A (MEN 2A) has been localized to the pericentromeric region of chromosome 10. Several markers that fail to recombine with MEN2A have been identified, including D10Z1, D10S94, D10S97, and D10S102. Meiotic mapping in the MEN2A region is limited by the paucity of critical crossovers identified and by the dramatically reduced rates of recombination in males. Additional approaches to mapping loci in the pericentromeric region of chromosome 10 are required. We have undertaken the generation of a detailed physical map by radiation hybrid mapping. Here we report the development of a radiation hybrid panel and its use in the mapping of new DNA markers in pericentromeric chromosome 10. The radiation-reduced hybrids used for mapping studies all retain small subchromosomal fragments that include both D10S94 and D10Z1. One hybrid was selected as the source of DNA for cloning. One hundred five human recombinant clones were isolated from a lambda library made with pp11A DNA. We have completed regional mapping of 22 of those clones using our radiation hybrid mapping panel. Seven markers have been identified and, when taken together with previously meiotically mapped markers, define eight radiation hybrid map intervals between D10S34 and RBP3. The identical order is found for a number of these using either the radiation hybrid mapping panel or the meiotic mapping panel. We believe that this combination cloning and mapping approach will facilitate the precise positioning of new markers in pericentromeric chromosome 10 and will help in refining further the localization of MEN2A.

Published

1992

17. Identification and characterization of a gene at D10S94 in the MEN2A region.

Author

McDonald H, Smailus D, Jenkins H, Adams K, Simpson NE, and Goodfellow PJ

Subjects

Amino Acid Sequence, Animals, Base Sequence, Chromosomes, Human, Pair 10, Cricetinae, Humans, Hybrid Cells, Mice genetics, Molecular Sequence Data, Nuclear Proteins genetics, Phosphoproteins genetics, Polymerase Chain Reaction, Sequence Homology, Nucleic Acid, Nucleolin, Genes, Dominant, Genetic Markers, Multiple Endocrine Neoplasia genetics, RNA-Binding Proteins

Abstract

We have identified a candidate for the gene responsible for multiple endocrine neoplasia type 2A (MEN 2A) at D10S94 in proximal 10q11.2. An evolutionarily conserved sequence from D10S94 was used as a probe to isolate cDNAs corresponding to a gene that we have termed mcs94-1. The gene spans 11 kb and has an unmethylated CpG island at its 5' end. The mcs94-1 transcript is approximately 2.4 kb in length and is widely expressed. It encodes a putative 415-amino-acid polypeptide that is similar in sequence to nucleolin, an abundant nucleolar protein. Mcs94-1 was examined as a candidate for MEN2A through nucleotide sequence analysis of mcs94-1 exons from an MEN 2A chromosome and its wildtype homologue from an MEN 2A patient. The major portion of the expressed mcs94-1 sequence was examined. No differences in sequence were found between the two alleles.

Published

1992

18. A cluster of CpG islands at D10S94, near the locus responsible for multiple endocrine neoplasia type 2A (MEN2A).

Author

Brooks-Wilson AR, Smailus DE, and Goodfellow PJ

Subjects

Base Sequence, Carcinoma genetics, Chromosome Walking, Cosmids, Electrophoresis, Gel, Pulsed-Field, Humans, Hybrid Cells, Male, Restriction Mapping, Thyroid Neoplasms genetics, Chromosomes, Human, Pair 10, Genes, Dominant, Genetic Markers, Multiple Endocrine Neoplasia genetics

Abstract

We report the characterization of a dense cluster of CpG islands at D10S94 in proximal 10q11.2. D10S94 is tightly linked to the gene responsible for multiple endocrine neoplasia type 2A (MEN 2A), a dominantly inherited tumor syndrome characterized by medullary thyroid carcinoma (MTC), pheochromocytoma, and/or parathyroid adenoma. To date, no recombinants between D10S94 and MEN2A have been identified. The gene(s) responsible for two additional dominantly inherited disorders involving cancer of the medullary thyroid, MEN 2B (MEN2B), and dominantly inherited MTC without additional clinical features (MTC1), also map to this region. The gene or genes responsible for these disorders may be located at or near the D10S94 locus. A 570-kb long-range restriction map has been generated by pulsed-field gel electrophoresis using probes developed during a 160-kb bidirectional cosmid walk at D10S94. Six CpG islands are clustered within a 180-kb region; five fall within a 145-kb NotI restriction fragment that is contained in its entirety in our cosmid contig. The SacII, SfiI, and NotI restriction maps for lymphoblast and cloned DNA are concordant. These CpG islands may represent the 5' ends of candidate genes for MEN2A, MEN2B, and/or MTC1. One gene designated mcs94-1, which is associated with one of the CpG islands in this cluster, has been isolated and characterized in detail.

Published

1992

19. Human repeat element-mediated PCR: cloning and mapping of chromosome 10 DNA markers.

Author

Brooks-Wilson AR, Smailus DE, Weier HU, and Goodfellow PJ

Subjects

Animals, Base Sequence, Cricetinae, Cricetulus, Humans, Hybrid Cells, Mice, Molecular Sequence Data, Multiple Endocrine Neoplasia genetics, Chromosomes, Human, Pair 10, Genetic Markers, Polymerase Chain Reaction methods, Repetitive Sequences, Nucleic Acid

Abstract

Repeat element-mediated PCR can facilitate rapid cloning and mapping of human chromosomal region-specific DNA markers from somatic cell hybrid DNA. PCR primers directed to human repeat elements result in human-specific DNA synthesis; template DNA derived from a somatic cell hybrid containing the human chromosomal region of interest provides region specificity. We have generated a series of repeat element-mediated PCR clones from a reduced complexity somatic cell hybrid containing a portion of human chromosome 10. The cloning source retains the centromere and tightly linked flanking markers, plus additional chromosome 10 sequences. Twelve new inter-Alu, two inter-L1, and four inter-Alu/L1 repeat element-mediated PCR clones were mapped by hybridization to Southern blots of repeat element-mediated PCR products amplified from somatic cell hybrid DNA templates. Two inter-Alu clones mapped to the pericentromeric region. We propose that a scarcity of Alu elements in the pericentromeric region of chromosome 10 contributed to the low number of clones obtained from this region. One inter-Alu clone, pC11/A1S-6-c23, defines the D10S94 locus, which is tightly linked to MEN2A and D10Z1.

Published

1992

20. Additional RFLPs at D10S94 and the development of PCR-based variant detection systems: implications for disease genotype prediction in MEN 2A, MEN 2B, and MTC1 families.

Author

Brooks-Wilson AR, Smailus D, Gilchrist D, and Goodfellow PJ

Subjects

Base Sequence, Endodeoxyribonucleases metabolism, Genetic Testing, Genotype, Humans, Molecular Sequence Data, Oligodeoxyribonucleotides genetics, Polymerase Chain Reaction, Carcinoma genetics, Chromosomes, Human, Pair 10, Multiple Endocrine Neoplasia genetics, Polymorphism, Restriction Fragment Length, Thyroid Neoplasms genetics

Published

1992

21. Isolation of probes specific to human chromosomal region 6p21 from immunoselected irradiation-fusion gene transfer hybrids.

Author

Ragoussis J, Jones TA, Sheer D, Shrimpton AE, Goodfellow PN, Trowsdale J, and Ziegler A

Subjects

Animals, Blotting, Southern, Cell Fusion, Complement System Proteins genetics, Cricetinae, Cricetulus, DNA Probes genetics, Genes, MHC Class I, Genes, MHC Class II, Genetic Markers, HLA Antigens genetics, Humans, Hybrid Cells radiation effects, Nucleic Acid Hybridization, Polymerase Chain Reaction, Repetitive Sequences, Nucleic Acid, Selection, Genetic, Chromosomes, Human, Pair 6, DNA Probes isolation & purification, Major Histocompatibility Complex

Abstract

A hybrid cell line (R21/B1) containing a truncated human chromosome 6 (6pter-6q21) and a human Y chromosome on a hamster background was irradiated and fused to A23 (TK-) or W3GH (HPRT-) hamster cells. Clones containing expressed HLA class I genes (4/40) were selected using monoclonal antibodies. These clones were recloned and analyzed with a panel of probes from the HLA region. One hybrid (4G6) contained the entire HLA complex. Two other hybrids (4J4 and 4H2) contained only the HLA class I region, while the fourth hybrid (5P9) contained HLA class I and III genes in addition to other genes located in the 6p21 chromosomal region. In situ hybridization showed that the hybrid cells contained more than one fragment of human DNA. Alu and LINE PCR products were derived from these cells and compared to each other as well as to products from two somatic cell hybrids having the 6p21 region in common. The PCR fragments were then screened on conventional Southern blots of the somatic cell hybrids to select a panel of novel probes encompassing the 6p21 region. In addition, the origin of the human DNA fragments in hybrid 4J4 was determined by regional mapping of PCR products.

Published

1991

22. Generation of novel sequence tagged sites (STSs) from discrete chromosomal regions using Alu-PCR.

Author

Cole CG, Goodfellow PN, Bobrow M, and Bentley DR

Subjects

Animals, Base Sequence, Cricetinae, Cricetulus, Genome, Human, Humans, Hybrid Cells radiation effects, Male, Mice, Molecular Sequence Data, Repetitive Sequences, Nucleic Acid, X Chromosome, Chromosome Mapping methods, Genetic Markers, Polymerase Chain Reaction methods, Sequence Tagged Sites

Abstract

Human DNA segments from discrete chromosomal regions were generated by utilizing Alu-element-based polymerase chain reaction (Alu-PCR) of an irradiation-fusion hybrid containing approximately 10 to 15 Mb of human DNA. Following cloning into a plasmid vector, a subset of the clones was used to generate sequence tagged sites (STSs) de novo. By means of a panel of hybrids containing portions of the human X chromosome, the STSs were shown to localize to two chromosomal regions, Xq24-Xq26 and Xcen-Xq13, reflecting the presence in the irradiation-fusion hybrid of two human chromosome fragments. These results demonstrate that high densities of STSs can be rapidly and efficiently generated from defined regions of the human genome using Alu-PCR.

Published

1991

23. Rapid cloning and characterization of new chromosome 10 DNA markers by Alu element-mediated PCR.

Author

Brooks-Wilson AR, Goodfellow PN, Povey S, Nevanlinna HA, de Jong PJ, and Goodfellow PJ

Subjects

Animals, Base Sequence, Blotting, Southern, Cloning, Molecular, DNA genetics, Gene Library, Humans, Hybrid Cells, Molecular Sequence Data, Nucleotide Mapping, Polymerase Chain Reaction, Templates, Genetic, Chromosomes, Human, Pair 10, Genetic Markers, Repetitive Sequences, Nucleic Acid

Abstract

Alu element-mediated polymerase chain reaction is a strategy for rapidly cloning and mapping human DNA markers from mixed DNA sources. A novel primer homologous to the 3' end of the human Alu repeat element provides the basis for preferential synthesis of human DNA fragments from human/rodent somatic cell hybrid DNA template. This approach has been used to isolate a series of new markers from chromosome 10. The Alu element-mediated PCR probes were regionally assigned on chromosome 10 by hybridization to Southern blots of Alu PCR-synthesized DNA derived from somatic cell hybrid template DNA. Alu element-mediated PCR is generally applicable and makes possible the analysis of complex genomes with a speed and sensitivity that has not been previously possible.

Published

1990

24. Cloning and mapping of a testis-specific gene with sequence similarity to a sperm-coating glycoprotein gene.

Author

Kasahara M, Gutknecht J, Brew K, Spurr N, and Goodfellow PN

Subjects

Amino Acid Sequence, Animals, Base Sequence, Blotting, Southern, Cell Adhesion Molecules, Chromosomes, Human, Pair 6, Cloning, Molecular, DNA genetics, DNA isolation & purification, Humans, Male, Membrane Proteins, Mice, Mice, Inbred BALB C, Molecular Sequence Data, Rats, Sequence Homology, Nucleic Acid, Glycoproteins genetics, Testis metabolism

Abstract

A testis-specific gene Tpx-1, located between Pgk-2 and Mep-1 on mouse chromosome 17, was isolated from a cosmid clone, and its cDNA sequences were determined. The predicted coding sequence of Tpx-1 isolated from BALB/c mice showed 64.2% nucleotide and 55.1% amino acid sequence similarity with that of a rat sperm-coating glycoprotein gene, the protein product of which is secreted by the epididymis. To examine the evolutionary relationship between Tpx-1 and a sperm-coating glycoprotein gene, the cDNA sequence of TPX1, the human counterpart of Tpx-1, was determined. The comparison of the predicted coding sequences of Tpx-1 and TPX1 showed 77.8% nucleotide and 70% amino acid sequence similarity. Since Tpx-1 (from mouse) is more similar to TPX1 (from man) than it is to a rat sperm-coating glycoprotein gene, we conclude that Tpx-1 (TPX1) and a sperm-coating glycoprotein gene are closely related, but distinct, genes belonging to the same gene family. The predicted Tpx-1 protein of a t mutant mouse CRO437 differs from that of BALB/c mice by one amino acid insertion in the putative signal peptide. TPX1 was mapped to 6p21-qter by Southern blot analysis of interspecies somatic hybrid cell lines.

Published

1989

25. A method for generating hybrids containing nonselected fragments of human chromosomes.

Author

Benham F, Hart K, Crolla J, Bobrow M, Francavilla M, and Goodfellow PN

Subjects

Animals, Blotting, Southern, Cell Fusion, Cricetinae, Cricetulus, DNA, Satellite analysis, Genetic Markers, Humans, X Chromosome, Chromosome Mapping methods, Chromosomes, Human radiation effects, Hybrid Cells radiation effects

Abstract

We have used an irradiation and fusion technique to generate somatic cell hybrids that contain human chromosomal fragments. As a model system, a human-hamster hybrid containing a single human X chromosome was gamma-irradiated and fused with a rodent line. Hybrids were obtained without imposing direct selection for human material. Analysis of 29 clones by in situ hybridization and Southern blotting revealed that human fragments were incorporated into the hybrid cell genomes in most lines. Like chromosome-mediated gene transfer (CMGT)-generated hybrids, these hybrids contained multiple human fragments and retained alphoid centromeric sequences with a high frequency. However, unlike the CMGT, human fragments (apart from alphoid sequences) of less than 10(7) bp showed no evidence for rearrangements. This technique provides a method for constructing hybrids that contain a limited number of small human fragments derived exclusively from any chromosome of choice without the need to impose selection. Such hybrids provide a valuable resource for high-resolution mapping over short distances and for the isolation of disease and other loci mapped genetically.

Published

1989

26. Human homologs of two testes-expressed loci on mouse chromosome 17 map to opposite arms of chromosome 6.

Author

Bibbins KB, Tsai JY, Schimenti J, Sarvetnick N, Zoghbi HY, Goodfellow P, and Silver LM

Subjects

Alleles, Animals, Blotting, Southern, Cell Line, Chromosome Inversion, Genetic Markers, Haplotypes, Humans, Hybrid Cells, Male, Mice, Multigene Family, Proteins, Ubiquitin-Protein Ligases, t-Complex Genome Region, Chromosome Mapping, Chromosomes, Human, Pair 6, Intracellular Signaling Peptides and Proteins, Microtubule-Associated Proteins, Nuclear Proteins genetics, Testis ultrastructure

Abstract

Our laboratory has recently cloned and characterized two testes-expressed loci--the Tcp-10 gene family cluster and the D17Si11 gene--that map to the proximal portion of mouse chromosome 17. Human homologs of both loci have been identified and cloned. Somatic cell hybrid lines have been used to map the human homolog of D17Si11 to the short arm of chromosome 6 (p11-p21.1) along with homologs of other genes from the (Pim-1)-(Pgk-2) region of the mouse chromosome. The human TCP 10 locus maps to the long arm of chromosome 6 (q21-qter) along with homologs of other genes from the mouse chromosome 17 region between the centromere and Pim-1. The mapping of large portions of the mouse t haplotype to unlinked regions on human chromosome 6 rules out the possibility that a t-haplotype-like chromosome could exist in humans.

Published

1989

27. Chromosomal localization of zinc finger protein genes in man and mouse.

Author

Ashworth A, Williams BP, Buchberg AM, Goodfellow PN, Solomon E, Potter J, and Willison KR

Subjects

Animals, Chromosome Mapping, Crosses, Genetic, Genes, Genetic Linkage, Humans, Hybrid Cells, Male, Mice, Inbred Strains genetics, Polymorphism, Restriction Fragment Length, Species Specificity, Chromosomes, Human, Pair 17, DNA-Binding Proteins genetics, Metalloproteins genetics, Mice genetics, Multigene Family

Abstract

We have determined the mouse and human chromosomal location of a gene (Zfp-3) that codes for a protein that contains potential DNA zinc-binding fingers. An analysis of the segregation of restriction fragment length polymorphisms in recombinant inbred strains and in an interspecific backcross demonstrated that Zfp-3 is located on mouse chromosome 11. Zfp-3 is very closely linked to the Trp53-1 locus but unlinked to another finger protein gene Zfp-4 located on mouse chromosome 8. In humans ZFP3 has been localized to chromosome 17p12-17pter and thus is part of the conserved linkage group between this chromosome and the distal half of mouse chromosome 11.

Published

1989