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101. Surgical Results in Ocular Trauma Involving the Posterior Segment

Author

Brinton, Gregory S., Aaberg, Thomas M., Reeser, Frederick H., Topping, Trexler M., and Abrams, Gary W.

Abstract

Of 106 eyes with trauma involving the posterior segment, 12 could not be repaired, 74 were treated with vitrectomy, and 20 without vitrectomy. Fifty-five eyes (52%) achieved functional success (defined as a final visual acuity of 6/30 [20/100] or better or as a postoperative improvement in visual acuity from light perception or worse to 6/240 [5/200] or better), 16 (15%) attained anatomic success (attached retinas and generally clear media) but were functional failures, and 35 (33%) were both anatomic and functional failures.

Published
1982
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103. Posttraumatic Endophthalmitis

Author

Brinton, Gregory S., Topping, Trexler M., Hyndiuk, Robert A., Aaberg, Thomas M., Reeser, Frederick H., and Abrams, Gary W.

Abstract

• Nineteen consecutive cases of culture-proved posttraumatic endophthalmitis occurred. Over an eight-year period, 19 (7.4%) of 257 patients with penetrating trauma had endophthalmitis develop, and 19 (31.1%) of 61 cases of endophthalmitis were due to trauma. Eleven (10.7%) of 103 patients with intraocular foreign bodies had endophthalmitis develop. Final visual acuity was 20/200 or better in eight (42.1%) of 19 and 20/30 or better in five (26.3%) of 19 cases of posttraumatic endophthalmitis. Organisms cultured were similar to those in the other types of endophthalmitis, except that Bacillus species were seen only in posttraumatic endophthalmitis (five [26.3%] of 19). Virulent organisms or retinal breaks or detachments seen at the time of primary repair indicated poor prognoses.

Published
1984
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105. Vitrectomy for Injury: The Effect on Intraocular Proliferation Following Perforation of the Posterior Segment of the Rabbit Eye

Author

Abrams, Gary W., Topping, Trexler M., and Machemer, Robert

Abstract

• Perforating injuries were produced in the posterior segments of rabbit eyes. A control group had no surgery; a second group underwent closed vitrectomy immediately after injury; and a third group had closed vitrectomy delayed two weeks following injury. The eyes were then observed for four weeks. Transvitreal proliferation, which was found in each of the control eyes, was effectively prevented in the eyes that underwent immediate vitrectomy. Established transvitreal proliferation was removed and its recurrence prevented by delayed vitrectomy. These results establish the principle that vitreous acts as a scaffold for proliferation. Removal of the vitreous eliminates the structures along which proliferation can occur and thus effectively prevents transvitreal proliferation. Early removal of vitreous in severely injured eyes with vitreous damage is recommended.

Published
1979
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106. Experimental Double-Perforating Injury of the Posterior Segment in Rabbit Eyes: The Natural History of Intraocular Proliferation

Author

Topping, Trexler M., Abrams, Gary W., and Machemer, Robert

Abstract

• A reproducible model of double perforating injury of the posterior segment of the rabbit eye was developed. Immediately after injury, a vitreous condensation was visible between wounds. The scleral exit wound was sealed by fibroblastic proliferation of probable episcleral origin by the fourth day and the entrance similarly by the seventh day. Cellular proliferations originating in the wounds crossed the vitreous cavity following the vitreous injury tract or condensed vitreous to the disc or to the vitreous base. The earliest intraocular proliferations, composed of spindle-shaped, fibroblast-like cells, were seen at day 4. Occasional pigment epithelia were present in and on these proliferations. Other proliferations occurred directly on the retinal surface adjacent to the wounds. The transvitreous proliferations employed the vitreous as a scaffold, while the surface proliferations used the retinal surface for contact guidance.

Published
1979
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107. Folding autonomy of the kringle 4 fragment of human plasminogen.

Author

Trexler, M and Patthy, L

Abstract

Kringle 4, an 88-residue plasminogen fragment carrying a lysine-binding site, loses its affinity for lysine-Sepharose upon reductive cleavage of its disulfide bridges. Aerobic incubation of the reduced, denatured fragment results in the rapid restoration of the disulfide bonds with concomitant recovery of lysine-Sepharose affinity. The ability of the unfolded fragment to regain its native conformation suggests that the kringle structure is an autonomous folding domain. During refolding of kringle 4 the native disulfide bonds, (formula; see text) and (formula; see text), appears first. The folding intermediate possessing these two disulfide bridges already binds to lysine-Sepharose, indicating that the third native bridge, which in native kringle 4 connects residues Cys1 and Cys79, is not essential for the maintenance of the biologically active conformation of kringle 4. Comparison of the sequences of human prothrombin, urokinase, and plasminogen kringles revealed that the residues surrounding the (formula; see text) and (formula; see text) bridges constitute the most conservative segments of kringles, whereas the residues neighboring the (formula; see text) bridge are not highly conserved. We propose that conservation of various residues in the different kringles reflects their importance for the folding autonomy of kringles.

Published
1983
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108. Posterior Segment Complications after Vitrectomy for Macular Hole

Author

Park, Susanna S., Marcus, Dennis M., Duker, Jay S., Pesavento, Richard D., Topping, Trexler M., Frederick, Albert R., and D'Amico, Donald J.

Abstract

Purpose:The purpose of this study is to assess the rate of posterior segment complications after vitreous surgery for macular holes and to evaluate the effect of such complications on final visual outcome.

Published
1995
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109. Ultrastructural Ocular Pathology of Hunter's Syndrome: Systemic Mucopolysaccharidosis Type II

Author

Topping, Trexler M., Kenyon, Kenneth R., Goldberg, Morton F., and Maumenee, A. Edward

Abstract

THE SYSTEMIC mucopolysaccharidoses (MPS) are of ophthalmologic interest because about 75% of patients with these inherited disorders of mucopolysaccharide metabolism develop clinically significant corneal clouding.1 The histologic and ultrastructural pathologic condition of the clouded corneas from these patients has been the subject of many reports.2-7 However, only one report8 has described the ocular histopathology of a systemic MPS case with clear corneas, which occurred in a patient with Hunter's syndrome.Hunter's syndrome (systemic MPS type II), one of the six or more variants of the systemic MPS,1 resembles the more common Hurler's syndrome (gargoylism, systemic MPS type I) in several respects. Clinically, Hunter's syndrome appears as a less severe form of Hurler's with respect to progressive growth and mental retardation, coarse gargoyle-like facies, multiple skeletal deformities, hepatosplenomegaly, and early death. Both syndromes are also characterized by the increased urinary excretion and excessive tissue accumulations of two

Published
1971
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110. Experimental double-perforating injury of the posterior segment in rabbit eyes: the natural history of intraocular proliferation

Author

Gary W. Abrams, Trexler M. Topping, and Robert Machemer

Subjects
Male, Time Factors, genetic structures, Wounds, Penetrating, Vitreous cavity, Contact guidance, Retina, chemistry.chemical_compound, Eye Injuries, Medicine, Animals, Pigment Epithelium of Eye, Intraocular Pressure, Wound Healing, business.industry, Rabbit (nuclear engineering), Retinal, Anatomy, Fibroblasts, eye diseases, Posterior segment of eyeball, Vitreous Body, Ophthalmology, Disease Models, Animal, chemistry, Female, sense organs, Rabbits, business, Vitreous base, Sclera
Abstract

• A reproducible model of double perforating injury of the posterior segment of the rabbit eye was developed. Immediately after injury, a vitreous condensation was visible between wounds. The scleral exit wound was sealed by fibroblastic proliferation of probable episcleral origin by the fourth day and the entrance similarly by the seventh day. Cellular proliferations originating in the wounds crossed the vitreous cavity following the vitreous injury tract or condensed vitreous to the disc or to the vitreous base. The earliest intraocular proliferations, composed of spindle-shaped, fibroblast-like cells, were seen at day 4. Occasional pigment epithelia were present in and on these proliferations. Other proliferations occurred directly on the retinal surface adjacent to the wounds. The transvitreous proliferations employed the vitreous as a scaffold, while the surface proliferations used the retinal surface for contact guidance.

Published
1979

111. Anaerobic bacterial endophthalmitis

Author

Joan Haaf, Barbara G. Paton, Ann Sullivan Baker, Trexler M. Topping, and L. David Ormerod

Subjects
Adult, Male, medicine.medical_specialty, Adolescent, medicine.medical_treatment, Eye disease, Propionibacterium acnes, Bacteria, Anaerobic, Endophthalmitis, medicine, Humans, Child, Aged, Aged, 80 and over, biology, business.industry, Bacterial Infections, Cataract surgery, Middle Aged, medicine.disease, biology.organism_classification, Prognosis, eye diseases, Surgery, Ophthalmology, Female, Anaerobic bacteria, business, Anaerobic exercise, Uveitis, Penetrating trauma
Abstract

Eighteen patients with endophthalmitis involving anaerobic bacteria are presented. Endophthalmitis followed cataract surgery in seven patients, penetrating trauma in six, a corneal graft in two, and an infected filtering bleb in two; there was one case of endogenous endophthalmitis. Propionibacterium acnes was the most frequent anaerobe isolated (78% of cases). Thirty-two percent of the patients had polymicrobial infection with mixed aerobic and anaerobic species. Six cases of acute P. acnes endophthalmitis were clinically indistinguishable from other cases of mild to moderately severe endophthalmitis. Four patients presented, after cataract surgery, with chronic, low-grade endophthalmitis of 1 to 15 months' duration, emphasizing that "sterile" endophthalmitis cannot be satisfactorily diagnosed clinically. The visual prognosis of treated P. acnes endophthalmitis was often good. Based on principles of anaerobic microbiology, recommendations are made for vitreous collection, transport, and culture.

Published
1987

112. Vitrectomy for injury: the effect on intraocular proliferation following perforation of the posterior segment of the rabbit eye

Author

Robert Machemer, Gary W. Abrams, and Trexler M. Topping

Subjects
Male, medicine.medical_specialty, Time Factors, genetic structures, medicine.medical_treatment, Perforation (oil well), Vitrectomy, Wounds, Penetrating, Eye, Eye injuries, Eye Injuries, Ophthalmology, Medicine, Animals, Wound Healing, business.industry, medicine.disease, eye diseases, Surgery, Posterior segment of eyeball, Vitreous Body, Female, sense organs, Rabbits, business, Wound healing
Abstract

Perforating injuries were produced in the posterior segments of rabbit eyes. A control group had no surgery; a second group underwent closed vitrectomy immediately after injury; and a third group had closed vitrectomy delayed two weeks following injury. The eyes were then observed for four weeks. Transvitreal proliferation, which was found in each of the control eyes, was effectively prevented in the eyes that underwent immediate vitrectomy. Established transvitreal proliferation was removed and its recurrence prevented by delayed vitrectomy. These results establish the principle that vitreous acts as a scaffold for proliferation. Removal of the vitreous eliminates the structures along which proliferation can occur and thus effectively prevents transvitreal proliferation. Early removal of vitreous in severely injured eyes with vitreous damage is recommended.

Published
1979

124. Ophthalmology (Pocket Consultant)

Author

Trexler M. Topping

Subjects
Ophthalmology, medicine.medical_specialty, business.industry, medicine, Optometry, business
Published
1982

125. Xenon Endophotocoagulation Under Air Using Sodium Hyavluronate

Author

Trexler M. Topping and George A. Williams

Subjects
Xenon, Materials science, Air, Lasers, Sodium, Radiochemistry, Retinal Detachment, chemistry.chemical_element, Ophthalmology, chemistry, Humans, Laser Therapy, Hyaluronic Acid
Published
1984

127. An International Classification of Retinopathy of Prematurity

Author

Andrew Q. McCormick, Michael T. Trese, Alice R. McPherson, Graham E. Quinn, John T. Flynn, Alec Garner, Joseph E. Robertson, Thomas M. Aaberg, Robert Y. Foos, Akio Majima, Yasuhiko Tanaka, Trexler M. Topping, William Tasman, Fritz Koerner, Robert Machemer, Helge Paulmann, Steve Charles, John G. Clarkson, Isaac Ben-Sira, Ben Zane Cohen, and Tatsuo Hirose

Subjects
medicine.medical_specialty, End stages, business.industry, Retinal detachment, Retinal, Retinopathy of prematurity, Disease, medicine.disease, Ophthalmology, chemistry.chemical_compound, chemistry, Medicine, business
Abstract

The purpose of this article is to complete the classification of retinopathy of prematurity (ROP) begun with the publication of the recent article on the subject entitled, "An International Classification of Retinopathy of Prematurity" (ICROP). 1-3 The previously published classification embodied three major concepts for the description of the early phases of the disease: specifying its location by zones of retinal involvement; recording the extent of retinal involvement by clock hours; and, finally, staging the disease according to the degree of vascular lesions observed (stages 1 through 4). That article specified posterior dilatation and tortuosity of retinal vessels as ominous prognostic signs. The committee that authored it left unclassified the sequelae that encompass the cicatricial phase of the disease. It recommended the use of the Reese classification 4 until a more satisfactory one could be developed. The reasons for completing the classification of the end stages of ROP at this

Published
1987

128. Ultrastructural Ocular Pathology of Hunter's Syndrome

Author

Morton F. Goldberg, Kenneth R. Kenyon, A. Edward Maumenee, and Trexler M. Topping

Subjects
Adult, Male, congenital, hereditary, and neonatal diseases and abnormalities, Pathology, medicine.medical_specialty, Adolescent, Ocular Pathology, Hepatosplenomegaly, Iris, Autopsy, Eye, Retina, Cornea, Retinitis pigmentosa, medicine, Humans, Mucopolysaccharidosis type II, Child, skin and connective tissue diseases, Mucopolysaccharidosis II, Inclusion Bodies, S syndrome, Choroid, business.industry, Ciliary Body, Infant, Newborn, Infant, nutritional and metabolic diseases, medicine.disease, Microscopy, Electron, Ophthalmology, medicine.anatomical_structure, Child, Preschool, Histopathology, sense organs, medicine.symptom, business, Retinitis Pigmentosa, Sclera
Abstract

THE SYSTEMIC mucopolysaccharidoses (MPS) are of ophthalmologic interest because about 75% of patients with these inherited disorders of mucopolysaccharide metabolism develop clinically significant corneal clouding. 1 The histologic and ultrastructural pathologic condition of the clouded corneas from these patients has been the subject of many reports. 2-7 However, only one report 8 has described the ocular histopathology of a systemic MPS case with clear corneas, which occurred in a patient with Hunter's syndrome. Hunter's syndrome (systemic MPS type II), one of the six or more variants of the systemic MPS, 1 resembles the more common Hurler's syndrome (gargoylism, systemic MPS type I) in several respects. Clinically, Hunter's syndrome appears as a less severe form of Hurler's with respect to progressive growth and mental retardation, coarse gargoyle-like facies, multiple skeletal deformities, hepatosplenomegaly, and early death. Both syndromes are also characterized by the increased urinary excretion and excessive tissue accumulations of two

Published
1971

130. The Endophthalmitis Vitrectomy Study: Relationship Between Clinical Presentation and Microbioloaic Spectrum

Author

Vine, Andrew K., Blodi, Barbara A., Elner, Susan G., Johnson, Mark W., Jessup, Laurie M., Khanderia, Sharad, Pierson, Carl L., Willis, Julie, McIver, Frances, Stanley, Sally, Sneed, Scott R., Capone, Antonio, Jr., Aaberg, Thomas M., Lim, Jennifer I., Sternberg, Paul, Jr., Coffman, Diana S., Moore, Cameile N., Gardner, Susanne K., Nolte, Frederick S., Fremstad, Ann, Gibbs, Deborah, Gilman, James, Swords, Ray, Aguilar, H.Edith, Meredith, Travis A., Lakhanpal, Vinod, Christian, Faith D., Hood, A., Schwalbe, Richard S., Billings, Emery E., Buie, William, Jr., Mallonee, James J., Jr., Millar, Mary Ann, Verbeek, Sharon, Campochiaro, Peter A., Palardy, Carol B., Reynolds, Lois, Dick, James D., Cain, Dennis, D'Amico, Donald J., Frederick, Albert R., Jr., Morley, Michael G., Pesavento, Richard D., Puliafito, Carmen A., Topping, Trexler M., Finn, Susan M., Raymond, Laura A., Baker, Ann Sullivan, Paton, Barbara, Evans, Claudia, Napoli, Jeffrey, Kierman, Christine, Makris, Kathryn, McInnes, Tom, Reidy, Wini T., White, Ruth, Garfinkel, Richard A., Pilkerton, A.Raymond, Frantz, Robert A., Abernathy, Gill B., Barbaccia, Jay G., Ensey, H.Russell, Ormes, Carol A., Park, Choong H., Caplan, Joel, Russell, Kathryn, Toma, Robert, Packo, Kirk H., de Bustros, Serge, Flood, Timothy P., Glazer, Louis, DeAlba, Maggie, Evanich, Evangeline, Montwill, Michael A., Rothman, Jeri J., Ruderman, Gail, Beard, Melodie, Landau, William, Shen, Min H., Gordon, Martha, Graff, Sharon, Kwiatkowski, Kathy, Pappas, Loreen, Bryant, Douglas, Doherty, Don, Morini, Frank, Arredondo, Linda, Garretson, Bruce R., Gerena, Carlos, Hunt, Maureen, Kinnaird, Sharon M., Neri, Toni, Rice, Thomas A., Novak, Michael A., Rowe, Pamela S., Jamieson, Scott, Newberry, Deborah, Rech, Glenn R., Dul, Michael J., Kinser, Livia, Strozewski, Krystyna, Clark-Rath, Susan, DeLisio, Marty, Dempsey, David L., Kukula, Donna, Pinter-Smith, Anne, Smith-Brewer, Sheila, Ludwig, Tracey, Chambers, Robert B., Davidorf, Frederick H., Taylor, Cindy S., Hale, Karen N., Buesching, William J., Chaudhuri, Chhanda, Cover, Nanci J., Shortlidge, Gail R., Keating, Michael J., Savage, Scott J., Andrzejewska, Paula, Cometet, Susan, Milliron, Jill D., Richmond, Rob, Schneider, Lori, Weisenberger, Debra, Cantrill, Herbert L., Ramsay, Robert C., Brallier, Amy B., Johnson, Timothy P., Rossing, Edith E., Knauth, Kathleen A., Monahan, Martha M., Oestreich, Neal W., Clark, Kenneth F., Glennen, Anita M., Yarian, David L., Green, Stuart N., Leff, Steven R., Masciulli, Leo, Lucido, Margaret M., Ludwig, Edward J., Marano, Charlotte L., Peters, Linda, Joho, Kim, Volkert, Doris C., Andersen, Finn, Coffey, Donna, Schlosser, Alex, Honeywell, Ann, Mames, Robert N., Driebe, William T., Jr., Stern, George A., Francis, Amye, Zam, Z.Suzanne, Cooper, Rhonda, Gaskins, Darla, Shamis, Diana J., Willingham, Melinda, Barker, Kay, Rosa, Harry, Friedman, Scott M., Gardner, Thomas W., Blankenship, George W., Coyle, Carole J., Bero, Christopher J., Halas, Cindy, Schick, Suzanne, Walker, Jean, Cunningham, Denise, Lambert, H.Michael, Clogston, Pamela S., Frady, Pamela M., Gardner, S.Neal, Osato, Michael S., Carr, Louise, Shigley, James, Lopez, Pedro F., Chong, Lawrence P., Frambach, Donald A., CisnerosMargaret^Padilla, Lupe, Yee, Edmond Ming, Nakamura, Tamako, Walonker, A.Frances, Morales, Ronald, Nichols, Tracy, Huete, Maria E., Liggett, Peter E., Ober, Richard R., Quillen-Thomas, Beth, Williams, Mark, Barr, Charles C., Bloom, Steven M., Greene, Pamela J., Whittington, Greg K., Martin, Mark E., Watson, Glen, Jenkins-Curry, Betty, Gilkey, Leigh A., Huelsman, Steven, Han, Dennis P., Burton, Thomas C., Mieler, William F., Pulido, Jose S., Reeser, Frederick H., Newman, Janet L., Werner, Kathy A., Pisarzewicz, Paul J., Reinerio, Nina A., Walloch, Mary Lee K., Wilmer, Zuzana, Laabs, Jan, Picchiottino, Ruth, Phillips, Jim, Wipplinger, Walter, Abrams, Gary W., Jurkiewicz, Dale T., Leet, Margaret L., Mandel, Paul, Metzger, Kim, Suchla, Lori, Zarling, Denise, Balles, Mark W., Ryan, Edwin H., Jr., Knobloch, William H., Cook, Sally M., Luke, Darlette G., Ferrieri, Patricia, Schiminsky, Norynne M., Genia, Anne, Philiph, David A., Stinson, Elizabeth K., Wright, Linda M., McMichael, William C., Mielke, Sandy J., Ponwith, Lisa J., Pavan, Peter Reed, Pautler, Scott E., Coats, Marion L., Kirk, Nancy M., Millard, Sharon M., Castellano, Frank C., Edwards, Charlotte R., Marquardt, Angela, McCormack, Amy J., McCormick, Michael T., Renshaw, Bernard, Restuccia, Angela, Campbell, Monica, Christopher, Nell, Garrett, L.Scott, Halkias, Demetrios G., Hothersall, Kim, Mickler, Karen, Minnick, Thomas S., Burr, Cheryl, Saxon, Wyatt, Arcacha, Miguel A., Jr., Carlton, Steve, Edison, Sonya K., Mallis, Marc J., Sayers, Tamre L., Sudds, Thomas W., Tiberia, Robert J., Wolabaugh, Sherry, Bradford, Reagan H., Jr., Parke, David W., II, Wolf, Thomas C., Shofner, Janie M., Tobey, Lee E., Jensen, Harold G., Sanchez, Dinah, Shofner, Janie, Burris, Russell, Drake, Kellie K., Grissom, Kay R., Rowsey, J.James, Wilkinson, Charles P., Brown, Gary C., Benson, William E., Federman, Jay L., Lucier, Alfred C., Maguire, Joseph I., Sarin, Lov K., Shakin, Eric P., Sivalingam, Arunan, Tasman, William, Vander, James F., Ward, Nancy, Weisbecker, Clement A., Agnew, Caroline L., Lambert, Richard, Torner, Terrance, Carlson, Kathy, Franchine, Gerrie, Serfass, Michelle S., Doft, Bernard H., Bergren, Robert L., Lobes, Louis A., Jr., Olsen, Karl R., Rinkoff, Jeffrey S., Metz, Donna J., Leonard, Margaret N., Karenchak, Lisa M., Kowalski, Regis P., Wellman, Lynn A., Wilcox, Linda A., Campbell, Alan F., Steinberg, David R., Vagstad, Gary L., Flook, Kimberly A., Good, Mary M., Keenen, Beverly J., Mellinger, Kim A., Margherio, Raymond R., Cox, Morton S., Jr., Murphy, Patrick L., Trese, Michael T., Werner, Jane C., Williams, George A., Manatrey, Patricia E., Prote, Janet L., Lucarotti, Richard, Martin, Susan, Band, Jeff, Bostic, Grace, Gumming, Kristi, Mitchell, Beth, Regan, Virginia S., Bridges, Craig, Cox, Sam, Houston, Gary, Johnson, John, Streasik, Pat, Wood, Betty, Blumenkranz, Mark S., Cayo, Lisa, Kaye, Virginia, Valenzuela, Carmen Luz, Orgel, Ira K., Poliner, Lon S., Tornambe, Paul E., Cannon, Sarah V., Nielsen, Janet L., Carlson, Anne, Chan, Pauline, Drake, Lynne, Grim, Martha, Peterson, Corky, Borg, Lynn A., Gillyatt, Joann, Beyer, Conny, Hammer, Mark E., Grizzard, W.Sanderson, Shannon, Theresa L., Traynom, Janet R., Collado, Melinda J., McManus, Dennis W., Sweeney, Daniel E., Adams, Donald H., Jr., Watson, Thomas T., Antworth, Michael V., Araos, Johanna Glacy, Greenwald, Mark A., Habib, Mohsen, Myers, Sandra K., Ockers, Karen M., Thibodeau, Judy-Ann, Watkins, Brett, Nelsen, Philip T., Rosenthal, J.Gregory, Mintz, Fay V., Biedenbach, Michael, Leonardy, Nicholas J., Lawniczak, Sue M., Bork, Chuck, Hageage, George, Hunter, Evelyn B., Marshall, MarLynn J., Roman, Patricia, Hill, Rick, Hofbauer, Thomas, Lemanowicz, Jack, Cupples, Howard P., Guzman, Gladys I., Brodeur, Richard J., Yee, Donald, Delaha, Edward C., Geyer, Stanley L., Slovis, Stacey, Shields, William J., Lauber, Susan, Michelitsch, Karl, Barza, Michael, Kassoff, Aaron, Watling, Sharon, Wilson, Louis A., Buehler, JoAnne C., McVay, Jeffrey, Kelsey, Sheryl F., Wisniewski, Stephen R., Podobinski, Gale K., Sillett, Robert L., Groer, Shirley, Avery, Brian, Belle, Steven H., Boles, James, Henry, Linda, Shema, Sarah J., Titus-Emstoff, Linda, Davis, Matthew, Magli, Yvonne L., Hubbard, Larry, Thomas, Suzanne, Everett, Donald F., Mowery, Richard, Everett, Donald, Davis, Kathryn, Azen, Stanley, Covey, Preston, McCuen, Brooks, Packer, Andrew, and Robin, Jeffrey

Published
1997
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132. The 1997 Kyoto Protocol: what does it mean for project-based climatechange mitigation

Author

Trexler, M. C. and Kosloff, L. H.

Subjects
CLIMATE change
Abstract

The Kyoto Protocol effectively ends the Activities Implemented Jointly (AIJ) pilot phase. However, it is premature to conclude that Articles 6 and 12 of the Protocol vindicate joint implementation and successfully conclude the AIJ pilot phase. Rather, Articles 6 and 12 can be seen as part of the price developing countries felt they had to payto obtain a Protocol. Debate over Articles 6 and 12 is likely to be as contentious as the JI/AIJ debates that preceded it. Indeed, the AIJ pilot phase has not answered many concerns posed by developing countries and other interest groups. While companies and countries participating in AIJ have had wide latitude to pursue almost any projects they wished, it remains to be seen how much of this flexibility will be preserved as Articles 6 and 12 become operational. This will determine whether the importance and cost-effectiveness originally predicted for the joint implementation concept comes to pass. A review of theJI and AIJ literature suggests many potential stumbling blocks to achieving large-scale and cost-effective emissions reductions through project-based mitigation efforts under the Kyoto Protocol. This paper identifies these stumbling blocks and systematically assesses their potential implications. The Greenhouse Gas Offset Cost Assessment and Decisionmaking Model (GGOCADc) is used to qualitatively as well as quantitatively evaluate the importance of key criteria and methodological decisions under Articles 6 and 12. It is easy to develop scenariosin which project-based mitigation through Articles 6 and 12 would not be permitted to contribute substantially to achievement of countries` obligations under Article 3. Overcoming the challenges facing project-based mitigation efforts is important to achieving the larger goals of the Kyoto Protocol. [ABSTRACT FROM AUTHOR]

Published
1998
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133. Posterior Retinal Folds Following Vitreoretinal Surgery-Reply

Author

Larrison, Wayne I., Frederick, Albert R., Topping, Trexler M., and Peterson, Timothy

Abstract

IN REPLY We appreciate the comments and suggestions of Avins et al with regard to avoiding retinal fold formation. Their recommendations regarding complete transvitreal drainage of SRF rather than transscleral drainage and the benefit of early prone positioning echo the sentiments discussed in our report. With the recognition of the benefits of posterior retinotomy and "complete" drainage, we have, for all intents and purposes, abandoned the transscleral drainage approach. We have never attempted the technique Avins et al describe of scleral depression to drive fluid into the vitreous after partial fluid gas exchange in eyes drained internally. The use of a posterior retinotomy makes these types of complicated maneuvers unnecessary.We believe the benefit of early prone positioning comes from the fact that the border of previously detached/attached retina is not below (dependent) the bubble meniscus. As discussed in our report, we believe it is the dependent movement of residual

Published
1994
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137. Improving Timely Administration of Essential Outpatient Medications in a Pediatric ED.

Author

Creedon JK, Marini M, Erdner K, Trexler M, Gerling M, Porter JJ, Kent C, Capraro A, Volpe D, Shah D, Paydar-Darian N, Perron C, Stack A, and Hudgins JD

Subjects
Humans, Child, Length of Stay, Medication Errors prevention & control, Medication Errors statistics & numerical data, Ambulatory Care, Electronic Health Records, Outpatients, Anticonvulsants administration & dosage, Anticonvulsants therapeutic use, Emergency Service, Hospital, Quality Improvement
Abstract

Background and Objectives: The complexity of pediatric patients' outpatient medication regimens is increasing, and risk for medication errors is compounded in a busy emergency department (ED). As ED length of stay (LOS) increases, timely and accurate administration of essential outpatient medications has become increasingly challenging. Our objective was to increase the frequency of ordering of essential outpatient medications for patients with ED LOS >4 hours from 56% to 80% by June 2023., Methods: We conducted a quality improvement (QI) initiative in a pediatric ED with ∼60 000 annual visits comprising a total of 91 000 annual medication orders. We defined essential outpatient medications as antiepileptic drugs, cardiovascular medications, and immunosuppressants. Our QI interventions included a combination of electronic health record interventions, a triage notification system to identify patients with essential outpatient medications, and widespread educational interventions including trainee orientation and individualized nursing education. The primary outcome measure was percentage of essential outpatient medications ordered among patients with an ED LOS >4 hours, with a secondary measure of outpatient medication safety events., Results: Baseline monthly ordering rate of selected medications for patients with an ED LOS >4 hours was 54%, with an increase to 66% over the study period. Refining our population yielded a rate of 81%. Outpatient medication safety events remained unchanged, with an average of 952 ED encounters between events., Conclusions: A multidisciplinary QI initiative led to increased essential outpatient medication ordering for patients in a pediatric ED with no change in safety events., (Copyright © 2024 by the American Academy of Pediatrics.)

Published
2024
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138. Arginines of the CGN codon family are Achilles' heels of cancer genes.

Author

Trexler M, Bányai L, Kerekes K, and Patthy L

Subjects
Humans, Mutation, Oncogenes genetics, Genes, Tumor Suppressor, Arginine genetics, Arginine chemistry, Codon genetics, Neoplasms genetics, CpG Islands genetics
Abstract

Recent studies have revealed that arginine is the most favorable target of amino acid alteration in most cancer types and it has been suggested that the high preference for arginine mutations reflects the critical roles of this amino acid in the function of proteins. High rates of mutations of arginine residues in cancer, however, might also be due to increased mutability of arginine codons of the CGN family as the CpG dinucleotides of these codons may be methylated. In the present work we have analyzed spectra of single base substitutions of cancer genes (oncogenes, tumor suppressor genes) and passenger genes in cancer tissues to assess the contributions of CpG hypermutability and selection to arginine mutations. Our studies have shown that arginines encoded by the CGN codon family display higher rates of mutation in both cancer genes and passenger genes than arginine codons AGA and AGG that are devoid of CpG dinucleotide, suggesting that the predominance of arginine mutations in cancer is primarily due to CpG hypermutability, rather than selection for arginine replacement. Nevertheless, our results also suggest that CGN codons for arginines may serve as Achilles' heels of cancer genes. CpG hypermutability of key arginines of proto-oncogenes, leading to high rates of recurrence of driver mutations, contributes significantly to carcinogenesis. Similarly, our results indicate that hypermutability of the CpG dinucleotide of CGA codons (converting them to TGA stop codons) contributes significantly to recurrent truncation and inactivation of tumor suppressor genes., (© 2024. The Author(s).)

Published
2024
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139. Evolution of termination codons of proteins and the TAG-TGA paradox.

Author

Trexler M, Bányai L, Kerekes K, and Patthy L

Subjects
Humans, Codon, Terminator genetics, Eukaryota, Mutation, Codon, Nonsense genetics, Magnoliopsida
Abstract

In most eukaryotes and prokaryotes TGA is used at a significantly higher frequency than TAG as termination codon of protein-coding genes. Although this phenomenon has been recognized several years ago, there is no generally accepted explanation for the TAG-TGA paradox. Our analyses of human mutation data revealed that out of the eighteen sense codons that can give rise to a nonsense codon by single base substitution, the CGA codon is exceptional: it gives rise to the TGA stop codon at an order of magnitude higher rate than the other codons. Here we propose that the TAG-TGA paradox is due to methylation and hypermutabilty of CpG dinucleotides. In harmony with this explanation, we show that the coding genomes of organisms with strong CpG methylation have a significant bias for TGA whereas those from organisms that lack CpG methylation use TGA and TAG termination codons with similar probability., (© 2023. Springer Nature Limited.)

Published
2023
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140. Use of Publication Dynamics to Distinguish Cancer Genes and Bystander Genes.

Author

Bányai L, Trexler M, and Patthy L

Subjects
Humans, PubMed, Genes, Neoplasm, Neoplasms genetics
Abstract

de Magalhães has shown recently that most human genes have several papers in PubMed mentioning cancer, leading the author to suggest that every gene is associated with cancer, a conclusion that contradicts the widely held view that cancer is driven by a limited number of cancer genes, whereas the majority of genes are just bystanders in carcinogenesis. We have analyzed PubMed to decide whether publication metrics supports the distinction of bystander genes and cancer genes. The dynamics of publications on known cancer genes followed a similar pattern: seminal discoveries triggered a burst of cancer-related publications that validated and expanded the discovery, resulting in a rise both in the number and proportion of cancer-related publications on that gene. The dynamics of publications on bystander genes was markedly different. Although there is a slow but continuous time-dependent rise in the proportion of papers mentioning cancer, this phenomenon just reflects the increasing publication bias that favors cancer research. Despite this bias, the proportion of cancer papers on bystander genes remains low. Here, we show that the distinctive publication dynamics of cancer genes and bystander genes may be used for the identification of cancer genes.

Published
2022
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141. Wnt Inhibitory Factor 1 Binds to and Inhibits the Activity of Sonic Hedgehog.

Author

Kerekes K, Trexler M, Bányai L, and Patthy L

Subjects
Animals, Cell Line, Hedgehog Proteins metabolism, Humans, Immobilized Proteins metabolism, Kinetics, Mice, NIH 3T3 Cells, Protein Binding, Signal Transduction, Adaptor Proteins, Signal Transducing metabolism, Hedgehog Proteins antagonists & inhibitors
Abstract

The hedgehog (Hh) and Wnt pathways, crucial for the embryonic development and stem cell proliferation of Metazoa, have long been known to have similarities that argue for their common evolutionary origin. A surprising additional similarity of the two pathways came with the discovery that WIF1 proteins are involved in the regulation of both the Wnt and Hh pathways. Originally, WIF1 (Wnt Inhibitory Factor 1) was identified as a Wnt antagonist of vertebrates, but subsequent studies have shown that in Drosophila , the WIF1 ortholog serves primarily to control the distribution of Hh. In the present, work we have characterized the interaction of the human WIF1 protein with human sonic hedgehog (Shh) using Surface Plasmon Resonance spectroscopy and reporter assays monitoring the signaling activity of human Shh. Our studies have shown that human WIF1 protein binds human Shh with high affinity and inhibits its signaling activity efficiently. Our observation that the human WIF1 protein is a potent antagonist of human Shh suggests that the known tumor suppressor activity of WIF1 may not be ascribed only to its role as a Wnt inhibitor.

Published
2021
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142. Avidin-biotin complex-based capture coating platform for universal Influenza virus immobilization and characterization.

Author

Trexler M, Brusatori M, and Auner G

Subjects
Binding Sites, Fluorescein-5-isothiocyanate chemistry, Hemagglutinin Glycoproteins, Influenza Virus chemistry, Hemagglutinin Glycoproteins, Influenza Virus metabolism, Humans, Microscopy, Atomic Force, N-Acetylneuraminic Acid chemistry, Orthomyxoviridae metabolism, Avidin chemistry, Biotin chemistry, Influenza, Human diagnosis, N-Acetylneuraminic Acid pharmacology, Orthomyxoviridae isolation & purification
Abstract

Influenza virus mutates quickly and unpredictably creating emerging pathogenic strains that are difficult to detect, diagnose, and characterize. Conventional tools to study and characterize virus, such as next generation sequencing, genome amplification (RT-PCR), and serological antibody testing, are not adequately suited to rapidly mutating pathogens like Influenza virus where the success of infection heavily depends on the phenotypic expression of surface glycoproteins. Bridging the gap between genome and pathogenic expression remains a challenge. Using sialic acid as a universal Influenza virus binding receptor, a novel virus avidin-biotin complex-based capture coating was developed and characterized that may be used to create future diagnostic and interrogation platforms for viable whole Influenza virus. First, fluorescent FITC probe studies were used to optimize coating component concentrations. Then atomic force microscopy (AFM) was used to profile the surface characteristics of the novel capture coating, acquire topographical imaging of Influenza particles immobilized by the coating, and calculate the capture efficiency of the coating (over 90%) for all four representative human Influenza virus strains tested., Competing Interests: The authors have declared that no competing interests exist.

Published
2021
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143. Use of signals of positive and negative selection to distinguish cancer genes and passenger genes.

Author

Bányai L, Trexler M, Kerekes K, Csuka O, and Patthy L

Subjects
Humans, Mutation, Neoplasms genetics, Selection, Genetic
Abstract

A major goal of cancer genomics is to identify all genes that play critical roles in carcinogenesis. Most approaches focused on genes positively selected for mutations that drive carcinogenesis and neglected the role of negative selection. Some studies have actually concluded that negative selection has no role in cancer evolution. We have re-examined the role of negative selection in tumor evolution through the analysis of the patterns of somatic mutations affecting the coding sequences of human genes. Our analyses have confirmed that tumor suppressor genes are positively selected for inactivating mutations, oncogenes, however, were found to display signals of both negative selection for inactivating mutations and positive selection for activating mutations. Significantly, we have identified numerous human genes that show signs of strong negative selection during tumor evolution, suggesting that their functional integrity is essential for the growth and survival of tumor cells., Competing Interests: LB, MT, KK, OC, LP No competing interests declared, (© 2021, Bányai et al.)

Published
2021
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144. High-performance chemical- and light-inducible recombinases in mammalian cells and mice.

Author

Weinberg BH, Cho JH, Agarwal Y, Pham NTH, Caraballo LD, Walkosz M, Ortega C, Trexler M, Tague N, Law B, Benman WKJ, Letendre J, Beal J, and Wong WW

Subjects
Animals, DNA Nucleotidyltransferases, Gene Regulatory Networks, HEK293 Cells, Humans, Integrases, Mice, Recombinases metabolism, Cold Temperature, DNA metabolism, Genetic Engineering methods, Light, Recombinases genetics
Abstract

Site-specific DNA recombinases are important genome engineering tools. Chemical- and light-inducible recombinases, in particular, enable spatiotemporal control of gene expression. However, inducible recombinases are scarce due to the challenge of engineering high performance systems, thus constraining the sophistication of genetic circuits and animal models that can be created. Here we present a library of >20 orthogonal inducible split recombinases that can be activated by small molecules, light and temperature in mammalian cells and mice. Furthermore, we engineer inducible split Cre systems with better performance than existing systems. Using our orthogonal inducible recombinases, we create a genetic switchboard that can independently regulate the expression of 3 different cytokines in the same cell, a tripartite inducible Flp, and a 4-input AND gate. We quantitatively characterize the inducible recombinases for benchmarking their performances, including computation of distinguishability of outputs. This library expands capabilities for multiplexed mammalian gene expression control.

Published
2019
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145. Analysis of Tks4 Knockout Mice Suggests a Role for Tks4 in Adipose Tissue Homeostasis in the Context of Beigeing.

Author

Vas V, Háhner T, Kudlik G, Ernszt D, Kvell K, Kuti D, Kovács KJ, Tóvári J, Trexler M, Merő BL, Szeder B, Koprivanacz K, and Buday L

Subjects
Adaptor Proteins, Signal Transducing genetics, Adipocytes, Beige cytology, Adipocytes, White cytology, Adipocytes, White metabolism, Adipogenesis, Animals, Cells, Cultured, Mice, Mice, Inbred C57BL, PPAR gamma genetics, PPAR gamma metabolism, Uncoupling Protein 1 genetics, Uncoupling Protein 1 metabolism, Adaptor Proteins, Signal Transducing metabolism, Adipocytes, Beige metabolism, Homeostasis
Abstract

Obesity and adipocyte malfunction are related to and arise as consequences of disturbances in signaling pathways. Tyrosine kinase substrate with four Src homology 3 domains (Tks4) is a scaffold protein that establishes a platform for signaling cascade molecules during podosome formation and epidermal growth factor receptor (EGFR) signaling. Several lines of evidence have also suggested that Tks4 has a role in adipocyte biology; however, its roles in the various types of adipocytes at the cellular level and in transcriptional regulation have not been studied. Therefore, we hypothesized that Tks4 functions as an organizing molecule in signaling networks that regulate adipocyte homeostasis. Our aims were to study the white and brown adipose depots of Tks4 knockout (KO) mice using immunohistology and western blotting and to analyze gene expression changes regulated by the white, brown, and beige adipocyte-related transcription factors via a PCR array. Based on morphological differences in the Tks4-KO adipocytes and increased uncoupling protein 1 (UCP1) expression in the white adipose tissue (WAT) of Tks4-KO mice, we concluded that the beigeing process was more robust in the WAT of Tks4-KO mice compared to the wild-type animals. Furthermore, in the Tks4-KO WAT, the expression profile of peroxisome proliferator-activated receptor gamma (PPARγ)-regulated adipogenesis-related genes was shifted in favor of the appearance of beige-like cells. These results suggest that Tks4 and its downstream signaling partners are novel regulators of adipocyte functions and PPARγ-directed white to beige adipose tissue conversion.

Published
2019
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146. Structure, function and disease relevance of Wnt inhibitory factor 1, a secreted protein controlling the Wnt and hedgehog pathways.

Author

Kerekes K, Bányai L, Trexler M, and Patthy L

Subjects
Adaptor Proteins, Signal Transducing chemistry, Adaptor Proteins, Signal Transducing genetics, Animals, Evolution, Molecular, Hedgehog Proteins genetics, Humans, Wnt Proteins genetics, Adaptor Proteins, Signal Transducing metabolism, Carcinogenesis genetics, Hedgehog Proteins metabolism, Wnt Proteins metabolism
Abstract

Wnts and Hedgehogs (Hh) are large, lipid-modified extracellular morphogens that play key roles in embryonic development and stem cell proliferation of Metazoa. Both morphogens signal through heptahelical Frizzled-type receptors of the G-Protein Coupled Receptor family and there are several other similarities that suggest a common evolutionary origin of the Hh and Wnt pathways. There is evidence that the secreted protein, Wnt inhibitory factor 1 (WIF1) modulates the activity of both Wnts and Hhs and may thus contribute to the intertwining of these pathways. In this article, we review the structure, evolution, molecular interactions and functions of WIF1 with major emphasis on its role in carcinogenesis.

Published
2019
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147. Applications of Raman spectroscopy in cancer diagnosis.

Author

Auner GW, Koya SK, Huang C, Broadbent B, Trexler M, Auner Z, Elias A, Mehne KC, and Brusatori MA

Subjects
Animals, Humans, Neoplasms pathology, Neoplastic Cells, Circulating pathology, Quantum Theory, Neoplasms diagnosis, Spectrum Analysis, Raman methods
Abstract

Novel approaches toward understanding the evolution of disease can lead to the discovery of biomarkers that will enable better management of disease progression and improve prognostic evaluation. Raman spectroscopy is a promising investigative and diagnostic tool that can assist in uncovering the molecular basis of disease and provide objective, quantifiable molecular information for diagnosis and treatment evaluation. This technique probes molecular vibrations/rotations associated with chemical bonds in a sample to obtain information on molecular structure, composition, and intermolecular interactions. Raman scattering occurs when light interacts with a molecular vibration/rotation and a change in polarizability takes place during molecular motion. This results in light being scattered at an optical frequency shifted (up or down) from the incident light. By monitoring the intensity profile of the inelastically scattered light as a function of frequency, the unique spectroscopic fingerprint of a tissue sample is obtained. Since each sample has a unique composition, the spectroscopic profile arising from Raman-active functional groups of nucleic acids, proteins, lipids, and carbohydrates allows for the evaluation, characterization, and discrimination of tissue type. This review provides an overview of the theory of Raman spectroscopy, instrumentation used for measurement, and variation of Raman spectroscopic techniques for clinical applications in cancer, including detection of brain, ovarian, breast, prostate, and pancreatic cancers and circulating tumor cells.

Published
2018
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148. Morphological Stasis and Proteome Innovation in Cephalochordates.

Author

Bányai L, Kerekes K, Trexler M, and Patthy L

Abstract

Lancelets, extant representatives of basal chordates, are prototypic examples of evolutionary stasis; they preserved a morphology and body-plan most similar to the fossil chordates from the early Cambrian. Such a low level of morphological evolution is in harmony with a low rate of amino acid substitution; cephalochordate proteins were shown to evolve slower than those of the slowest evolving vertebrate, the elephant shark. Surprisingly, a study comparing the predicted proteomes of Chinese amphioxus, Branchiostoma belcheri and the Florida amphioxus, Branchiostoma floridae has led to the conclusion that the rate of creation of novel domain combinations is orders of magnitude greater in lancelets than in any other Metazoa, a finding that contradicts the notion that high rates of protein innovation are usually associated with major evolutionary innovations. Our earlier studies on a representative sample of proteins have provided evidence suggesting that the differences in the domain architectures of predicted proteins of these two lancelet species reflect annotation errors, rather than true innovations. In the present work, we have extended these studies to include a larger sample of genes and two additional lancelet species, Asymmetron lucayanum and Branchiostoma lanceolatum. These analyses have confirmed that the domain architecture differences of orthologous proteins of the four lancelet species are because of errors of gene prediction, the error rate in the given species being inversely related to the quality of the transcriptome dataset that was used to aid gene prediction., Competing Interests: The authors declare no conflict of interest. The founding sponsors had no role in the design of the study; in the collection, analyses, or interpretation of data; in the writing of the manuscript, and in the decision to publish the results.

Published
2018
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149. Influence of WFIKKN1 on BMP1-mediated activation of latent myostatin.

Author

Szláma G, Vásárhelyi V, Trexler M, and Patthy L

Subjects
Animals, Binding Sites genetics, Bone Morphogenetic Protein 1 genetics, Carrier Proteins genetics, Cell Line, Furin metabolism, Heparin metabolism, Humans, Models, Molecular, Mutation, Myostatin chemistry, Myostatin genetics, Protein Binding, Protein Domains, Protein Multimerization, Protein Precursors chemistry, Protein Precursors genetics, Protein Precursors metabolism, Recombinant Proteins chemistry, Bone Morphogenetic Protein 1 metabolism, Carrier Proteins metabolism, Myostatin metabolism, Recombinant Proteins metabolism
Abstract

The NTR domain of WFIKKN1 protein has been shown to have significant affinity for the prodomain regions of promyostatin and latent myostatin but the biological significance of these interactions remained unclear. In view of its role as a myostatin antagonist, we tested the assumption that WFIKKN1 inhibits the release of myostatin from promyostatin and/or latent myostatin. WFIKKN1 was found to have no effect on processing of promyostatin by furin, the rate of cleavage of latent myostatin by BMP1, however, was significantly enhanced in the presence of WFIKKN1 and this enhancer activity was superstimulated by heparin. Unexpectedly, WFIKKN1 was also cleaved by BMP1 and our studies have shown that the KKN1 fragment generated by BMP1-cleavage of WFIKKN1 contributes most significantly to the observed enhancer activity. Analysis of a pro-TGF-β -based homology model of homodimeric latent myostatin revealed that the BMP1-cleavage sites are buried and not readily accessible to BMP1. In view of this observation, the most plausible explanation for the BMP1-enhancer activity of the KKN1 fragment is that it shifts a conformational equilibrium of latent myostatin from the closed circular structure of the homodimer to a more open form, making the cleavage sites more accessible to BMP1. On the other hand, the observation that the enhancer activity of KKN1 is superstimulated in the presence of heparin is explained by the fact KKN1, latent myostatin, and BMP1 have affinity for heparin and these interactions with heparin increase the local concentrations of the reactants thereby facilitating the action of BMP1., Enzymes: Furin: EC 3.4.21.75; BMP1, bone morphogentic protein 1 or procollagen C-endopeptidase: EC 3.4.24.19., (© 2016 The Authors. The FEBS Journal published by John Wiley & Sons Ltd on behalf of Federation of European Biochemical Societies.)

Published
2016
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150. Influence of collagen source on fibrillar architecture and properties of vitrified collagen membranes.

Author

Majumdar S, Guo Q, Garza-Madrid M, Calderon-Colon X, Duan D, Carbajal P, Schein O, Trexler M, and Elisseeff J

Subjects
Animals, Cattle, Dermis chemistry, Humans, Recombinant Proteins chemistry, Collagen chemistry, Membranes, Artificial, Vitrification
Abstract

Collagen vitrigel membranes are transparent biomaterials characterized by a densely organized, fibrillar nanostructure that show promise in the treatment of corneal injury and disease. In this study, the influence of different type I collagen sources and processing techniques, including acid-solubilized collagen from bovine dermis (Bov), pepsin-solubilized collagen from human fibroblast cell culture (HuCC), and ficin-solubilized collagen from recombinant human collagen expressed in tobacco leaves (rH), on the properties of the vitrigel membranes was evaluated. Postvitrification carbodiimide crosslinking (CX) was also carried out on the vitrigels from each collagen source, forming crosslinked counterparts BovXL, HuCCXL, and rHXL, respectively. Collagen membrane ultrastructure and biomaterial properties were found to rely heavily on both collagen source and crosslinking. Bov and HuCC samples showed a random fibrillar organization of collagen, whereas rH vitrigels showed remarkable regional fibril alignment. After CX, light transmission was enhanced in all groups. Denaturation temperatures after CX increased in all membranes, of which the highest increase was seen in rH (14.71°C), suggesting improved thermal stability of the collagen fibrils in the membranes. Noncrosslinked rH vitrigels may be reinforced through CX to reach levels of mechanical strength and thermal stability comparable to Bov., (© 2015 Wiley Periodicals, Inc.)

Published
2016
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