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1. Androgen and estrogen receptor expression in the developing human penis and clitoris.

Author

Baskin, Laurence, Cao, Mei, Sinclair, Adriane, Li, Yi, Overland, Maya, Isaacson, Dylan, and Cunha, Gerald

Subjects
Androgen receptor, Estrogen receptors alpha and beta, Human fetal penile and clitoral development, Hypospadias, Clitoris, Female, Humans, Male, Microscopy, Electron, Scanning, Morphogenesis, Penis, Receptors, Androgen, Receptors, Estrogen
Abstract

To better understand how the human fetal penis and clitoris grows and remodels, we undertook an investigation to define active areas of cellular proliferation and programmed cell death spatially and temporally during development of human fetal external genitalia from the indifferent stage (8 weeks) to 18 weeks of gestation. Fifty normal human fetal penile and clitoral specimens were examined using macroscopic imaging, scanning electron microscopy and immunohistochemical localization for the cellular proliferation and apoptotic markers, Ki67 and Caspase-3. A number of hot spots of cellular proliferation characterized by Ki67 localization are present in the penis and clitoris especially early in development, most notably in the corporal body, glans, remodeling glanular urethra, the urethral plate, the roof of the urethral groove and the fully formed penile urethra. The 12-fold increase in penile length over 10 weeks of growth from 8 to 18 weeks of gestation based on Ki67 labelling appears to be driven by cellular proliferation in the corporal body and glans. Throughout all ages in both the developing penis and clitoris Ki67 labeling was consistently elevated in the ventral epidermis and ventral mesenchyme relative to the dorsal counterparts. This finding is consistent with the intense morphogenetic activity/remodeling in the ventral half of the genital tubercle in both sexes involving formation of the urethral/vestibular plates, canalization of the urethral/vestibular plates and fusion of the urethral folds to form the penile urethra. Areas of reduced or absent Ki67 staining include the urethral fold epithelium that fuses to form the penile tubular urethra. In contrast, the urethral fold mesenchyme is positive for Ki67. Apoptosis was rarely noted in the developing penis and clitoris; the only area of minimal Caspase-3 localization was in the epithelium of the ventral epithelial glanular channel remodeling.

Published
2020

2. Imaging the developing human external and internal urogenital organs with light sheet fluorescence microscopy.

Author

Isaacson, Dylan, McCreedy, Dylan, Calvert, Meredith, Shen, Joel, Sinclair, Adriane, Cao, Mei, Li, Yi, McDevitt, Todd, Cunha, Gerald, and Baskin, Laurence

Subjects
Urogenital System, Humans, Imaging, Three-Dimensional, Microscopy, Fluorescence, Specimen Handling, Image Processing, Computer-Assisted, CLARITY, Genital development, Light sheet fluorescence microscopy, Microscopy, Selective plane illumination microscopy, Urogenital development, Urologic Diseases, Pediatric, Biochemistry and Cell Biology, Paediatrics and Reproductive Medicine, Developmental Biology
Abstract

Technological advances in three-dimensional (3D) reconstruction techniques have previously enabled paradigm shifts in our understanding of human embryonic and fetal development. Light sheet fluorescence microscopy (LSFM) is a recently-developed technique that uses thin planes of light to optically section whole-mount cleared and immunolabeled biologic specimens. The advent of commercially-available light sheet microscopes has facilitated a new generation of research into protein localization and tissue dynamics at extremely high resolution. Our group has applied LSFM to study developing human fetal external genitalia, internal genitalia and kidneys. This review describes LSFM and presents our group's technique for preparing, clearing, immunostaining and imaging human fetal urogenital specimens. We then present light sheet images and videos of each element of the developing human urogenital system. To the extent of our knowledge, the work conducted by our laboratory represents the first description of a method for performing LSFM on the full human urogenital system during the embryonic and fetal periods.

Published
2020

3. Computed Tomography Radiation Exposure Among Referred Kidney Stone Patients: Results from the Registry for Stones of the Kidney and Ureter.

Author

Tzou, David T, Zetumer, Samuel, Usawachintachit, Manint, Taguchi, Kazumi, Bechis, Seth K, Duty, Brian D, Harper, Jonathan D, Hsi, Ryan S, Sorensen, Mathew, Sur, Roger L, Reliford-Titus, Shalonda, Chang, Helena C, Isaacson, Dylan, Bayne, David B, Wang, Zhen J, Stoller, Marshall L, and Chi, Thomas

Subjects
Abdomen, Humans, Kidney Calculi, Ureteral Calculi, Radiation Injuries, Tomography, X-Ray Computed, Registries, Radiation Dosage, Adult, Aged, Middle Aged, Referral and Consultation, Female, Male, Radiation Exposure, CT, effective dose, ionizing radiation, kidney stones, low-dose CT, radiation dose limit, Kidney Disease, Biomedical Imaging, Urologic Diseases, Clinical Sciences, Urology & Nephrology
Abstract

Purpose: Kidney stone patients routinely have CT scans during diagnostic work-up before being referred to a tertiary center. How often these patients exceed the recommended dose limits for occupational radiation exposure of >100 mSv for 5 years and >50 mSv in a single year from CT alone remains unknown. This study aimed to quantify radiation doses from CTs received by stone patients before their evaluation at a tertiary care stone clinic. Methods: From November 2015 to March 2017, consecutive new patients enrolled into the Registry for Stones of the Kidney and Ureter (ReSKU™) had the dose-length product of every available CT abdomen/pelvis within 5 years of their initial visit recorded, allowing for an effective dose (EDose) calculation. Multivariate logistic regression analysis identified factors associated with exceeding recommended dose limits. Models were created to test radiation reducing effects of low-dose and phase-reduction CT protocols. Results: Of 343 noncontrast CTs performed, only 29 (8%) were low-dose CTs (calculated EDose 20 mSv and >50 mSv/year, respectively. Increased body mass index, number of scans, and multiphase scans were associated with exceeding exposure thresholds (p 50%. Conclusions: Stone patients referred to a tertiary stone center may receive excessive radiation from CT scans alone. Unnecessary phases and underutilization of low-dose CT protocols continue to take place. Enacting new approaches to CT protocols may spare stone patients from exceeding recommended dose limits.

Published
2019

4. Identifying factors associated with need for flexible ureteroscope repair: a Western Endourology STone (WEST) research consortium prospective cohort study

Author

Taguchi, Kazumi, Harper, Jonathan D, Stoller, Marshall L, Duty, Brian D, Sorensen, Mathew D, Sur, Roger L, Usawachintachit, Manint, Tzou, David T, Wenzler, David L, Isaacson, Dylan, Xu, Angela, Chu, Carissa, Zaid, Uwais B, Taylor, Eric R, Ramaswamy, Krishna, and Chi, Thomas

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Clinical Research, Adult, Equipment Design, Equipment Failure Analysis, Female, Humans, Lithotripsy, Male, Perioperative Period, Prospective Studies, United States, Ureter, Ureteroscopes, Ureteroscopy, Urolithiasis, Young Adult, Reusable flexible ureteroscope, Scope repair, Durability, Ureteral access sheath, Urology & Nephrology, Clinical sciences
Abstract

Maintenance of flexible ureteroscopes can involve high costs and administrative burden. Instrument fragility necessitates eventual repair, rendering scopes inaccessible during refurbishment. We conducted a multi-institutional prospective cohort study to identify perioperative factors influencing flexible ureteroscope durability. Patients undergoing flexible ureteroscopy (URS) at six United States endourology centers were enrolled between August 2014 and June 2015. Surgeon self-reported concern and satisfaction with scope performance as well as upward and downward angles of deflection for each scope tip were measured before and after each procedure. The need for scope repair was determined by the operating surgeon at the time of the procedure and recorded. 424 URS cases using 74 flexible ureteroscopes were identified. Scope repair was required in 28 cases (6.6%) involving 26 scopes (35.1%). Upon univariate analysis, shorter patient height, absence of guidewire use, presence of a ureteral access sheath (UAS), longer procedure time, larger stone size, lithotrite type, surgeon training level, and self-reported concern were associated with scope repair. Upon multivariate analysis, UAS use (OR = 2.53, p = 0.005) and degree loss of scope upward flexion during a case (OR = 1.02, p = 0.03) increased the odds of a scope needing repair while the use of safety guidewire decreased the odds of a scope repair (OR = 0.50, p = 0.045). Lithotrite use and surgeon concern were associated with degree loss of scope upward flexion. The use of a UAS, absence of a safety guidewire, and the loss of upward ureteroscope flexion should be considered when evaluating means of optimizing reusable ureteroscope durability.

Published
2018

5. Three-dimensional imaging of the developing human fetal urogenital-genital tract: Indifferent stage to male and female differentiation.

Author

Isaacson, Dylan, Shen, Joel, Overland, Maya, Li, Yi, Sinclair, Adriane, Cao, Mei, McCreedy, Dylan, Calvert, Meredith, McDevitt, Todd, Cunha, Gerald R, and Baskin, Laurence

Subjects
Urogenital System, Humans, Imaging, Three-Dimensional, Microscopy, Electron, Scanning, Fetal Development, Sex Differentiation, Female, Male, Human fetal urogenita tract, Lightsheet microscopy, Optical projection tomography, Scanning electron microscopy, Three-dimensional imaging, Developmental Biology, Biochemistry and Cell Biology, Paediatrics and Reproductive Medicine
Abstract

Recent studies in our lab have utilized three imaging techniques to visualize the developing human fetal urogenital tract in three dimensions: optical projection tomography, scanning electron microscopy and lightsheet fluorescence microscopy. We have applied these technologies to examine changes in morphology and differential gene expression in developing human external genital specimens from the ambisexual stage (13 weeks fetal age). This work outlines the history and function of each of these three imaging modalities, our methods to prepare specimens for each and the novel findings we have produced thus far. We believe the images in this paper of human fetal urogenital organs produced using lightsheet fluorescence microscopy are the first published to date.

Published
2018

6. Development of the human female reproductive tract.

Author

Cunha, Gerald R, Robboy, Stanley J, Kurita, Takeshi, Isaacson, Dylan, Shen, Joel, Cao, Mei, and Baskin, Laurence S

Subjects
Genitalia, Female, Uterus, Vagina, Mullerian Ducts, Humans, Homeodomain Proteins, Tumor Suppressor Proteins, Receptors, Progesterone, Transcription Factors, Female, LIM-Homeodomain Proteins, Cervix, Human Müllerian duct, Urogenital sinus, Uterovaginal canal, Wolffian duct, Human Mullerian duct, Developmental Biology, Biochemistry and Cell Biology, Paediatrics and Reproductive Medicine
Abstract

Development of the human female reproductive tract is reviewed from the ambisexual stage to advanced development of the uterine tube, uterine corpus, uterine cervix and vagina at 22 weeks. Historically this topic has been under-represented in the literature, and for the most part is based upon hematoxylin and eosin stained sections. Recent immunohistochemical studies for PAX2 (reactive with Müllerian epithelium) and FOXA1 (reactive with urogenital sinus epithelium and its known pelvic derivatives) shed light on an age-old debate on the derivation of vaginal epithelium supporting the idea that human vaginal epithelium derives solely from urogenital sinus epithelium. Aside for the vagina, most of the female reproductive tract is derived from the Müllerian ducts, which fuse in the midline to form the uterovaginal canal, the precursor of uterine corpus and uterine cervix an important player in vaginal development as well. Epithelial and mesenchymal differentiation markers are described during human female reproductive tract development (keratins, homeobox proteins (HOXA11 and ISL1), steroid receptors (estrogen receptor alpha and progesterone receptor), transcription factors and signaling molecules (TP63 and RUNX1), which are expressed in a temporally and spatially dynamic fashion. The utility of xenografts and epithelial-mesenchymal tissue recombination studies are reviewed.

Published
2018

7. Development of the human prostate.

Author

Cunha, Gerald R, Vezina, Chad M, Isaacson, Dylan, Ricke, William A, Timms, Barry G, Cao, Mei, Franco, Omar, and Baskin, Laurence S

Subjects
Urogenital System, Urethra, Prostate, Epithelial Cells, Mesoderm, Humans, Prostatic Neoplasms, Androgens, Estrogens, Cell Differentiation, Female, Male, Urologic Diseases, Cancer, Developmental Biology, Biochemistry and Cell Biology, Paediatrics and Reproductive Medicine
Abstract

This paper provides a detailed compilation of human prostatic development that includes human fetal prostatic gross anatomy, histology, and ontogeny of selected epithelial and mesenchymal differentiation markers and signaling molecules throughout the stages of human prostatic development: (a) pre-bud urogenital sinus (UGS), (b) emergence of solid prostatic epithelial buds from urogenital sinus epithelium (UGE), (c) bud elongation and branching, (d) canalization of the solid epithelial cords, (e) differentiation of luminal and basal epithelial cells, and (f) secretory cytodifferentiation. Additionally, we describe the use of xenografts to assess the actions of androgens and estrogens on human fetal prostatic development. In this regard, we report a new model of de novo DHT-induction of prostatic development from xenografts of human fetal female urethras, which emphasizes the utility of the xenograft approach for investigation of initiation of human prostatic development. These studies raise the possibility of molecular mechanistic studies on human prostatic development through the use of tissue recombinants composed of mutant mouse UGM combined with human fetal prostatic epithelium. Our compilation of human prostatic developmental processes is likely to advance our understanding of the pathogenesis of benign prostatic hyperplasia and prostate cancer as the neoformation of ductal-acinar architecture during normal development is shared during the pathogenesis of benign prostatic hyperplasia and prostate cancer.

Published
2018

8. Macroscopic whole-mounts of the developing human fetal urogenital-genital tract: Indifferent stage to male and female differentiation

Author

Shen, Joel, Cunha, Gerald R, Sinclair, Adriane, Cao, Mei, Isaacson, Dylan, and Baskin, Laurence

Subjects
Biochemistry and Cell Biology, Biological Sciences, Urologic Diseases, Contraception/Reproduction, Reproductive health and childbirth, Cell Differentiation, Female, Fetal Development, Fetus, Genitalia, Humans, Male, Ovary, Testis, Urogenital System, Paediatrics and Reproductive Medicine, Developmental Biology, Biochemistry and cell biology
Abstract

We present a detailed review of fetal development of the male and female human urogenital tract from 8 to 22 weeks gestation at the macroscopic and morphometric levels. Human fetal specimens were sexed based on macroscopic identification of fetal testes or ovaries, Wolffian or Müllerian structures and the presence of the SRY gene in the specimens at or near the indifferent stage (8-9 weeks). Specimens were photographed using a dissecting microscope with transmitted and reflected light. Morphometric measurements were taken of each urogenital organ. During this time period, development of the male and female urogenital tracts proceeded from the indifferent stage to differentiated organs. The kidneys, ureters, and bladder developed identically, irrespective of sex with the same physical dimensions and morphologic appearance. The penis, prostate and testis developed in males and the clitoris, uterus and ovary in females. Androgen-dependent growth certainly influenced size and morphology of the penile urethra and prostate, however, androgen-independent growth also accounted for substantial growth in the fetal urogenital tract including the clitoris.

Published
2018

9. Development of the human penis and clitoris

Author

Baskin, Laurence, Shen, Joel, Sinclair, Adriane, Cao, Mei, Liu, Xin, Liu, Ge, Isaacson, Dylan, Overland, Maya, Li, Yi, and Cunha, Gerald R

Subjects
Biochemistry and Cell Biology, Biological Sciences, Urologic Diseases, Genetics, Clitoris, Female, Humans, Male, Microscopy, Electron, Scanning, Penis, Urethra, Development, Human, Canalization and usion, Canalization and fusion, Paediatrics and Reproductive Medicine, Developmental Biology, Biochemistry and cell biology
Abstract

The human penis and clitoris develop from the ambisexual genital tubercle. To compare and contrast the development of human penis and clitoris, we used macroscopic photography, optical projection tomography, light sheet microscopy, scanning electron microscopy, histology and immunohistochemistry. The human genital tubercle differentiates into a penis under the influence of androgens forming a tubular urethra that develops by canalization of the urethral plate to form a wide diamond-shaped urethral groove (opening zipper) whose edges (urethral folds) fuse in the midline (closing zipper). In contrast, in females, without the influence of androgens, the vestibular plate (homologue of the urethral plate) undergoes canalization to form a wide vestibular groove whose edges (vestibular folds) remain unfused, ultimately forming the labia minora defining the vaginal vestibule. The neurovascular anatomy is similar in both the developing human penis and clitoris and is the key to successful surgical reconstructions.

Published
2018

10. Immunohistochemical expression analysis of the human fetal lower urogenital tract

Author

Shen, Joel, Isaacson, Dylan, Cao, Mei, Sinclair, Adriane, Cunha, Gerald R, and Baskin, Laurence

Subjects
Biochemistry and Cell Biology, Biological Sciences, Urologic Diseases, Congenital Structural Anomalies, Pediatric, Reproductive health and childbirth, Clitoris, Epithelium, Female, Fetal Development, Gene Expression Regulation, Developmental, Genitalia, Female, Hepatocyte Nuclear Factor 3-alpha, Humans, Immunohistochemistry, Keratin-10, Male, PAX2 Transcription Factor, Penis, Urethra, Urogenital System, Vagina, Immunohistochemical, Human fetal lower urogenital tract, Sagittal sections, Paediatrics and Reproductive Medicine, Developmental Biology, Biochemistry and cell biology
Abstract

We have studied the ontogeny of the developing human male and female urogenital tracts from 9 weeks (indifferent stage) to 16 weeks (advanced sex differentiation) of gestation by immunohistochemistry on mid-sagittal sections. Sixteen human fetal pelvises were serial sectioned in the sagittal plane and stained with antibodies to epithelial, muscle, nerve, proliferation and hormone receptor markers. Key findings are: (1) The corpus cavernosum in males and females extends into the glans penis and clitoris, respectively, during the ambisexual stage (9 weeks) and thus appears to be an androgen-independent event. (2) The entire human male (and female) urethra is endodermal in origin based on the presence of FOXA1, KRT 7, uroplakin, and the absence of KRT10 staining. The endoderm of the urethra interfaces with ectodermal epidermis at the site of the urethral meatus. (3) The surface epithelium of the verumontanum is endodermal in origin (FOXA1-positive) with a possible contribution of Pax2-positive epithelial cells implying additional input from the Wolffian duct epithelium. (4) Prostatic ducts arise from the endodermal (FOXA1-positive) urogenital sinus epithelium near the verumontanum. (5) Immunohistochemical staining of mid-sagittal and para-sagittal sections revealed the external anal sphincter, levator ani, bulbospongiosus muscle and the anatomic relationships between these developing skeletal muscles and organs of the male and female reproductive tracts. Future studies of normal human developmental anatomy will lay the foundation for understanding congenital anomalies of the lower urogenital tract.

Published
2018

11. Human glans and preputial development

Author

Liu, Xin, Liu, Ge, Shen, Joel, Yue, Aaron, Isaacson, Dylan, Sinclair, Adriane, Cao, Mei, Liaw, Aron, Cunha, Gerald R, and Baskin, Laurence

Subjects
Biochemistry and Cell Biology, Biological Sciences, Urologic Diseases, Cell Differentiation, Endoderm, Epithelial Cells, Gene Expression Regulation, Developmental, Hepatocyte Nuclear Factor 3-alpha, Humans, Male, Morphogenesis, Penis, Receptors, Androgen, Urethra, Uroplakins, Development, Human, Glans, Prepuce, Canalization, Paediatrics and Reproductive Medicine, Developmental Biology, Biochemistry and cell biology
Abstract

The urethra within the human penile shaft develops via (1) an "Opening Zipper" that facilitates distal canalization of the solid urethral plate to form a wide urethral groove and (2) a "Closing Zipper" that facilitates fusion of the epithelial surfaces of the urethral folds. Herein, we extend our knowledge by describing formation of the human urethra within the glans penis as well as development of the prepuce. Forty-eight normal human fetal penile specimens were examined using scanning electron microscopy and optical projection tomography. Serial histologic sections were evaluated for morphology and immunohistochemical localization for epithelial differentiation markers: Cytokeratins 6, 7, 10, FoxA1, uroplakin and the androgen receptor. As the closing zipper completes fusion of the urethral folds within the penile shaft to form a tubular urethra (~ 13 weeks), canalization of the urethral plate continues in proximal to distal fashion into the glans penis to directly form the urethra within the glans without forming an open urethral groove. Initially, the urethral plate is attached ventrally to the epidermis via an epithelial seam, which is remodeled and eliminated, thus establishing mesenchymal confluence ventral to the glanular urethra. The morphogenetic remodeling involves the strategic expression of cytokeratin 7, FoxA1 and uroplakin in endodermal epithelial cells as the tubular glanular urethra forms. The most ventral epithelial cells of the urethral plate are pinched off from the glanular urethra and are reabsorbed into the epidermis ultimately losing expression of their markers, a process undoubtedly regulated by androgens. The prepuce initially forms on the dorsal aspect of the glans at approximately 12 weeks of gestation. After sequential proximal to distal remodeling of the ventral urethral plate along the ventral aspect of glans, the prepuce of epidermal origin fuses in the ventral midline.

Published
2018

12. Micro-Costing Analysis Demonstrates Comparable Costs for LithoVue Compared to Reusable Flexible Fiberoptic Ureteroscopes

Author

Taguchi, Kazumi, Usawachintachit, Manint, Tzou, David T, Sherer, Benjamin A, Metzler, Ian, Isaacson, Dylan, Stoller, Marshall L, and Chi, Thomas

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Clinical Research, Costs and Cost Analysis, Disposable Equipment, Equipment Design, Equipment Reuse, Fiber Optic Technology, Humans, Operating Rooms, Prospective Studies, Ureteroscopes, Ureteroscopy, Urologists, micro-costing, disposable flexible ureteroscope, reusable flexible ureteroscope, Urology & Nephrology, Clinical sciences
Abstract

INTRODUCTION:Reusable ureteroscope durability and need for repair are significant sources of expense and inefficiency for patients and urologists. Utilization of LithoVue™, a disposable flexible digital ureteroscope, may address some of these concerns. To identify its economic impact on clinical care, we performed a micro-cost comparison between flexible reusable fiberoptic ureteroscopes (URF-P6™) and LithoVue. PATIENTS AND METHODS:For this prospective, single-center micro-costing study, all consecutive ureteroscopies performed during 1 week each in July and August 2016 utilized either URF-P6 or LithoVue ureteroscopes respectively. Workflow data were collected, including intraoperative events, postoperative reprocessing cycle timing, consumables usage, and ureteroscope cost data. RESULTS:Intraoperative data analysis showed mean total operating room time for URF-P6 and LithoVue cases were 93.4 ± 32.3 and 73.6 ± 17.4 minutes, respectively (p = 0.093). Mean cost of operating room usage per case was calculated at $1618.72 ± 441.39 for URF-P6 and $1348.64 ± 237.40 for LithoVue based on institutional cost rates exclusive of disposables. Postoperative data analysis revealed costs of $107.27 for labor and consumables during reprocessing for URF-P6 cases. The costs of ureteroscope repair and capital acquisition for each URF-P6 case were $957.71 and $116.02, respectively. The total ureteroscope cost per case for URF-P6 and LithoVue were $2799.72 and $2852.29, respectively. CONCLUSIONS:Micro-cost analysis revealed that the cost of LithoVue acquisition is higher per case compared to reusable fiberoptic ureteroscopes, but savings are realized in labor, consumables, and repair. When accounting for these factors, the total cost per case utilizing these two ureteroscopes were comparable.

Published
2018

13. Variation in Radiologic and Urologic Computed Tomography Interpretation of Urinary Tract Stone Burden: Results From the Registry for Stones of the Kidney and Ureter.

Author

Tzou, David T, Isaacson, Dylan, Usawachintachit, Manint, Wang, Zhen J, Taguchi, Kazumi, Hills, Nancy K, Hsi, Ryan S, Sherer, Benjamin A, Reliford-Titus, Shalonda, Duty, Brian, Harper, Jonathan D, Sorensen, Mathew, Sur, Roger L, Stoller, Marshall L, and Chi, Thomas

Subjects
Humans, Kidney Calculi, Ureteral Calculi, Tomography, X-Ray Computed, Radiography, Diagnostic Techniques, Urological, Registries, Prospective Studies, Middle Aged, Female, Male, Urologic Diseases, Biomedical Imaging, Kidney Disease, Renal and urogenital, Urology & Nephrology, Clinical Sciences
Abstract

OBJECTIVE:To compare the measured stone burden recorded between urologists and radiologists, and examine how these differences could potentially impact stone management. As current urologic stone surgery guideline recommendations are based on stone size, accurate stone measurements are crucial to direct appropriate treatment. This study investigated the discrepant interpretation that often exists between urologic surgeons and radiologists' estimation of patient urinary stone burden. MATERIALS AND METHODS:From November 2015 through August 2016, new patients prospectively enrolled into the Registry for Stones of the Kidney and Ureter (ReSKU) were included if they had computed tomography images available and an accompanying official radiologic report at the time of their urologist provider visit. Stone number and aggregate stone size were compared between the urologic interpretation and the corresponding radiologic reports. RESULTS:Of 219 patients who met the inclusion criteria, concordance between urologic and radiologic assessment of aggregate stone size was higher for single stone sizing (63%) compared with multiple stones (32%). Statistical significance was found in comparing the mean difference in aggregate stone size for single and multiple stones (P

Published
2018

14. Qualitative, rather than quantitative, differences between HLA‐DQ alleles affect HLA‐DQ immunogenicity in organ transplantation

Author

Maguire, Chelsea, primary, Crivello, Pietro, additional, Fleischhauer, Katharina, additional, Isaacson, Dylan, additional, Casillas, Aurora, additional, Kramer, Cynthia S. M., additional, Copley, Hannah C., additional, Heidt, Sebastiaan, additional, Kosmoliaptsis, Vasilis, additional, Meneghini, Maria, additional, Gmeiner, Michael, additional, Schold, Jesse, additional, Louzoun, Yoram, additional, and Tambur, Anat R., additional

Published
2024
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15. Renal Subcapsular xenografing of human fetal external genital tissue – A new model for investigating urethral development

Author

Isaacson, Dylan, Shen, Joel, Cao, Mei, Sinclair, Adriane, Yue, Xuan, Cunha, Gerald, and Baskin, Laurence

Subjects
Biochemistry and Cell Biology, Biological Sciences, Urologic Diseases, Estrogen, Animals, Endocrine Disruptors, Female, Genitalia, Female, Humans, Hypospadias, Kidney, Male, Mice, Organogenesis, Penis, Receptors, Androgen, Urethra, Genital tubercle, Xenograft, Endocrine disruptors, Nude mouse, Paediatrics and Reproductive Medicine, Developmental Biology, Biochemistry and cell biology
Abstract

In this paper, we introduce our novel renal subcapsular xenograft model for the study of human penile urethral and clitoral development. We grafted fifteen intact fetal penes and clitorides 8-11 weeks fetal age under the renal capsules of gonadectomized athymic mice. The mice were treated with a subcutaneous pellet of dihydrotestosterone (DHT), diethylstilbestrol (DES) or untreated with hormones. Xenografts were harvested after fourteen days of growth and analyzed via serial histologic sectioning and immunostaining for Ki-67, cytokeratins 6, 7 and 10, uroplakin and the androgen receptor. Non-grafted specimens of similar fetal age were sectioned and immunostained for the same antigenic markers. 14/15 (93.3%) grafts were successfully propagated and harvested. The developing urethral plate, urethral groove, tubular urethra, corporal bodies and preputial lamina were easily identifiable. These structures demonstrated robust cellularity, appropriate architecture and abundant Ki-67 expression. Expression patterns of cytokeratins 6, 7 and 10, uroplakin and the androgen receptor in xenografted specimens demonstrated characteristic male/female differences analogous to non-grafted specimens. DHT treatment reliably produced tubularization of nascent urethral and vestibular structures and male patterns of androgen receptor expression in grafts of both genetic sexes while estrogenic or hormonally absent conditions reliably resulted in a persistent open urethral/vestibular groove and female patterns of androgen receptor expression. This model's success enables further study into causal pathways by which endocrine-disrupting and endocrine-mimicking substances may directly cause disruption of normal human urethral development or hypospadias.

Published
2017

16. Defining the Costs of Reusable Flexible Ureteroscope Reprocessing Using Time-Driven Activity-Based Costing

Author

Isaacson, Dylan, Ahmad, Tessnim, Metzler, Ian, Tzou, David T, Taguchi, Kazumi, Usawachintachit, Manint, Zetumer, Samuel, Sherer, Benjamin, Stoller, Marshall, and Chi, Thomas

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Clinical Research, Prevention, Costs and Cost Analysis, Equipment Failure, Equipment Reuse, Humans, Infection Control, Operating Rooms, Sterilization, Time and Motion Studies, Ureteroscopes, Ureteroscopy, ureteroscope, sterile processing, cost analysis, time-driven activity-based costing, Urology & Nephrology, Clinical sciences
Abstract

PurposeCareful decontamination and sterilization of reusable flexible ureteroscopes used in ureterorenoscopy cases prevent the spread of infectious pathogens to patients and technicians. However, inefficient reprocessing and unavailability of ureteroscopes sent out for repair can contribute to expensive operating room (OR) delays. Time-driven activity-based costing (TDABC) was applied to describe the time and costs involved in reprocessing.Materials and methodsDirect observation and timing were performed for all steps in reprocessing of reusable flexible ureteroscopes following operative procedures. Estimated times needed for each step by which damaged ureteroscopes identified during reprocessing are sent for repair were characterized through interviews with purchasing analyst staff. Process maps were created for reprocessing and repair detailing individual step times and their variances. Cost data for labor and disposables used were applied to calculate per minute and average step costs.ResultsTen ureteroscopes were followed through reprocessing. Process mapping for ureteroscope reprocessing averaged 229.0 ± 74.4 minutes, whereas sending a ureteroscope for repair required an estimated 143 minutes per repair. Most steps demonstrated low variance between timed observations. Ureteroscope drying was the longest and highest variance step at 126.5 ± 55.7 minutes and was highly dependent on manual air flushing through the ureteroscope working channel and ureteroscope positioning in the drying cabinet. Total costs for reprocessing totaled $96.13 per episode, including the cost of labor and disposable items.ConclusionsUtilizing TDABC delineates the full spectrum of costs associated with ureteroscope reprocessing and identifies areas for process improvement to drive value-based care. At our institution, ureteroscope drying was one clearly identified target area. Implementing training in ureteroscope drying technique could save up to 2 hours per reprocessing event, potentially preventing expensive OR delays.

Published
2017

17. A Prospective Case–Control Study Comparing LithoVue, a Single-Use, Flexible Disposable Ureteroscope, with Flexible, Reusable Fiber-Optic Ureteroscopes

Author

Usawachintachit, Manint, Isaacson, Dylan S, Taguchi, Kazumi, Tzou, David T, Hsi, Ryan S, Sherer, Benjamin A, Stoller, Marshall L, and Chi, Thomas

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Clinical Research, Urologic Diseases, Adult, Aged, Case-Control Studies, Equipment Design, Female, Fiber Optic Technology, Humans, Kidney Calculi, Male, Middle Aged, Operative Time, Patient Safety, Prospective Studies, Treatment Outcome, Ureteroscopes, Ureteroscopy, Urinary Bladder Neoplasms, Urinary Calculi, Urothelium, equipment design, kidney calculi, ureteroscopes, urolithiasis, Urology & Nephrology, Clinical sciences
Abstract

ObjectiveLithoVue™ is a novel, single-use, digital flexible ureteroscope that was released to the US market in January 2016. There are scant data regarding its performance in humans. Procedural outcomes comparing LithoVue with reusable ureteroscopes are presented in patients undergoing ureteroscopy for upper urinary tract pathology.Patients and methodsClinical outcomes between two groups of patients undergoing flexible ureteroscopy for upper urinary tract pathology were analyzed. The first group underwent surgery utilizing LithoVue, and the second group used reusable fiber-optic flexible ureteroscopes. Differences in procedural outcomes, operative times, and time spent in hospital were analyzed using two-tailed t-tests and chi-squared and Fisher's exact tests.ResultsOne hundred fifteen cases utilizing LithoVue and 65 cases utilizing reusable ureteroscopes were included in this study. Demographics, surgical indications, stone size, location, total stone burden, composition, procedural outcomes, and complications were comparable between groups. For all cases, LithoVue procedures lasted 54.1 ± 25.7 minutes compared with 64.5 ± 37.0 minutes for reusable scope procedures (p

Published
2017

22. MP40-04 LONG-TERM TUMOR NECROSIS FACTOR-ALPHA INHIBITOR USE DECREASES THE RISK OF PROSTATE CANCER

Author

Driscoll, Conor, primary, Rich, Jordan, additional, Isaacson, Dylan, additional, Nicolas, Joseph, additional, Jiang, Yu, additional, Mi, Xinlei, additional, Yang, Christopher, additional, Kocsuta, Victoria, additional, Goh, Regine, additional, Patel, Niti, additional, Li, Eric, additional, Siddiqui, Rashid, additional, Meyers, Travis, additional, Witte, John, additional, Kachuri, Linda, additional, Zhang, Hui, additional, Beestrum, Molly, additional, Schaeffer, Edward, additional, and Kundu, Shilajit, additional

Published
2023
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23. PD08-03 LONG-TERM TUMOR NECROSIS FACTOR-ALPHA INHIBITOR USE INCREASES THE RISK OF RENAL CELL CARCINOMA

Author

Driscoll, Conor, primary, Rich, Jordan, additional, Isaacson, Dylan, additional, Nicolas, Joseph, additional, Jiang, Yu, additional, Mi, Xinlei, additional, Yang, Christopher, additional, Kocsuta, Victoria, additional, Goh, Regine, additional, Patel, Niti, additional, Li, Eric, additional, Siddiqui, Rashid, additional, Meyers, Travis, additional, Witte, John, additional, Kachuri, Linda, additional, Zhang, Hui, additional, Beestrum, Molly, additional, Schaeffer, Edward, additional, and Kundu, Shilajit, additional

Published
2023
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29. Contributors

Author

Abaza, Ronney, Abu-Ghanem, Yasmin, Ahlering, Thomas E., Ahmad, Sarfraz, Albert, Matthew, Alip, Sylvia, Allaf, Mohamad E., Almeida, Aubrey Anthony, Antippa, Phillip, Aquina, Christopher T., Asairinachan, Ashwinna, Assumma, Simone, Autorino, Riccardo, Beksac, Alp Tuna, Bermeo, Adriana Pedraza, Bloom, Scott W., Bocciardi, Aldo M., Borin, James F., Breda, Alberto, Cadeddu, Jeffrey A., Challacombe, Ben, Chan, Yvonne Y., Changoor, Navin R., Chen, Yi, Cheng, Nathan, Chung, Catherine, Cleary, Robert K., Coelho, Rafael Ferreira, Collins, Justin W., Costello, Anthony J., Costello, Daniel M., Costello, Samuel, Costello, Timothy, Crawford, Julia A., Dai, Jessica C., Dasgupta, Prokar, de Carvalho, Paulo Afonso, Nero, Alberto Del, Dell’Oglio, Paolo, Deruyver, Yves, Diana, Pietro, Diaz, John P., Dixon, Benjamin, Dovey, Zachary, Dowthwaite, Samuel, Dundee, Philip, Dunne, Ben, Everaerts, Wouter, Fitzsimmons, Christine K., Floros, Peter, Foreman, Andrew, Fricke, Tyson A., Fuglestad, Matthew, Furrer, Marc Alain, Galfano, Antonio, Gallagher, Richard, Gallant, Thomas, Gallioli, Andrea, Gaya, J.M., Ghazi, Ahmed, Gray, Matthew, Gross, Tobias, Guru, Khurshid A., Hampton, Lance J., Hazen, Nick, Heriot, Alexander G., Hodge, John-Charles, Holloway, Robert W., Huang, Erica, Hung, Andrew J., Hussein, Ahmed Aly, Huynh, Linda My, Iglesia, Cheryl B., Iqbal, Umar, Isaacson, Dylan, Jacobson, Jillian C., Jenks, Carolyn M., Johnston, Douglas R., Kahn, Ryan M., Kaouk, Jihad, Katz, Eric G., Kavoussi, Parviz K., Kennard, Jessica A., Ko, Young Hwii, Kogan, Paul, Kornfeld, Belen, Krishnan, Giri, Krishnan, Suren, Kudish, Bela, Riva, Anibal La, Larkins, Kirsten M., Lawrentschuk, Nathan, Lee, Ryan S., Lindgren, Bruce W., Linnartz, Kirsten, Lira, Renan, Low, David, Lucking, Jonathan, Ma, Runzhuo, Magnuson, J. Scott, Martini, Alberto, Maurrasse, Sarah E., McDowell, Zachary, McKenzie, Nathalie Dauphin, Megison, Steve, Meyer, P. Hunter, Mishra, Kirtishri, Mittakanti, Harsha, Mohan, Helen M., Monson, John R.T., Mora, Cristina, Moschovas, Marcio Covas, Nair, Rajesh, Norris, Briony L., Omana, Harold John, Palou, Joan, Pandya, Samir R., Parekh, Sneha, Patel, Vipul, Perez, Laura C., Peters, Craig A., Peters, Justin S., Piana, Alberto, Plazarte, Victor Calderon, Plumblee, Leah, Polotti, Charles F., Porter, James Roscoe, Pullatt, Rana, Rai, Sonpreet, Raison, Nicholas, Rajkomar, Amrish K.S., Ratnaraj, Vignesh, Rayman, Shlomi, Reeves, Fairleigh A., Rha, Koon Ho, Robinson, James, Rocco, Bernardo, Rodrigues, Gilberto José, Rosemurgy, Alexander S., II, Ross, Sharona B., Sahota, Bindy, Savoni, Jessica, Sayegh, Aref S., Schulster, Michael L., Shapera, Emanuel, Sighinolfi, Maria Chiara, Singh, Ravjit, Layne, Alyssa Small, Soliman, Mark K., Sotelo, Rene, Stifelman, Michael, Stockwell, Erica, Sucandy, Iswanto, Takhar, Arunjit, Territo, Angelo, Terzoni, Stefano, Tewari, Ashutosh, Thomas, Benjamin C., Tissot, Sophie J., Tosco, Lorenzo, Touadi, Melissa, Tutungi, Elli, Van der Aa, Frank, Visser, William, Wagaskar, Vinayak, Warrier, Satish K., White, Jonah, Wiklund, Peter, Xu, Alex J., Yu, Eileen, and Zhao, Lee C.

Published
2024
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37. Macroscopic whole-mounts of the developing human fetal urogenital-genital tract: Indifferent stage to male and female differentiation.

Author

Sinclair, Adriane, Sinclair, Adriane, Cao, Mei, Isaacson, Dylan, Baskin, Laurence, Shen, Joel, Cunha, Gerald, Sinclair, Adriane, Sinclair, Adriane, Cao, Mei, Isaacson, Dylan, Baskin, Laurence, Shen, Joel, and Cunha, Gerald

Abstract

We present a detailed review of fetal development of the male and female human urogenital tract from 8 to 22 weeks gestation at the macroscopic and morphometric levels. Human fetal specimens were sexed based on macroscopic identification of fetal testes or ovaries, Wolffian or Müllerian structures and the presence of the SRY gene in the specimens at or near the indifferent stage (8-9 weeks). Specimens were photographed using a dissecting microscope with transmitted and reflected light. Morphometric measurements were taken of each urogenital organ. During this time period, development of the male and female urogenital tracts proceeded from the indifferent stage to differentiated organs. The kidneys, ureters, and bladder developed identically, irrespective of sex with the same physical dimensions and morphologic appearance. The penis, prostate and testis developed in males and the clitoris, uterus and ovary in females. Androgen-dependent growth certainly influenced size and morphology of the penile urethra and prostate, however, androgen-independent growth also accounted for substantial growth in the fetal urogenital tract including the clitoris.

Published
2018

39. Development of the human prostate

Author

Cunha, Gerald R., primary, Vezina, Chad M., additional, Isaacson, Dylan, additional, Ricke, William A., additional, Timms, Barry G., additional, Cao, Mei, additional, Franco, Omar, additional, and Baskin, Laurence S., additional

Published
2018
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40. Human glans and preputial development

Author

Liu, Xin, primary, Liu, Ge, additional, Shen, Joel, additional, Yue, Aaron, additional, Isaacson, Dylan, additional, Sinclair, Adriane, additional, Cao, Mei, additional, Liaw, Aron, additional, Cunha, Gerald R., additional, and Baskin, Laurence, additional

Published
2018
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44. Development of the human penis and clitoris

Author

Baskin, Laurence, primary, Shen, Joel, additional, Sinclair, Adriane, additional, Cao, Mei, additional, Liu, Xin, additional, Liu, Ge, additional, Isaacson, Dylan, additional, Overland, Maya, additional, Li, Yi, additional, and Cunha, Gerald R., additional

Published
2018
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48. Variation in Radiologic and Urologic Computed Tomography Interpretation of Urinary Tract Stone Burden: Results From the Registry for Stones of the Kidney and Ureter

Author

Tzou, David T., primary, Isaacson, Dylan, additional, Usawachintachit, Manint, additional, Wang, Zhen J., additional, Taguchi, Kazumi, additional, Hills, Nancy K., additional, Hsi, Ryan S., additional, Sherer, Benjamin A., additional, Reliford-Titus, Shalonda, additional, Duty, Brian, additional, Harper, Jonathan D., additional, Sorensen, Mathew, additional, Sur, Roger L., additional, Stoller, Marshall L., additional, and Chi, Thomas, additional

Published
2018
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49. Identifying factors associated with need for flexible ureteroscope repair: a Western Endourology STone (WEST) research consortium prospective cohort study

Author

Taguchi, Kazumi, primary, Harper, Jonathan D., additional, Stoller, Marshall L., additional, Duty, Brian D., additional, Sorensen, Mathew D., additional, Sur, Roger L., additional, Usawachintachit, Manint, additional, Tzou, David T., additional, Wenzler, David L., additional, Isaacson, Dylan, additional, Xu, Angela, additional, Chu, Carissa, additional, Zaid, Uwais B., additional, Taylor, Eric R., additional, Ramaswamy, Krishna, additional, and Chi, Thomas, additional

Published
2017
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