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151. Well‐differentiated lipomatous neoplasms with p53 alterations: a clinicopathological and molecular study of eight cases with features of atypical pleomorphic lipomatous tumour.

Author

Hammer, Phoebe M, Kunder, Christian A, Howitt, Brooke E, and Charville, Gregory W

Subjects
BENIGN tumors, FAT cells, THIGH, TUMORS, LI-Fraumeni syndrome, DELETION mutation, CLINICAL pathology
Abstract

Aims: Well‐differentiated lipomatous neoplasms encompass a broad spectrum of benign and malignant tumours, many of which are characterised by recurrent genetic abnormalities. Although a key regulator of p53 signalling, MDM2, is characteristically amplified in well‐differentiated liposarcoma, recurrent abnormalities of p53 itself have not been reported in well‐differentiated adipocytic neoplasms. Here, we present a series of well‐differentiated lipomatous tumours characterised by p53 alterations and histological features in keeping with atypical pleomorphic lipomatous tumour (APLT). Methods and results: We reviewed the morphological, immunohistochemical and molecular genetic features of eight lipomatous tumours with p53 alterations. Four tumours arose in the thigh, and one case each arose in the shoulder, calf, upper back, and subclavicular regions; six tumours were deep/subfascial and two were subcutaneous. Relevant clinical history included two patients with Li–Fraumeni syndrome. Morphologically, all cases showed well‐differentiated adipocytes with prominent nuclear pleomorphism, limited mitotic activity, and no tumour cell necrosis. All cases were negative for MDM2 overexpression and amplification as determined with immunohistochemistry and fluorescence in‐situ hybridisation, respectively. Immunohistochemically, p16 was diffusely overexpressed in all cases; seven tumours (88%) showed abnormal loss of Rb and p53. TP53 mutation or deletion was identified in four of six tumours evaluated with exon‐targeted hybrid capture‐based massively parallel sequencing; RB1 mutation or deletion was present in five of six cases. Conclusions: We present a series of eight well‐differentiated lipomatous neoplasms characterised by p53 alterations in addition to Rb loss and histological features of APLT. These findings suggest that impaired p53 signalling may contribute to the pathogenesis of APLT in a subset of cases. [ABSTRACT FROM AUTHOR]

Published
2022
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152. Pathological chemotherapy response score is prognostic in tubo-ovarian high-grade serous carcinoma: A systematic review and meta-analysis of individual patient data

Author

Cohen, Paul A., Powell, Aime, Böhm, Steffen, Gilks, C. Blake, Stewart, Colin J.R., Meniawy, Tarek M., Bulsara, Max, Avril, Stefanie, Brockbank, Eleanor C., Bosse, Tjalling, de Azevedo Focchi, Gustavo Rubino, Ganesan, Raji, Glasspool, Rosalind M., Howitt, Brooke E., Kim, Hyun-Soo, Lee, Jung-Yun, Le, Nhu D., Lockley, Michelle, Manchanda, Ranjit, Mandalia, Trupti, McCluggage, W. Glenn, McNeish, Iain, Midha, Divya, Srinivasan, Radhika, Tan, Yun Yi, van der Griend, Rachael, Yunokawa, Mayu, Zannoni, Gian F., Singh, Naveena, Aggarwal, Simi, Bronger, Holger, Brown, Elizabeth B., Buck, Martin, Bukhari, Syed A., Coghlan, Edwina, Cope, Nichola, de Almeida, Michelle Samora, De Kroon, Cornelius D., Dean, Andrew, Devlin, Michael-John, Ditzel, Helena M., Drecoll, Enken, Ebata, Takahiro, Fagotti, Anna, Faruqi, Asma, Feeney, Laura, Gupta, Kavita, Harley, Ian, Inzani, Frediano, Jeyarajah, Arjun R., Koay, M.H. Eleanor, Kroep, Judith R., Leung, Yee, Loft, Alice R., MaGee, Daniel, McKenna, Sarah, Millan, David, Millar, Joanne, Miller, Rowan, Mohan, Ganendra R., Mughal, Sohail, Nicolau, Sergio Mancini, Nevin, James, Oakley, Abigail S., Quigley, Mary, Rai, Bhavana, Rajwanshi, Arvind, Salfinger, Stuart G., Scambia, Giovanni, Scatchard, Kate, Schmalfeldt, Barbara, Simcock, Bryony, Singh, Priya, Strickland, Kyle C., Suri, Vainta, Syed, Sheeba, Sykes, Peter, Tamura, Kenji, Tan, Adeline, Tan, Jason, Thompson, Emily, Tinker, Anna V., Trevisan, Georgia, Uyeda, Maria Gabriela Baumgarten Kuster, Vaughan, Michelle M., Weichert, Wilko, Williams, Anthony, Williams, Sarah, Yoshida, Hiroshi, and Zorzato, Pier Carlo

Abstract

Objective:\ud There is a need to develop and validate biomarkers for treatment response and survival in tubo-ovarian high-grade serous carcinoma (HGSC). The chemotherapy response score (CRS) stratifies patients into complete/near-complete (CRS3), partial (CRS2), and no/minimal (CRS1) response after neoadjuvant chemotherapy (NACT). Our aim was to review current evidence to determine whether the CRS is prognostic in women with tubo-ovarian HGSC treated with NACT.\ud \ud Methods:\ud We established an international collaboration to conduct a systematic review and meta-analysis, pooling individual patient data from 16 sites in 11 countries. Patients had stage IIIC/IV HGSC, 3–4 NACT cycles and >6-months follow-up. Random effects models were used to derive combined odds ratios in the pooled population to investigate associations between CRS and progression free and overall survival (PFS and OS).\ud \ud Results:\ud 877 patients were included from published and unpublished studies. Median PFS and OS were 15 months (IQR 5–65) and 28 months (IQR 7–92) respectively. CRS3 was seen in 249 patients (28%). The pooled hazard ratios (HR) for PFS and OS for CRS3 versus CRS1/CRS2 were 0·55 (95% CI, 0·45–0·66; P

Published
2019

153. Germline BRCA-Associated Endometrial Carcinoma Is a Distinct Clinicopathologic Entity

Author

Jonge, Marthe M. de, Ritterhouse, Lauren L., Kroon, Cornelis D. de, Vreeswijk, Maaike P.G., Segal, Jeremy P., Puranik, Rutika, Wevers, M.R., Mensenkamp, A.R., Boer, M. de, Howitt, Brooke E., Bosse, T., Jonge, Marthe M. de, Ritterhouse, Lauren L., Kroon, Cornelis D. de, Vreeswijk, Maaike P.G., Segal, Jeremy P., Puranik, Rutika, Wevers, M.R., Mensenkamp, A.R., Boer, M. de, Howitt, Brooke E., and Bosse, T.

Abstract

Contains fulltext : 216691.pdf (Publisher’s version ) (Closed access)

Published
2019

158. Germline BRCA-Associated Endometrial Carcinoma Is a Distinct Clinicopathologic Entity

Author

de Jonge, Marthe M., primary, Ritterhouse, Lauren L., additional, de Kroon, Cornelis D., additional, Vreeswijk, Maaike P.G., additional, Segal, Jeremy P., additional, Puranik, Rutika, additional, Hollema, Harry, additional, Rookus, Matti A., additional, van Asperen, Christi J., additional, van Leeuwen, Flora E., additional, Smit, Vincent T.H.B.M., additional, Howitt, Brooke E., additional, and Bosse, Tjalling, additional

Published
2019
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159. Abstract AP01: LINEAGE CONTINUITY BETWEEN EARLY TUBAL SEROUS PROLIFERATIONS (ESPS/STILS) AND DISSEMINATED HIGH-GRADE SEROUS CARCINOMAS: A MODEL FOR “PRECURSOR ESCAPE”

Author

Soong, Thing Rinda, primary, Howitt, Brooke E., additional, Miron, Alexander, additional, Horowitz, Neil, additional, Campbell, Frank, additional, Feltmate, Colleen M., additional, Muto, Michael G., additional, Berkowitz, Ross S., additional, Nucci, Marisa R., additional, Xian, Wa, additional, and Crum, Christopher P., additional

Published
2019
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160. Abstract AP22: DNA DAMAGE RESPONSES AND IMMUNE PROFILING THROUGH HIGHLY MULTIPLEXED TISSUE IMMUNOFLUORESCENCE (T-CYCIF) IN HIGH-GRADE SEROUS OVARIAN CANCER

Author

Färkkilä, Anniina, primary, Lin, Jia-Ren, additional, Maliga, Zoltan, additional, Chopra, Sameer S., additional, Koruchupakkal, Bose, additional, Howitt, Brooke E., additional, Strickland, Kyle C., additional, Santagata, Sandro, additional, Swisher, Elizabeth M., additional, Matulonis, Ursula A., additional, Guerriero, Jennifer. L., additional, Elias, Kevin, additional, Konstantinopoulos, Panagiotis, additional, Sorger, Peter K., additional, and D'Andrea, Alan D., additional

Published
2019
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170. Contributors

Author

Amin, Mahul B., Ayala, Alberto G., Basturk, Olca, Calonje, J. Eduardo, Campbell, Fiona, Carter, Jodi M., Chan, John K.C., Cheuk, Wah, Clement, Philip B., Crum, Christopher P., Divatia, Mukul K., Eble, John N., Ellis, Ian O., Ferrell, Linda D., Fletcher, Christopher D.M., Fletcher, Jonathan A., Folberg, Robert, Garg, Karuna, Grignon, David J., Gru, Alejandro A., Hornick, Jason L., Howitt, Brooke E., Hunter, Keith D., Inwards, Carrie Y., Irving, Julie A., Kakar, Sanjay, Klimstra, David S., Klöppel, Günter, Kozakewich, Harry P.W., Kutok, Jeffery L., Lack, Ernest E., Lauwers, Gregory Y., Lee, Andrew H.S., Lee, Kenneth R., Lee, Yonghee, Lin, Amy, Lindeman, Neal I., Longtine, Janina A., Lopes, M. Beatriz S., Lovitch, Scott B., Maleszewski, Joseph J., Mino-Kenudson, Mari, Mutter, George L., Nucci, Marisa R., Oliveira, André M., Parast, Mana M., Perren, Aurel, Pinder, Sarah E., Pozdnyakova, Olga, Rakha, Emad A., Ro, Jae Y., Santa, Daniel J., Shen, Steven S., Sholl, Lynette M., Sipos, Bence, Speight, Paul M., Tazelaar, Henry D., Thompson, Lester D.R., VandenBerg, Scott, Wenig, Bruce M., Young, Robert H., and Zaloudek, Charles

Published
2021
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171. Scattering-Based Light-Sheet Microscopy Imaging of Human Papillomavirus–Associated Squamous Lesions of the Anal Canal: A Proof-of-Principle Study

Author

Liang, Brooke, Zhao, Jingwei, Kim, Yongjun, Barry-Holson, Keegan Q., Bingham, David B., Charville, Gregory W., Darragh, Teresa M., Folkins, Ann K., Howitt, Brooke E., Kong, Christina S., Longacre, Teri A., McHenry, Austin J., Toland, Angus M.S., Zhang, Xiaoming, Lim, Koeun, Khan, Michelle J., Kang, Dongkyun, and Yang, Eric J.

Abstract

Demand for anal cancer screening is expected to rise following the recent publication of the Anal Cancer–HSIL Outcomes Research trial, which showed that treatment of high-grade squamous intraepithelial lesions significantly reduces the rate of progression to anal cancer. While screening for human papillomavirus–associated squamous lesions in the cervix is well established and effective, this is less true for other sites in the lower anogenital tract. Current anal cancer screening and prevention rely on high-resolution anoscopy with biopsies. This procedure has a steep learning curve for providers and may cause patient discomfort. Scattering-based light-sheet microscopy (sLSM) is a novel imaging modality with the potential to mitigate these challenges through real-time, microscopic visualization of disease-susceptible tissue. Here, we report a proof-of-principle study that establishes feasibility of dysplasia detection using an sLSM device. We imaged 110 anal biopsy specimens collected prospectively at our institution’s dysplasia clinic (including 30 nondysplastic, 40 low-grade squamous intraepithelial lesion, and 40 high-grade squamous intraepithelial lesion specimens) and found that these optical images are highly interpretable and accurately recapitulate histopathologic features traditionally used for the diagnosis of human papillomavirus–associated squamous dysplasia. A reader study to assess diagnostic accuracy suggests that sLSM images are noninferior to hematoxylin and eosin images for the detection of anal dysplasia (sLSM accuracy = 0.87; hematoxylin and eosin accuracy = 0.80; P = .066). Given these results, we believe that sLSM technology holds great potential to enhance the efficacy of anal cancer screening by allowing accurate sampling of diagnostic tissue at the time of anoscopy. While the current imaging study was performed on ex vivo biopsy specimens, we are currently developing a handheld device for in vivo imaging that will provide immediate microscopic guidance to high-resolution anoscopy providers.

Published
2024
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173. Malignant tumours of the uterus and ovaries with Mullerian and germ cell or trophoblastic components have a somatic origin and are characterised by genomic instability .

Author

Acosta, Andres M, Sholl, Lynette M, Cin, Paola D, Howitt, Brooke E, Otis, Christopher N, and Nucci, Marisa R

Subjects
GERM cells, FEMALE reproductive organs, TUMORS, CELL anatomy, OVARIES, UTERUS
Abstract

Aims: Tumours of the female genital tract with a combination of malignant Mullerian and germ cell or trophoblastic tumour (MMGC/T) components are usually diagnosed in postmenopausal women, and pursue an aggressive clinical course characterised by poor response to therapy and early relapses. These clinical features suggest that MMGC/T are somatic in origin, but objective molecular data to support this interpretation are lacking. This study evaluates the molecular features of nine MMGC/T, including seven tumours containing yolk sac tumour (YST), one tumour containing choriocarcinoma and one tumour containing epithelioid trophoblastic tumour. The objectives were to: (i) investigate whether MMGC/T show a distinct genetic profile and (ii) explore the relationship between the different histological components. Methods and results: Next‐generation sequencing of paired samples demonstrated that the mutational profile of the Mullerian and non‐Mullerian components of the tumour were almost identical in all cases. Moreover, the driver mutations identified were those expected in the specific subtype of Mullerian component present in each case. In contrast, variants expected in postpubertal germ cell tumours and gestational trophoblastic tumours were not identified, and FISH for i(12p) was negative in all cases tested. In this study, mismatch repair‐proficient MMGC/T (eight of nine) were characterised by a complex copy‐number variant profile, including numerous focal, regional, arm‐level and chromosome‐level events. Conclusions: Comparison of paired samples supports that the YST and trophoblastic tumour components of MMGC/T have a somatic origin and often show numerous copy‐number variants, suggestive of underlying genomic instability. [ABSTRACT FROM AUTHOR]

Published
2020
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174. Evidence for lineage continuity between early serous proliferations (ESPs) in the Fallopian tube and disseminated high‐grade serous carcinomas

Author

Soong, Thing Rinda, primary, Howitt, Brooke E, additional, Miron, Alexander, additional, Horowitz, Neil S, additional, Campbell, Frank, additional, Feltmate, Colleen M, additional, Muto, Michael G, additional, Berkowitz, Ross S, additional, Nucci, Marisa R, additional, Xian, Wa, additional, and Crum, Christopher P, additional

Published
2018
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177. Abstract A04: Profiling DNA damage repair and immunophenotypes in BRCA1/2 mutated high-grade serous ovarian cancers

Author

Farkkila, Anniina, primary, Kochupurakkal, Bose, additional, Howitt, Brooke E., additional, Strickland, Kyle C., additional, Chowdhury, Dipanjan, additional, Shapiro, Geoffrey, additional, Gjini, Evisa, additional, Rodig, Scott J., additional, Matulonis, Ursula A., additional, Konstantinopoulos, Panagiotis, additional, and D’Andrea, Alan D., additional

Published
2018
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178. Abstract 139: DNA damage and immunoprofiling with highly multiplexed tissue immunofluorescence (t-CycIF) in high-grade serous ovarian cancer

Author

Farkkila, Anniina, primary, Chopra, Sameer S., additional, Lin, Jia-Ren, additional, Maliga, Zoltan, additional, Koruchupakkal, Bose, additional, Strickland, Kyle C., additional, Howitt, Brooke E., additional, Santagata, Sandro, additional, Matulonis, Ursula A., additional, Elias, Kevin, additional, Swisher, Elizabeth M., additional, Konstantinopoulos, Panagiotis A., additional, Sorger, Peter, additional, and D'Andrea, Alan D., additional

Published
2018
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183. Pathological Chemotherapy Response Score Predicts Survival in Patients with Advanced Ovarian Cancer Receiving Neoadjuvant Chemotherapy: Systematic Review and Meta-Analysis of Individual Patient Data

Author

Cohen, Paul, primary, Powell, Aime, additional, Böhm, Steffen, additional, Gilks, C. Blake, additional, Stewart, Colin J.R., additional, Meniawy, Tarek M., additional, Bulsara, Max, additional, Avril, Stefanie, additional, Brockbank, Elly C., additional, Bosse, Tjalling, additional, Focchi, Gustavo Rubino de Azevedo, additional, Ganesan, Raji, additional, Glasspool, Rosalind M., additional, Howitt, Brooke E., additional, Kim, Hyun-Soo, additional, Lee, Jung-Yun, additional, Lee, Nhu D., additional, Lockley, Michelle, additional, Manchanda, Ranchit, additional, Mandalia, Trupti, additional, McCluggage, W. Glenn, additional, McNeish, Iain, additional, Midha, Divya, additional, Srinivasan, Radhika, additional, Tan, Yun Yi, additional, van der Griend, Rachael, additional, Yunokawa, Mayu, additional, Zannoni, Gian F., additional, Network, HGSC CRS Collaborative, additional, and Singh, Naveena, additional

Published
2018
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184. Prospective molecular classification of endometrial carcinomas: institutional implementation, practice, and clinical experience

Author

Devereaux, Kelly A., Weiel, Julianna J., Pors, Jennifer, Steiner, David F., Ho, Chandler, Charu, Vivek, Suarez, Carlos J., Renz, Malte, Diver, Elisabeth, Karam, Amer, Litkouhi, Babak, Dorigo, Oliver, Kidd, Elizabeth A., Yang, Eric J., Folkins, Ann K., Longacre, Teri A., and Howitt, Brooke E.

Abstract

The comprehensive genomic analysis of endometrial carcinoma (EC) by The Cancer Genome Atlas (TCGA) led to the discovery of four distinct and prognostically significant molecular subgroups. Molecular classification has the potential to improve risk-stratification when integrated with clinicopathologic features and has recently been included in national and international patient management EC guidelines. Thus, the adoption of molecular classification into routine pathologic and clinical practice is likely to grow significantly in the upcoming years. Establishing an efficient and standardized workflow for performing molecular classification on ECs, and reporting both the molecular and histologic findings in an integrative manner, is imperative. Here we describe our effort to implement rapid and routine molecular classification on all ECs diagnosed at our institution. To this effect, we performed immunohistochemistry as a surrogate marker for identifying genetic and/or epigenetic alterations in DNA mismatch repair (e.g., MLH1, PMS2, MSH6, MSH2), and TP53 genes. In addition, we have developed and employed a single-gene POLESNaPshot assay, which is a rapid and analytically sensitive method for detecting select POLEexonuclease domain mutations (EDMs). We report our molecular testing workflow and integrative reporting system as well as the clinicopathologic and molecular features of 310 ECs that underwent routine molecular classification at our institution. The 310 ECs were molecularly classified as follows: 15 (5%) POLE mutant (POLEmut), 79 (25%) mismatch repair-deficient (MMRd), 135 (44%) no specific molecular profile (NSMP), and 81 (26%) p53 abnormal (p53abnl). This work provides an initial framework for implementing routine molecular classification of ECs.

Published
2021
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193. Frequency of “incidental” serous tubal intraepithelial carcinoma (STIC) in women without a history of or genetic risk factor for high-grade serous carcinoma: A six-year study

Author

Meserve, Emily E.K., primary, Mirkovic, Jelena, additional, Conner, James R., additional, Yang, Eric, additional, Muto, Michael G., additional, Horowitz, Neil, additional, Strickland, Kyle C., additional, Howitt, Brooke E., additional, and Crum, Christopher P., additional

Published
2017
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194. Prevalence of Contralateral Tumors in Patients with Follicular Variant of Papillary Thyroid Cancer

Author

Sullivan, Michael C., primary, Graham, Paul H., additional, Alexander, Erik K., additional, Ruan, Daniel T., additional, Nehs, Matthew A., additional, Gawande, Atul A., additional, Moore, Francis D., additional, Howitt, Brooke E., additional, Strickland, Kyle C., additional, Krane, Jeffrey F., additional, Barletta, Justine A., additional, and Cho, Nancy L., additional

Published
2017
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197. Prognostic importance of p16 status for women with vulvar squamous cell carcinoma (SCC) treated with radiotherapy.

Author

Lee, Larissa Janeen, primary, Howitt, Brooke E., additional, Oliva, Esther, additional, Zhang, Hongkai, additional, Catalano, Paul J., additional, Crum, Christopher, additional, Bu, Paula, additional, Cimbak, Nicole, additional, Demaria, Rebecca, additional, Murphy, Rita, additional, Horowitz, Neil S., additional, Matulonis, Ursula A., additional, and Russo, Andrea Lyn, additional

Published
2017
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199. Clear cell ovarian cancers with microsatellite instability: A unique subset of ovarian cancers with increased tumor-infiltrating lymphocytes and PD-1/PD-L1 expression

Author

Howitt, Brooke E., primary, Strickland, Kyle C., additional, Sholl, Lynette M., additional, Rodig, Scott, additional, Ritterhouse, Lauren L., additional, Chowdhury, Dipanjan, additional, D'Andrea, Alan D., additional, Matulonis, Ursula A., additional, and Konstantinopoulos, Panagiotis A., additional

Published
2017
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200. Clinicopathologic and Immunohistochemical Correlates of CTNNB1Mutated Endometrial Endometrioid Carcinoma

Author

Costigan, Danielle C., Dong, Fei, Nucci, Marisa R., and Howitt, Brooke E.

Abstract

Endometrial endometrioid carcinomas (EECs) with exon 3 CTNNB1mutations characterize a more aggressive subset of tumors in patients with low-grade low-stage disease. Thus, prospectively identifying these cases may be clinically relevant. The aim of this study was to examine the feasibility of β-catenin and Cyclin D1 immunohistochemistry to identify EECs harboring CTNNB1mutations and to evaluate the clinicopathologic features of EECs with exon 3 CTNNB1mutations. Thirty-nine CTNNB1mutated EECs and 40 CTNNB1wild-type EECs were identified from a cohort of previously sequenced endometrial carcinomas using a targeted next-generation sequencing panel. Immunohistochemistry for β-catenin and Cyclin D1 was performed on all cases. Immunohistochemistry results were correlated with CTNNB1mutation status and clinicopathologic parameters. Patients with CTNNB1mutated EECs were younger than those with CTNNB1wild-type (56.2 vs. 61.5 y; P=0.033). Nuclear β-catenin expression correlated with exon 3 CTNNB1mutation (P<0.0001) with a sensitivity of 91% and a specificity of 89%. Cyclin D1 expression correlated with CTNNB1exon 3 mutation with relatively high specificity (90%) but low sensitivity (29%). Recurrence rate in patients with stage IA disease at diagnosis was significantly higher in patients whose tumors were CTNNB1mutated compared with CTNNB1wild-type (30% vs. 0%; P=0.025) and included distant metastases; all recurrent tumors in this group harbored exon 3 mutations and were histologically low grade (5 grade 1, 2 grade 2). Nuclear β-catenin expression appears to be an acceptable proxy for CTNNB1mutation.

Published
2020
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