Epidemiology and correlates of acquisition and clearance of ASC-US cytological abnormalities

Lau, Susie Kit Sze.

January 2008

The Papanicolaou Smear is a screening test which detects premalignant lesions of the uterine cervix. By treating these lesions, cervical cancer can be evaded. In 1988, a cytological diagnosis which communicated a state of uncertainty in the atypicality of cervical cells was first created in the Bethesda Cytology Classification scheme. This diagnosis is now known as atypical squamous cells of undetermined significance (ASC-US) and still little is known about its natural history. / This paper analyzes the results of a longitudinal study incorporating repeated regular measurements of viral and cytological endpoints as well as lifestyle and behavioural aspects, to understand the natural history of an ASC-US Pap smear and identify determinants of ASC-US acquisition and clearance. / Overall, the median duration of ASC-US is short, and is dependent on the definition of clearance since most lesions regress to normal. The factors most predictive of ASC-US acquisition but not clearance relate to HPV infection.

Vaginal Smears.

Precancerous Conditions -- pathology.

Longitudinal Studies.

Análise clinicopatológica, da expressão imunoistoquímica de KI-67, MCM 2 e geminina e da ploidia do DNA em leucoplasia verrucosa proliferativa / Clinicopathological features, DNA ploidy analysis and KI-67, MCM2 e geminin immunohistochemical expression in proliferative verrucous leukoplakia

Gouvêa, Adriele Ferreira

02 November 2011

Orientador: Marcio Ajudarte Lopes / Tese (doutorado) - Universidade Estadual de Campinas, Faculdade de Odontologia de Piracicaba / Made available in DSpace on 2018-08-17T15:24:01Z (GMT). No. of bitstreams: 1 Gouvea_AdrieleFerreira_D.pdf: 1529519 bytes, checksum: 67d58c675522b5dd769d5fcad163d152 (MD5) Previous issue date: 2011 / Resumo: Leucoplasia verrucosa proliferativa (LVP) tem como principais características acometer principalmente mulheres, com idades acima dos 60 anos, sem hábitos nocivos, com lesões multifocais, recorrentes após excisão e com altas taxas de malignização. Alguns estudos com proteínas que podem estar envolvidas no controle do ciclo celular, incluindo Mcm2 e geminina, e análise de ploidia do DNA têm sido realizados com o objetivo de identificar lesões com maior predisposição para transformação maligna. Objetivos: Determinar a correlação das características clinicopatológicas de 21 pacientes com diagnóstico de LVP a seu estado de ploidia do DNA e expressão de Ki-67, Mcm2 e geminina. Métodos: 65 amostras de biópsia de 21 pacientes com LVP e 12 amostras de mucosa oral normal foram coletados, feitas imunoistoquímicas para ki-67, Mcm2 e geminina e realizada a análise da ploidia do DNA utilizando citometria de imagem (ACIS III); Resultados: Relação mulher: homem foi de 6:1 e a média de idade foi 65,5 anos. Dos 21 casos, 17 (80,96%) não reportaram fumo ou consumo de bebidas alcoólicas. Transformação maligna foi observada em nove pacientes (42,86%), em um tempo de seguimento clínico de 7,38 anos. Dos 21 pacientes, vinte tiveram seu DNA analisado por citometria de imagem e aneuploidia foi encontrada em 95,24% dos casos. A freqüência e severidade da aneuploidia e valores médios do índice de heterogeneidade (HI) aumentaram de acordo com o aumento das anormalidades epiteliais (p<0.0001), assim como as frações excedentes de 5n (p=0.0007). Os casos que desenvolveram carcinoma não apresentaram status aneuplóide mais grave do que as outras amostras (a maioria foi moderadamente aneuplóide). Em cinco casos as biópsias iniciais apresentando hiperqueratose e acantose ou displasia leve mostraram status aneuplóides e progrediram para carcinoma (55,5%). Não houve correlação entre os graus de displasia e a expressão de das diferentes proteínas estudadas, exceto para Mcm2 (p= 0.0317). Conclusões: Estes achados associados aos altos índices de anormalidades na ploidia do DNA podem contribuir para previsão de áreas com chances de malignização e suportam a afirmação de que LVP é uma entidade de fato distinta. / Abstract: Proliferative verrucous leukoplakia (PVL) presents as main characteristics: affects mostly women, with ages over 60 years, not presenting harmful habits; presence of multifocal lesions, recurrent after excision, with high malignization rates. Some studies with proteins that may be involved in the cell cycle control, including Mcm2 and geminin, and DNA ploidy analyzis has been performed aiming to identify lesions with a greater predisposition to malignant transformation. Objectives: To determine the correlation of the clinicopathological features of 21 PVL patients with their DNA ploidy status and Mcm2, geminin and Ki-67 expression. Methods: 65 biopsy specimens of 21 PVL patients and 12 normal oral mucosa were collected; immunohistochemistry to Mcm2, geminin and ki-67 and DNA ploidy analysis using image based citometry (ACIS III) were performed. Results: Female: male ratio was of 6:1 and the average age was 65.5 years. Of the 21 PVL cases, seventeen (80.96%) did not report smoking or alcoholic habit. Malignant transformation was observed in nine patients (42.86%). Of the 21 patients, twenty had the DNA examined by an image-based cytometry and aneuploidy was found in 95.24% of the cases. The frequency and severity of aneuploidy and the mean values of DNA HI increased according to the epithelial abnormality (p<0.0001), as well the 5n exceeding fractions (p=0.0007). Cases that developed carcinoma did not presented higher ploidy status compared to the other samples (the majority was moderately aneuploidy). In five cases (55.5%), initial biopsies presenting hyperkeratosis and acanthosis or mild dysplasia showed aneuploid status and latter developed carcinoma. There was no correlation between the grades of dysplasia and the LI of different immunohistochemically studied proteins, except for Mcm2 (p= 0.0317). Conclusions: This finding associated to the high incidences of DNA ploidy abnormalities may contribute to predict areas prone to malignant transformation and to support the hypothesis that PVL is a distinct entity. / Doutorado / Patologia / Doutor em Estomatopatologia

Neoplasias bucais

Condições pré-cancerosas

Proliferação celular

Aneuploidia

Prognóstico

Mouth - Cancer

Precancerous conditions

Cell proliferation

Aneuploidy

Prognosis

Epidemiology and correlates of acquisition and clearance of ASC-US cytological abnormalities

Lau, Susie Kit Sze.

January 2008

No description available.

Longitudinal Studies.

Vaginal Smears.

Precancerous Conditions -- pathology.

Učestalost, vrsta i lokalizacija premalignih i malignih lezija kože kod bolesnika nakon transplantacije bubrega / Frequency, type and localization of premalignant and malignant skin lesions in renal transplant recipients

Roš Tatjana

27 September 2016

<p>Osobe kojima su transplantirani organi imaju povećan rizik pojave malignih oboljenja, među kojima dominiraju maligni tumori kože. Smatra se da je osnovni razlog primena imunosupresivne terapije, ali jo&scaron; nije sasvim jasan mehanizam i nivo dejstva različitih imunosupresiva. Važan uticaj na nastanak većine malignih tumora kože ima ultraljubičasto (UV) zračenje koje izaziva pojačano starenje kože u vidu histolo&scaron;ki prepoznatljivog fotoo&scaron;tećenja, sa odlikama razvoja elastoze i limfocitne infiltracije. U na&scaron;oj zemlji do sada nisu sprovođena istraživanja rizika pojave maligniteta kože kod transplantiranih pacijenata, ne postoje podaci o njihovoj incidenci, uticaju imunosupresivne terapije i drugim potencijalnim faktorima rizika. U dostupnoj literaturi nema objavljenih radova iz oblasti analize histolo&scaron;kog fotoo&scaron;tećenja kože kod osoba na imunosupresivnoj terapiji. Ciljevi ove studije preseka bili su utvrđivanje učestalosti, vrste i lokalizacije premalignih i malignih lezija kože kod pacijenata nakon transplantacije bubrega, povezanosti njihove pojave sa dužinom, vrstom i režimom primene imunosupresivne terapije i sa histolo&scaron;ki verifikovanim fotoo&scaron;tećenjem perilezionalne kože. U studiju je uključeno 66 pacijenata kojima je transplantiran bubreg (primaoci organskog transplantata &ndash; POT). Relevantni podaci su prikupljeni putem upitnika i iz medicinske dokumentacije, kliničko-dermoskopskim pregledom kože uočene suspektne lezije su bioptirane u cilju postavljanja dijagnoze i utvrđivanja histolo&scaron;kih parametara fotoo&scaron;tećenja, a u studiju su uključeni i maligni tumori kože POT ispitanika uklonjeni u periodu od prethodnih 5 godina ali nakon transplantacije. Radi komparacije prisutnih faktora rizika i stepena fotoo&scaron;tećenja kože sa op&scaron;tom populacijom formirana je kontrolna grupa (KG) ispitanika kojima je prethodno bioptirana koža, bez oboljenja bubrega i bez imunosupresije, slična po polu i životnoj dobi sa onim POT ispitanicima kojima je urađena biopsija. Za svaku leziju iz POT grupe obezbeđene su po 2 lezije iz KG, tako da je pojedinim ispitanicima POT grupe analizirano vi&scaron;e lezija, dok je u KG 1 ispitanik &ndash; 1 lezija. Osnovno oboljenje bubrega do započinjanja dijalize kod ispitanika POT grupe prosečno je trajalo 7,67 godina, u strukturi oboljenja bubrega dominirao je hronični glomerulonefritis sa 31,8%, a ispitanici su na dijalizi bili prosečno 4,54 godine. Prosečna životna dob ispitanika u momentu transplantacije iznosila je 42,5 godina, 60,6% imalo je isključivo kadaveričnu transplantaciju, a prosečno trajanje jatrogene imunosupresije iznosilo je 4,89 god. U POT grupi bioptirane su 33 lezije, među kojima su od značaja za studiju bile 2 (6,1%) aktinične keratoze (AK), 3 (9,1%) displastična nevusa (DN), 1 (3,0%) melanom (MM), 3 (9,1%) skvamocelularna karcinoma (SCK) i 6 (18,2%) bazocelularnih karcinoma (BCK). U POT grupi učestalost MM bila je 1,5%, učestalost SCK 4,5%, učestalost BCK 9,1%, dok je utvrđeni relativan rizik pojave MM u POT populaciji 227 puta veći, BCK 316 puta veći, a SCK 805 puta veći nego u op&scaron;toj populaciji. Relativan rizik nastanka AK i DN nije određen zbog izostanka zvanične registracije u op&scaron;toj populaciji. POT grupa i KG nisu se statistički značajno razlikovale po Ficpatrikovom fototipu kože, profesionalnoj izloženosti UV zračenju, upotrebi solarijuma, broju solarnih opekotina, ličnoj anamnezi malignih tumora kože i konzumiranju cigareta. Pripadnici KG su se značajno vi&scaron;e rekreativno izlagali UV zračenju, če&scaron;će koristili sredstva za za&scaron;titu od sunčevog zračenja, če&scaron;će imali bliske srodnike sa malignim tumorima kože, če&scaron;će konzumirali alkohol, značajno veći broj ispitanika KG imao je pregled kompletne kože i informaciju o merama prevencije od strane lekara, dok 50% ispitanika POT grupe nije znalo da su pod povećanim rizikom pojave maligniteta kože. U stepenu elastoze među grupama nije postojala statistički značajna razlika, dok je limfocitna infiltracija bila marginalno izrazitija u POT grupi bez obzira na vrstu lezije. U POT grupi utvrđena je statistički značajna povezanost prisustva malignog tumora sa većim stepenom perilezionalne limfocitne infiltracije i elastoze. U KG utvrđena je statistički značajna povezanost prisustva malignog tumora sa većim stepenom limfocitne infiltracije, dok nije bilo statistički značajne razlike u stepenu perilezionalne elastoze. U studiji je utvrđeno da osobe nakon transplantacije bubrega imaju statistički značajno veći rizik nastanka BCK, SCK i MM kože u odnosu na op&scaron;tu populaciju, sa najče&scaron;ćom lokalizacijom ovih tumora u predelu glave. Dužina primene imunosupresivne terapije uop&scaron;teno nije statistički značajno uticala na pojavu premalignih i malignih tumora kože, ali je kumulativna doza pojedinih imunosupresiva poput ciklosporina i azatioprina imala statistički značajan uticaj na pojavu premalignih i malignih lezija kože. Dužina imunosupresije je statistički značajno uticala na stepen elastoze, ali je imala marginalan uticaj na stepen perilezionalne limfocitne infiltracije.</p> / <p>Organ transplant recipients are at an increased risk of developing malignancies, with the predominance of malignant skin tumors. The main cause is considered to be the administration of immunosuppressive therapy, but the mechanism and effect levels of different immunosuppressive agents are still not completely clear. Ultraviolet (UV) rays also influence the development of malignant skin tumors, causing increased skin aging with histologically recognisable photo damage, with its hallmark being development of elastosis and lymphocytic infiltration. No research on the topic of risks of malignant skin tumors in transplant patients has been done in our country, there is no data on their incidence, or on the effects of immunosuppressive agents and other potential risk factors. There are also no published studies in the field of hystological photo damage analysis in patients on immunosuppressive therapy. The aims of this study were to establish the rates of occurance, types and localisation of premalignant and malignant skin lesions in kidney transplant recipients (KTR) and to associate their advent with the length, type and regimen of immunosuppressive therapy. A total of 66 KTR patients were enrolled in the study. Relevant information was gathered through a specially constructed questionnaire and from the medical records, followed by combined clinical and dermoscopic skin examination to detect suspicious lesions which were biopsied in order to determine the histopathologic diagnosis of the lesion and perilesional degree of photo damage. The study also encompassed malignant skin tumors of KTR patients that have been removed in the last 5 years, but after the transplantation. For the sake of comparison of the risk factors and the levels of photo damage with the general population, an age and sex - matched control group (CG) of patients with previous skin biopsy but without kidney disease and immunosuppression was formed. For each lesion from KTR group, 2 lesions from CG were provided, meaning that some KTR patients had several lesions analysed, whereas in the CG only 1 lesion per patient was analyzed. The average duration of underlying kidney diseases in KTR was 7,67 years, the most frequent being chronic glomerulonephritis (31,8%), and an average duration of dialysis was 4,54 years. The mean age at transplantation was 42,5 years, with 60,6% of the KTR having exclusively cadaveric graft. The mean duration of the iatrogenic immunosuppression was 4,89 years. In the KTR group a total of 33 lesions were biopsied, 2 of which were actinic keratoses (AK) (6,1%), 3 were dysplastic nevi (DN) (9,1%), 1 melanoma (MM) (3,0%), 3 squamous cell carcinomas (SCC) (9,1%) and 6 basal cell carcinomas (BCC) (18,2%). The estimated frequency of MM was 1,5%, SCC 4,5%, BCC 9,1%, and the estimated relative risk of MM in KTR being 227, BCC 316, and SCC 805 times higher compared to the general population. The relative risk of AK and DN development could not have been estimated as there are no official records in the general population. The KTR and CG were not significantly different judging by the Fitzpatrick skin phototype, occupational UV exposure, sunbed usage, personal history of skin cancers, or smoking. The controls were recreationally more exposed to UV rays, used sun protective measures more frequently, had more relatives with skin cancers and consumed alcohol more frequently. A significantly greater number of controls had had complete skin examination and protective measures counceling by the doctor, while 50% of KTR patients did not even know that they were at an increased risk of malignant skin tumor development. There was no significant difference in elastosis levels among the groups, whereas the lymphocitic infiltration was only marginally greater in the KTR group. A significant association between the level of perilesional photodamage and developement of malignant tumors was estimated for the KTR group, whereas in the CG only the perilesional lymphocitic infiltration was strongly associated to malignant lesions. The study results suggest that KTR patients have a significantly higher risk of BCC, SCC and MM development in comparison with the general population, the most common localisation being in the head region. The duration of the immunosuppressive therapy had no significant effect on the premalignant and malignant tumors development, whereas the cummulative dose of certain immunosuppressives (such as cyclosporine and azathioprine) affected the development notably. The duration of immunosuppression statistically influenced the elastosis levels, but had only a marginal influence on the perilesional lymphocitic infiltration levels.</p>

Detekcija intervalnih malignih i premalignih lezija debelog creva kod bolesnika sa urednim nalazom na inicijalnoj kolonoskopiji / Detection of malignant and premalignant colon lesions in patients with clear colon on first colonoscopy

Kukić Biljana

28 September 2016

<p>UVOD: Kolorektalni karcinom je na trećem mestu po učestalosti oboljevanja od svih karcinoma uz porast incidencije CRC u visoko razvijenim zemljama.70% obolelih od CRC je starije od 65 godina uz veću incidenciju proksimalnih karcinoma u odnosu na distalne u svim uzrasnim grupama i kod oba pola. Smatra se da bi 66-75% slučajeva CRC moglo biti izbegnuto zdravim načinom života. 75% CRC nastaje iz adenomatoznih preko polip kancer sekvence i da vi&scaron;e od 90% adenoma neće progredirati u karcinom. U studijama skrining kolonoskopija prijavljeno je 6-12% neviđenih velikih polipa i ko 5% CRC na inicijalnom kolonoskopskom pregledu. Postoperativne periodične kolonoskopije nakon operacije kolorektalonog karicinoma imaju za cilj otkrivanje metahronih carcinoma polipa kao pojavu bolesti na anastomozi ali nije dokazani benefit u preživljavanju bolesnika koji su imali učestalije postoperativne kolonoskopije (na godinu dana) u odnosu na one koji su praćenina 3 ili 5 godina. CILJEVI ISTRAŽIVANJA: Prospektivno ispitivanje pojave intervalnih lezija kolona (malignih i premalignih) u periodu od 2-7 godine od prve negativne kolonoskopije bez obzira na razlog pregleda. Ispitivanje razlike u životnim navikama između ispitanika u zavisnosti od nalaza na ponovljenoj kolonoskopiji. Retrospektivna analiza svih dijagnostičkih i kontrolnih kolonoskopija. MATERIJAL I METODE: Ponavljana je kolonoskopija kod ispitanika koj su na dijagnostičkim kolonoskopijama rađenim na Institutu za onkologiju Vojvodine u periodu 2005-2011. imali uredan kolonoskopski nalaz. Od 160 pozvanih ispitanika na ponovnu kolonoskopiju se odazvalo 64 ispitanika a 151 ispitanik je popunio upitnik o životnim navikama. Urađena je i retospektivna analiza 2750 dijagnostičkih kolonoskopija. Analizirani su rezultati 1064 prvih postoperativnih kolonoskopija kao i nalazi sa 1147 ponovljenih kolonoskopija kod ispitanika operisanih od kolorektalnog carcinoma koji su imali uredan nalaz na prvoj kolonoskopiji. REZULTATI: Od 160 pozvanih ispitanika,njih 64 (42,3%) se odazvalo na ponovni pregled (45 žena i 19 mu&scaron;karaca) prosečne starosti60,13 godina. Kod 15 ispitanika(24.3%) nađeno je ukupno 22 polipa (10 žena i 5 mu&scaron;karaca) bez statistički značajne razlike u pozitivnosti nalaza u odnosu na pol (x2test; x2=0,014; p=0,904) i pozitivnu porodičnu anamnezu (x2test; x2=0,125; p=0,724). 12 slucajeva (14,06%) su bili polipi visokog rizika: 5 (41.6%) lokalizovano u proksimalnom kolonu i 7 (58.3% ) u distalnom kolonu. Nije dijagnostikovan nijedan intervalni karcinom. Nije dokazana statistički značajna razlika u pozitivnosti nalaza na ponovljenoj kolonoskopiji u odnosu na razmak posmatran u grupama do 3 i do 5 godina od predhodne kolonoskpije (x2test; x2=0,020; p=0,887) niti ukoliko se posmatra po grupama do 5 i preko 5 godina od negative kolonoskopije (x2test; x2=3,082; p=0,079). Nema statistički značajne razlike u pozitivnosti nalaza na ponovljenoj kolonoskopiji u odnosu na to da li su pacijenti konzumiraju alkohol ili ne (x2test; x2=0,113; p=0,911) kao i u odnosu na to da li su pacijenti imali redovnu fizičku aktivnost (x2test; x2=0,476; p=0,490). Na dijagnostičkim kolonoskopijama je uočena statistički značajna razlika u uzrastu pacijenata u zavisnosti od razloga kolonoskopije (F=7,111; p=0,000) kod pacijenata kod kojih su dijagnostikovani polipi. Oni sa pozitivnom porodičnom anamnezom i polipima su statistički značajno mlađi u odnosu na ostale osim onih koji su se na pregled javili zbog bola u trbuhu poremećaja ritma stolice. Nije bilo statistički značajne razlike po polu, uzrastu, u razlogu kolonoskopije kod osoba sa dijagnostikovanim polipima. Statistički je značajniji broj žena sa lokalizacijom polipa u distalnom delu debelog creva u odnosu na proksimalni (x2test; x2=18,495; p=0,000). Kod mlađih uzrasnih grupa statistički značajnije su zastupljeni polipi u rektumu(x2test; x2=79,963; p=0,000). Ispitanici sa proksimalnom lokalizacijom polipa imaju 1,724 puta veću &scaron;ansu za adenome visokog rizika u odnosu na one sa distalnom lokalizacijom. Nema statistički značajne razlike u distribuciji karcinoma u odnosuna pol (x2test; x2=3,2110; p=0,201). Na 1064 prvih postoperativnih kolonoskopija je bilo ukupno 346 (32,5%) pozitivnih nalaza. Dijagnostikovano je 60 karcinoma od kojih je 43,3 % lokalizovano na anastomozi a kod 286 ispitanika nađeno je ukupno 546 polipa. Mu&scaron;karci statistički značajnije če&scaron;će imaju pozitiva nalaz (x2 test; x2=17,252; p=0,000). Bonferroni post hoc testom je utvrđeno da su polipi proksimalne lokalizacije statistički značajno veći od onih u rektumu (p=0,043). Na kontrolnim kolonoskopijama rađenim u cilju praćenja nakon resekcije kolorektalnog karcinoma multivarijatnom analizom ( pol, uzrast i vreme od operacije) utvrđeno je da mu&scaron;karci imaju 1,4 puta veću &scaron;ansu (OR=1,457) od žena za pojavu promena (polipa i karcinoma).Ispitanici kod kojih je od operacije pro&scaron;lo od 3 do 5 godina imaju 1,6 puta veću &scaron;ansu za pojavu promene u odnosu na one kod kojih je pro&scaron;la 1 godina (OR=1,605). ZAKLJUČAK: Kod 24.3% pregledanih ispitanika dijagnostikovani su polipi(jedan hipeplastičnii 21 adenoma ). 14,06% svih polipa je imalo karakteristike polipa visokog rizika bez statistički značajne razlike u pojavi polipa kod ispitanika kod kojih je pregled rađen 3,5 ili nakon 5 godina od prve negativne kolonoskopije. Nije dijagnostikovan niti jedan karcinom &scaron;to znači da nema potrebe za ponavljanjem kolonoskopija u kraćem vremenskom intervalu od unapred planirane kolonoskopije kod ispitanika koji su imali uredan inicijalni kolonoskopski nalaz &scaron;to se odnosi i na ponavljane kolonoskopije kod ispitanika operisanih od CRC-a. Na dijagnostičkim kolonoskopijama statistički značajniji broj žena sa lokalizacijom polipa u distalnom delu debelog creva u odnosu na proksimalni i nije zapažena razlika u distribuciji karcinoma u odnosu na pol i uzrast ispitanika.</p> / <p>INTRODUCTION:Colorectal cancer is the third most frequent illness of all carcinomas with an increase in the incidence of CRC in highly developed countries. 70% of patients with CRC are older than 65 years with higher incidence of proximal cancers compared to distal in all age groups and in both sexes. It is believed that 66-75% of CRC could be avoided through healthy lifestyle. 75% of CRC arise from adenomatous polyp cancer via sequences, and that more than 90% of adenoma will not progress to carcinoma. In studies of screening colonoscopy was reported 6-12% of unobserved large polyps and approximately 5% of the CRC on the initial colonoscopy.Postoperative periodic colonoscopy after colorectal cancer surgery aim to detect metachronous cancer and polyps and disease occurrence anastomoses but not proven survival benefit in subjects who had more frequent postoperative colonoscopy (per year) compared to those who were followed for 3 or 5 years. AIM:Prospective study of interval colon lesions occurrence (malignant and pre-malignant) in the period from 2-7 years after initial negative colonoscopy regardless of the reason for the check. Test of differences in lifestyle between subjects depending on the findings of the repeated colonoscopy.A retrospective analysis of all the diagnostic and control colonoscopy. METHODOLOGY: Repeated colonoscopy in subjects who are at-made diagnostic colonoscopy at the Oncology Institute of Vojvodina in the period 2005-2011 had normal colonoscopy findings. Of the 160 subjects invited to re colonoscopy for review responded 64 subjects and 151 subjects filled out a questionnaire about life habits. Retrospective analysis of 2750 and diagnostic colonoscopy has been done. Results of the 1064 first postoperative colonoscopy and results of the 1147 repeated colonoscopy in patients operated on for colorectal cancer that had normal findings on the first colonoscopy has been analyzed. RESULTS:Of the 160 invited subjects, 64 of them (42.3%) responded to the repeated review (45 women and 19 men), mean age 60.13 years. In 15 subjects (24.3%) found a total of 22 polyps (10 women and 5 men) with no statistically significant differences in positivity findings in relation to sex (x2test; x2 = 0.014; p = 0.904) and a positive family anamnesis (x2test; x2 = 0.125; p = 0.724).12 cases (14.06%) were high risk of polyps: 5 (41.6%) localized in the proximal colon, and 7 (58.3%) in the distal colon. Not a single interval cancer diagnosed. There was no statistically significant difference in positivity findings with repeated colonoscopy in relation to the distance observed in groups of 3 to 5 years from the previous colonoscopy (x2test; x2 = 0.020; p = 0.887) or when observed in groups up to 5 and over 5 years of negative colonoscopy (x2test; x2 = 3.082; p = 0.079). No statistically significant differences in positivity findings with repeated colonoscopy in relation to whether the patients consume alcohol or not (x2test; x2 = 0.113; p = 0.911) as well as in relation to whether patients are regularly exercising (x2test; x 2 = 0.476; p = 0.490). Statistically significant difference is confirmed in the age of patients at the diagnostic colonoscopy, depending on the reason for colonoscopy (F = 7.111; p = 0.000) in patients who were diagnosed polyps. Those with a family anamnesis and polyps were statistically significant younger in comparison to others except those who have come forward for review because of abdominal pain and bowel movement rhythm disturbances.There were no statistically significant differences by sex, age, the reason for colonoscopy in patients diagnosed with polyps.Statistically is more significant number of women with the localization of polyps in the distal part of the colon comparing to the proximal (x2test; x2 = 18,495; p = 0.000).In younger age groups are represented statistically significant polyps in the rectum (x2test; x2 = 79.963, p = 0.000). Subjects with proximal localization of polyps are 1,724 times more likely for high-risk adenomas compared to those with distal localization.No statistically significant differences in the distribution of cancer in relation to sex (x2test; x2 = 3.2110; p = 0.201).On the first postoperative colonoscopy in 1064 subjects there were a total 346 (32.5%) positive findings. 60 carcinoma diagnosed of which 43.3% is localized on the anastomosis and in 286 of the subjects had a total of 546 of the polyps.Men statistically significantly more likely to have positive findings (x2 test; x2 = 17,252; p = 0.000). Bonferroni post hoc test showed that polyps proximal localization significantly bigger than those in the rectum (p = 0.043). On the control colonoscopy-made for the purpose of monitoring after resection of colorectal cancer by multivariate analysis (sex, age and time of surgery) it has been found that men are 1.4 times more likely (OR = 1.457) than women for the occurrence of changes (polyps and cancers).Subjects having passed since the operation of 3 to 5 years are 1.6 times more likely to develop a change with respect to those in which the more than one year elapsed (OR = 1.605). CONCLUSION:In 24.3% subjects were diagnosed polyps (one hyperplastic and 21 adenomas).14.06% of all polyps had the characteristics of high-risk polyps with no statistically significant difference in the occurrence of polyps in subjects where the examination was done after 3,5 or 5 years since the first negative colonoscopy. No cancers diagnosed, meaning there is no need to repeat colonoscopy in a shorter period of time than pre-planned colonoscopy in subjects who had normal initial colonoscopy findings which refers to the repeated colonoscopies in subjects operated on for CRC.For diagnostic colonoscopy statistically significant number of women with the localization of polyps in the distal part of the colon compared to proximal and was not observed differences in the distribution of carcinoma in relation to sex and age of the subject.</p>

Analyse et méta-analyse des niveaux d'expression d'GF-R, c-erbB-2, Ki-67 et des micro-vaisseaux aux différents stades de développement des cancers bronchiques

Meert, Anne-Pascale

28 March 2007

Dans un premier temps, nous avons réalisé des revues systématiques de la littérature avec méta-analyses des données de survie. Ceci nous a conduits à sélectionner 4 marqueurs de mauvais pronostic pour la survie des CBNPC: le récepteur au facteur de croissance épidermique (EGF-R), un autre récepteur de cette famille (c-erbB-2) ainsi que deux autres facteurs potentiellement témoins de leur activité, Ki-67 (impliqué dans la prolifération) et le nombre des micro-vaisseaux (témoins de la néoangiogenèse).<p>Dans une deuxième phase, nous avons étudié au laboratoire diverses questions sur des tumeurs bronchiques invasives.<p>Premièrement, nous avons investigué le mécanisme de surexpression d’EGF-R et de c-erbB-2 et évalué si des anomalies génétiques pouvaient prédire cette surexpression, en recourant à des techniques d’immunohistochimie et de FISH. Ceci nous a permis d’observer que, si la majorité des CBNPC réséqués présentent des anomalies génétiques d’EGF-R et/ou de c-erbB-2, une amplification de ces gènes n’est présente que dans une minorité d’entre eux et n’est pas strictement corrélée à l’expression protéique. D’autre part, la survie de ces patients exprimant ou ayant une anomalie génique d’EGF-R et/ou c-erbB-2 est plus courte sans atteindre le seuil de signification statistique.<p>Deuxièmement, nous avons recherché sur des tumeurs opérées d’éventuels liens entre les expressions d’EGF-R, de c-erbB-2 et de Ki-67. Aucune corrélation n’a été mise en évidence entre l’expression de ces 3 facteurs. Par contre, chez ces patients, l’expression de Ki-67 dans la tumeur s’est avérée être un facteur de mauvais pronostic pour la survie.<p>Troisièmement, nous avons voulu savoir si un de ces marqueurs (EGF-R) présentait une valeur pronostique dans un groupe plus restreint de tumeurs plus avancées, les CBNPC de stade III. Pour mener cette recherche sur des biopsies, nous avons d’abord démontré que l’évaluation des marqueurs biologiques (EGF-R, c-erbB-2 et Ki-67) sur biopsie ne différait pas de celle réalisée sur des tumeurs réséquées. Comme les résultats étaient équivalents, nous avons pu étudier EGF-R sur les biopsies de CBNPC au stade III et montrer qu’EGF-R n’était pas un facteur pronostique pour la survie dans ce groupe assez homogène de tumeurs avancées.<p>Dans la dernière phase, nous avons étudié des lésions représentatives des différents stades prénéoplasiques et néoplasiques précoces radiooccultes. Ces lésions ont été prélevées lors d’examens endoscopiques de photodétection. EGF-R, c-erbB-2, Ki-67 et le nombre des micro-vaisseaux ont été étudiés par immunohistochimie dans ces différents stades de lésions prénéoplasiques et néoplasiques précoces. Nous avons observé qu’EGF-R et Ki-67 sont statistiquement plus exprimés dans les dysplasies sévères et les carcinomes in que dans les dysplasies légères suggérant que, au moins pour ces 2 marqueurs, les dysplasies sévères se rapprochent plus des carcinomes in situ que des dysplasies légères. Alors que l’expression d’EGF-R est présente dès le stade de dysplasie sévère, une augmentation du nombre des micro-vaisseaux n’est présente qu’au stade de tumeurs micro-invasives. C-erbB-2 n’est quant à lui pas exprimé dans ces lésions bronchiques prénéoplasiques et néoplasiques précoces. <p>En conclusion, les facteurs biologiques, EGF-R, c-erbB-2 et Ki-67 et le nombre des micro-vaisseaux s’avèrent des facteurs de mauvais pronostic dans le CBNPC. La surexpression d’EGF-R et de c-erbB-2 dans les cancers réséqués résulte très rarement d’une amplification génique et nous n’avons pas trouvé dans ces tumeurs de corrélation entre l’expression des marqueurs moléculaires étudiés. Dans les tumeurs plus avancées de stade III, EGF-R n’est pas un facteur discriminant pour le pronostic. Les anomalies de certains de ces marqueurs (EGF-R et Ki-67) apparaissent précocement, dès les stades prénéoplasiques, avec un seuil se situant entre les lésions bronchiques de bas et de haut grades. La néoangiogénèse, évaluée par le nombre des micro-vaisseaux, s’observe à partir des cancers micro-invasifs tandis que c-erbB-2 n’apparaît qu’au stade invasif. Dans la séquence d’apparition des anomalies génétiques conduisant au cancer invasif, l’atteinte d’EGF-R précède la néoangiogénèse.<p> / Doctorat en sciences médicales / info:eu-repo/semantics/nonPublished

Médecine pathologie humaine

Bronchi -- Cancer

Bronchi -- Cancer -- Etiology

Bronchi -- Precancerous conditions

Neovascularization

Bronches -- Cancer

Bronches -- Cancer -- Etiologie

Bronches -- Etats précancéreux

Néovascularisation

carcinogenèse bronchique

Ki-67

angiogenèse

c-erbB-2

EGF-R

lésions prénéoplasiques

cancer bronchique

Rastreamento da displasia anal em pacientes infectados pelo HIV: há concordância entre o estregaço anal e a biópsia guiada por anuscopia de alta resolução? / Screening anal dysplasia in HIV-infected patients : is there an agreement between anal pap smear and high resolution anoscopy guided biopsy?

Nahas, Caio Sergio Rizkallah

19 April 2012

OBJETIVO: O objetivo deste estudo foi analisar a concordância entre o esfregaço anal e a biópsia guiada por anuscopia de alta resolução no diagnóstico da displasia anal em pacientes infectados pelo HIV. MÉTODO: Conduzimos uma análise transversal de pacientes infectados pelo HIV submetidos a rastreamento de displasia anal rotineiro. A concordância entre mensurações foi estimada por índice de kappa ponderado através de sistema de avaliação citológica e histológica de três categorias (normal, displasia de baixo grau, e displasia de alto grau). Estimativas de sensibilidade, especificidade e valores preditivos foram calculados através de sistema de avaliação citológica e histológica de duas categorias (ausência de displasia e displasia de qualquer grau). Estimativas foram calculadas também para a detecção de displasia de alto grau. RESULTADOS: No decorrer de um ano, 222 pacientes foram submetidos a 330 esfregaços anais seguidos de biópsias guiadas por anuscopia de alta resolução. Trezentos e onze (311) esfregaços com biópsias concomitantes foram satisfatórios. Considerando-se a histologia como padrão, a freqüência de displasia anal foi de 46%. O índice kappa ponderado para concordância entre o esfregaço anal e a biópsia foi de 0,20. Para detecção de displasia anal de qualquer grau, o esfregaço anal demonstrou sensibilidade de 61%, especificidade de 60%, valor preditivo positivo de 56% e valor preditivo negativo de 64%. Para displasia de alto grau, o esfregaço anal demonstrou sensibilidade de 16% e especificidade de 97%. CONCLUSÃO: Os resultados obtidos no presente estudo, em que comparamos os achados da citologia dos esfregaços com os achados histológicos das biópsias dirigidas pela anuscopia de alta resolução em pacientes infectados pelo HIV permitiram concluir que houve baixa concordância entre eles / Purpose: To analyze the agreement between anal Pap smear and high resolution anoscopy guided biopsy to diagnose anal dysplasia in HIV-infected patients. Methods: Cross sectional analysis of HIV-infected patients receiving anal dysplasia screening as part of routine care. Agreement between measures was estimated by weighted kappa-statistics, using 3-tiered cytologic and histologic grading system (normal, low grade dysplasia, and high grade dysplasia). Estimates of sensitivity, specificity, and predictive values were calculated using a 2-tiered cytologic and histologic grading system (without dysplasia, and with dysplasia of any grade). Estimates were also calculated for the detection of high grade dysplasia. Results: Two hundred and twenty-two patients underwent 330 anal Pap smears followed by high resolution anoscopy guided biopsies in one year period. There were 311 satisfactory Pap smears with concurrent biopsy. Considering histology the standard, the frequency of anal dysplasia was 46 percent (95 percent confidence interval: 40-51 percent). Kappa-agreement between anal Pap smear and biopsy was 0.20 (95 percent confidence interval: 0.10 0.29). Anal Pap smear showed sensitivity of 61 percent, specificity of 60 percent, positive predictive value of 56 percent, and negative predictive value of 64 percent for detection of anal dysplasia of any grade. For high grade dysplasia, anal Pap smear showed sensitivity of 16 percent, and specificity of 97 percent. Conclusion: The present study showed a low concordance between anal Pap smears and high resolution anoscopy-guided biopsy

Anal canal

Anus diseases

Anus neoplasms

Biópsia

Biopsy

Canal anal

Carcinoma de células escamosas

Carcinoma in situ

Carcinoma in situ

Carcinoma squamous cell

Cervical intraepithelial neoplasia

Citodiagnóstico

Colposcopia

Colposcopy

Cytodiagnosis

Cytological techniques

Diagnosis

Diagnóstico

Doenças do ânus

Doenças sexualmente transmissíveis

Esfregaço vaginal

HIV seropositivity

Homosexuality

Infecções por papillomavirus

Lesões pré-cancerosas

Neoplasia intra-epitelial cervical

Neoplasias do ânus

Papillomavirus infections

Precancerous conditions

Sexualidade

Sexually transmitted diseases

Soropositividade para HIV

Técnicas citológicas

Vaginal smears

Rastreamento da displasia anal em pacientes infectados pelo HIV: há concordância entre o estregaço anal e a biópsia guiada por anuscopia de alta resolução? / Screening anal dysplasia in HIV-infected patients : is there an agreement between anal pap smear and high resolution anoscopy guided biopsy?

Caio Sergio Rizkallah Nahas

19 April 2012

OBJETIVO: O objetivo deste estudo foi analisar a concordância entre o esfregaço anal e a biópsia guiada por anuscopia de alta resolução no diagnóstico da displasia anal em pacientes infectados pelo HIV. MÉTODO: Conduzimos uma análise transversal de pacientes infectados pelo HIV submetidos a rastreamento de displasia anal rotineiro. A concordância entre mensurações foi estimada por índice de kappa ponderado através de sistema de avaliação citológica e histológica de três categorias (normal, displasia de baixo grau, e displasia de alto grau). Estimativas de sensibilidade, especificidade e valores preditivos foram calculados através de sistema de avaliação citológica e histológica de duas categorias (ausência de displasia e displasia de qualquer grau). Estimativas foram calculadas também para a detecção de displasia de alto grau. RESULTADOS: No decorrer de um ano, 222 pacientes foram submetidos a 330 esfregaços anais seguidos de biópsias guiadas por anuscopia de alta resolução. Trezentos e onze (311) esfregaços com biópsias concomitantes foram satisfatórios. Considerando-se a histologia como padrão, a freqüência de displasia anal foi de 46%. O índice kappa ponderado para concordância entre o esfregaço anal e a biópsia foi de 0,20. Para detecção de displasia anal de qualquer grau, o esfregaço anal demonstrou sensibilidade de 61%, especificidade de 60%, valor preditivo positivo de 56% e valor preditivo negativo de 64%. Para displasia de alto grau, o esfregaço anal demonstrou sensibilidade de 16% e especificidade de 97%. CONCLUSÃO: Os resultados obtidos no presente estudo, em que comparamos os achados da citologia dos esfregaços com os achados histológicos das biópsias dirigidas pela anuscopia de alta resolução em pacientes infectados pelo HIV permitiram concluir que houve baixa concordância entre eles / Purpose: To analyze the agreement between anal Pap smear and high resolution anoscopy guided biopsy to diagnose anal dysplasia in HIV-infected patients. Methods: Cross sectional analysis of HIV-infected patients receiving anal dysplasia screening as part of routine care. Agreement between measures was estimated by weighted kappa-statistics, using 3-tiered cytologic and histologic grading system (normal, low grade dysplasia, and high grade dysplasia). Estimates of sensitivity, specificity, and predictive values were calculated using a 2-tiered cytologic and histologic grading system (without dysplasia, and with dysplasia of any grade). Estimates were also calculated for the detection of high grade dysplasia. Results: Two hundred and twenty-two patients underwent 330 anal Pap smears followed by high resolution anoscopy guided biopsies in one year period. There were 311 satisfactory Pap smears with concurrent biopsy. Considering histology the standard, the frequency of anal dysplasia was 46 percent (95 percent confidence interval: 40-51 percent). Kappa-agreement between anal Pap smear and biopsy was 0.20 (95 percent confidence interval: 0.10 0.29). Anal Pap smear showed sensitivity of 61 percent, specificity of 60 percent, positive predictive value of 56 percent, and negative predictive value of 64 percent for detection of anal dysplasia of any grade. For high grade dysplasia, anal Pap smear showed sensitivity of 16 percent, and specificity of 97 percent. Conclusion: The present study showed a low concordance between anal Pap smears and high resolution anoscopy-guided biopsy

Biópsia

Canal anal

Carcinoma de células escamosas

Carcinoma in situ

Citodiagnóstico

Colposcopia

Diagnóstico

Doenças do ânus

Doenças sexualmente transmissíveis

Esfregaço vaginal

Infecções por papillomavirus

Lesões pré-cancerosas

Neoplasia intra-epitelial cervical

Neoplasias do ânus

Sexualidade

Soropositividade para HIV

Técnicas citológicas

Anal canal

Anus diseases

Anus neoplasms

Biopsy

Carcinoma in situ

Carcinoma squamous cell

Cervical intraepithelial neoplasia

Colposcopy

Cytodiagnosis

Cytological techniques

Diagnosis

HIV seropositivity

Homosexuality

Papillomavirus infections

Precancerous conditions

Sexually transmitted diseases

Vaginal smears

Chemoprevention for Colorectal Cancer

Krishnan, K, Ruffin, M T., Brenner, D E.

01 March 2000

No description available.

adenoma (genetics

pathology)

animals

anti-inflammatory agents

non-steroidal (therapeutic use)

antioxidants (therapeutic use)

apoptosis

arachidonic acids (metabolism)

bile acids and salts (metabolism)

biomarkers

calcium (therapeutic use)

cell cycle

cell transformation

neoplastic (chemically induced)

clinical trials as topic

colonic polyps (genetics

pathology)

colorectal neoplasms (genetics

pathology

prevention & control)

dna methylation

DNA repair (genetics)

eflornithine (therapeutic use)

enzyme inhibitors (therapeutic use)

estrogens (pharmacology

therapeutic use)

genetic predisposition to disease

humans

mice

ornithine decarboxylase inhibitors

patient compliance

patient selection

polyamines (metabolism)

precancerous conditions (metabolism

pathology)

pyrazines (therapeutic use)

rats

retinoids (therapeutic use)

thiones

thiophenes

tumor cells

cultured

vitamins (therapeutic use)

Internal Medicine