Global ETD Search

101	Patientens upplevelse av ett cancerbesked / Patient's experience of receiving a cancer diagnosis Nielsen, Isabell, Werner, Hanna January 2010 (has links) Varje år diagnostiseras över 50 000 individer med cancer i Sverige. Ett cancerbesked väcker blandade känslor och associeras ofta med lidande och död. Ett svårt besked kan leda till en förändrad livssituation och kan även ses som början på en lång och mödosam resa. En vetenskaplig litteraturstudie baserad på 15 originalartiklar genomfördes med syftet att belysa patientens upplevelse av ett cancerbesked och därmed öka sjuksköterskans förståelse för patientens situation samt fördjupa kunskaperna inom ämnet. Genom litteraturgranskningen identifierades tre teman: information, emotionella reaktioner samt psykosocialt stöd. Patienten upplever att det är viktigt att informationen ges på ett öppet och ärligt sätt. Vidare framkom det betydelsefullt att uppmärksamma patientens emotionella reaktioner i samband med beskedet. Eftersom upplevelsen av ett cancerbesked påverkar patientens fortsatta upplevelse av sin sjukdom, har sjuksköterskan en viktig roll att fylla genom att erbjuda psykosocialt stöd i de olika tänkbara situationer som kan uppkomma i samband med ett livsavgörande besked. Fortsatt forskning behövs för att jämföra hur de rekommendationer som finns angående delgivandet av ett svårt besked överensstämmer med patienternas egna upplevelser och önskemål. / Every year, over 50 000 individuals in Sweden are diagnosed with cancer. The disclosure of the cancer diagnosis arouses emotions and is often associated with suffering and death. Receiving bad news may lead to changes in life and can also be seen as the beginning of a long and difficult journey. A scientific study based on 15 original articles was carried out with the purpose to identify the patient’s experience of receiving a cancer diagnosis and therefore increase the nurse’s understanding for the patient’s situation and deepen the knowledge of the subject. When examining the articles three themes were identified: information, emotional reactions and psychosocial support. The patient experience that it is important that the information is given in an open and honest manner. Patients also find it important that their emotional reaction is being observed as receiving the diagnosis. As the disclosure of the cancer diagnosis affects the patient’s further perception of the disease the nurse has an important role providing psychosocial support in various situations that may arise in connection with the disclosure. Continued research is needed to compare how guidelines for giving bad news to a patient correspond with the patient’s own experiences and preferences. Cancer diagnosis Disclosure Experience Patient Cancer Cancerbesked Patient Upplevelse Cancer and Oncology Cancer och onkologi Cell and Molecular Biology Cell- och molekylärbiologi Nursing Omvårdnad
102	Extratumoral effects of highly aggressive prostate cancer / Aggressiv prostatacancer : tidig påverkan i extratumoral vävnad Strömvall, Kerstin January 2017 (has links) Prostate cancer (PC) is the most common cancer in Sweden. Most patients have slow growing tumors that will not cause them any harm within their lifetime, but some have aggressive tumors and will die from their disease. The ability of current clinical practice to predict tumor behavior and disease outcome is limited leading to both over- and undertreatment of PC patients. The men who die from their disease are those that develop metastases. It is therefore of great value to find better and more sensitive prognostic techniques, so that metastatic spread can be detected (or predicted) at an early time point, and so that appropriate treatment can be offered to each subgroup of patients. The aim of this thesis was to investigate if, and by what means, highly aggressive prostate tumors influence extratumoral tissues such as the non-malignant parts of the prostate and regional lymph nodes (LN), and also if any of our findings could be of prognostic importance. Gene- and protein expression analysis were the main methods used to address these questions. Our research group has previously introduced the expression Tumor Instructed (Indicating) Normal Tissue (TINT), and we use the term TINT-changes when referring to alterations in non-malignant tissue due to the growth of a tumor nearby or elsewhere in the body. In the Dunning rat PC-model we found that MatLyLu (MLL)-tumors, having a high metastatic ability, caused pre-metastatic TINT-changes that differ from those caused by AT1-tumors who have low metastatic ability. Prostate-TINT surrounding MLL-tumors had elevated immune cell infiltration, and gene ontology enrichment analysis suggested that biological functions promoting tumor growth and metastasis were activated in MLL- while inhibited in AT1-prostate-TINT. In the regional LNs we found signs of impaired antigen presentation, and decreased quantity of T cells in the MLL-model. One of the downregulated genes in the MLL-LNs was Siglec1 (also known as Cd169), expressed by LN resident macrophages that are important for antigen presentation. When examining metastasis-free LN tissue from PC patients we found CD169 expression to be a prognostic factor for PC-specific survival, and reduced expression was linked to an increased risk of PC-specific death. Some of our findings in prostate- and LN-TINT could be seen already when the tumors were very small suggesting that differences in TINT-changes between tumors with different metastatic capability can be detected early in tumor progression. However, before coming of use in the clinic more research is needed to better define a suitable panel of prognostic TINT-factors as well as the right time window of when to use them. / Populärvetenskaplig sammanfattning Prostatacancer är den i särklass vanligaste cancerformen hos män i Sverige. De flesta patienter har en mycket långsamt växande tumör som inte orsakar dem några större besvär under deras livstid, men enbart i Sverige dör ca 2500 patienter/år av sjukdomen. Det är först vid uppkomst av metastaser som sjukdomen blir dödlig. Befintliga diagnos- och prognosmetoder är otillräckliga när det gäller att uppskatta och förutse tumörens aggressivitet och risk för att bilda metastaser. Detta gör att vissa patienter inte får tillräcklig behandling eller behandlas försent medan andra behandlas i onödan. Behovet av förbättrad diagnostik är därför stort. Om vi kan hitta markörer för potentiellt metastaserande sjukdom, och i bästa fall också behandla innan metastaser uppstår, skulle det förbättra chansen för överlevnad markant. För att kunna växa och spridas behöver en tumör inte bara förbereda närliggande vävnader utan förmodligen hela kroppen. Vår hypotes är att potentiell dödliga tumörer sannolikt är bättre på detta än mer ofarliga. Man vet från studier av andra cancerformer att farliga tumörer orsakar förändringar i det organ dit cancern senare sprids. Dessa förändringar sker för att de tumörceller som senare anländer ska kunna överleva, och processen har fått namnet pre-metastatisk nisch. Bl.a. har man sett att immunsystemet hämmas och nybildning av kärl ökar. Det är vanligt att metastaser uppstår i närliggande lymfkörtlar innan uppkomst av metastaser i andra organ. Dock är väldigt lite känt om pre-metastatiska förändringar i lymfkörtlar eftersom den forskning som hittills är gjord främst har tittat på andra organ. Inom prostatacancer finns det förvånande få studier av premetastatiska nischer överhuvudtaget, och man vet därför inte om de alls förekommer eller vilka förändringar som i så fall sker. Vår grupp har tidigare myntat uttrycket TINT som står för Tumor Instructed (Indicating) Normal Tissue (TINT är ett engelskt verb som betyder färga) och syftar på förändringar i normal vävnad som inducerats av tumören, dvs. att tumörer färgar av sig på omgivningen. Det kan vara förändringar i normal vävnad nära tumören, som i det här fallet resten av prostatan, eller i vävnad långt ifrån tumören som till exempel regionala lymfkörtlar, lungor och benmärg. Syftet med det här avhandlingsarbetet var att undersöka TINT-förändringar inducerade av aggressiv cancer och se om dessa skiljer sig från TINT-förändringar inducerade av mindre farliga tumörer, samt att utvärdera om någon TINT-förändring skulle kunna användas för att prognostisera vilka patienter som har hög risk att få metastaser. Vi har använt oss av en prostatacancer-modell i råtta där vi analyserat genoch proteinuttryck i pre-metastatiska regionala lymfkörtlar, tumörer och prostata-TINT (dvs. prostatavävnad utanför tumören). TINT-förändringar inducerade av MatLyLu (MLL), en tumör med hög metastaserande förmåga, jämfördes mot TINT-förändringar inducerade av AT1, en snabbväxande tumör men med låg förmåga att bilda metastaser. Vi kunde vi se flera skillnader mellan modellerna. Genuttrycket i MLL-prostata-TINT indikerade en aktivering av cellulära funktioner som visat sig stimulera tumörväxt och spridning såsom celldelning, viabilitet, migration, invasion, och angiogenes (nybildning av kärl). I AT1-prostata-TINT var genuttrycket kopplat till samma funktioner men verkade istället inhibera dessa. Genom att titta på vävnaderna i mikroskop kunde vi se att MLL-tumörer rekryterade färre T-celler (som har en viktig funktion i immunsvaret mot tumören), men istället fler makrofager och granulocyter till både tumören och prostata-TINT (dessa typer av immunceller har visats kunna hjälpa tumörer att växa och sprida sig). MLL-tumörer hade också fler blodkärl och lymfkärl strax utanför tumören. I de regionala lymfkörtlarna från djur med MLL-tumörer visade genuttrycket tecken på försämrad antigenpresentation, samt immunhämning och/eller induktion av immuntolerans. Immuntolerans innebär att immuncellen inte längre reagerar mot det specifika antigen den blivit tolerant emot. Detta är vanligt förekommande hos individer med cancer och är ett sätt för tumören att undkomma immunförsvaret. I vävnadsprover av lymfkörtlarna kunde vi se färre antigenpresenterande celler, och liksom i tumörerna fanns det färre T-celler i MLL-modellen, något vi kunde se redan när tumörerna var väldigt små. CD169 är ett protein som bl.a. uttrycks av sinus-makrofager i lymfkörtlar. Dessa makrofager har en central funktion i att aktivera ett tumör-specifikt immunsvar. I råttmodellen kunde vi se att regionala lymfkörtlar från djur med MLL-tumörer hade lägre nivåer av CD169 än regionala lymfkörtlar från djur med AT1-tumörer, och då antalet sinus-makrofager visat sig ha prognostiskt värde i t.ex. tjocktarmscancer, ville vi se om det kunde vara så även i prostatacancer. Därför kvantifierade vi uttrycket av CD169 i metastasfria regionala lymfkörtlar från prostatacancerpatienter och såg att låga nivåer av CD169 medförde en ökad risk för att dö i prostatacancer. Sammantaget tyder resultaten på att MLL-tumören jämfört med AT1- tumören bättre lyckas förbereda omgivande vävnad för att gynna tumörväxt och spridning, både lokalt i prostatan men också längre bort från tumören i de regionala lymfkörtlarna. Våra fynd stämmer väl överens med aktuell tumörbiologisk forskning om hur tumörer påverkar sin omgivning. Något som inte visats tidigare är att miljön utanför tumören verkar skilja sig drastiskt beroende på tumörens metastaserande förmåga, samt att dessa skillnader går att se relativt tidigt under sjukdomsförloppet och förmodligen även långt bort från tumören. Vi har också visat att särskilt aggressiv prostatacancer verkar inducera en pre-metastatisk nisch i tumördränerande lymfkörtlar likt det som beskrivits i andra modellsystem och i andra cancertyper, men hittills inte i prostatacancer. Fler studier behövs för att bättre karaktärisera de förändringar som en potentiellt dödlig prostatacancer orsakar i andra vävnader, och för att ta reda på hur denna kunskap kan användas för att förbättra diagnostik och behandling. Prostate cancer tumor instructed normal tissue TINT non-malignant prostate tissue lymph nodes lymph node metastasis pre-metastatic niche tumor microenvironment tumor macroenvironment tumor immunoediting Dunning rat model of prostate cancer Cancer and Oncology Cancer och onkologi
103	Interactions between Rho-ROCK signaling and the tumor microenvironment in neuroblastoma Pepich, Adena January 2021 (has links) Neuroblastoma is a childhood cancer of the peripheral sympathetic nervous system, emerging from cells of the neural crest. In Sweden, neuroblastoma accounts for 20 cases out of all, 300-350, pediatric cancer cases each year (Barncancerfonden 2019, Turup on behalf of Cancer Centrum 2019). This cancer often appears in the sympathetic ganglia and/or the adrenal gland and has a high rate of metastasis that often results in morbidity (Matthay et al. 2016). Recent findings implicating a mutation in the Rho/Rac signaling pathway, a pathway involved in neural crest differentiation and migration, were found in every fourth neuroblastoma patient (Dyberg et al. 2017) These mutations tend to shift Rho to a more active state which is believed to lead to more downstream Rho-associated Kinase (ROCK) activation. While inhibition of ROCK has been seen to promote MYCN protein degradation, induce neuroblastoma cell differentiation and repress neuroblastoma growth in vitro and in vivo (Dyberg et al. 2017). Rho/ROCK signaling pathway effects on cytoskeletal arrangement and cell shape have also been suggested to be involved in tumor promoted changes of the TME (Johan and Samuel, 2018). In this master’s thesis project, we explore the effects of the Rho/ROCK pathway on the tumor microenvironment (TME) and immune response (IR) in neuroblastoma. More specifically we are focusing on populations of T cells, macrophages and fibroblasts in tumors, and looking into tumor vascular structure (such as blood vessel) and extracellular matrix (ECM) formation after ROCK inhibitor treatment within neuroblastoma tumors from transgenic mice model TH-MYCN and multi-cellular tumor spheroids (MCTS), a three-dimensional (3D) in vitro model simulating TME in neuroblastoma cell lines. Through our studies we hope to find insights into the Rho/ROCK signaling pathway and involvement of the tumor microenvironment in cancer therapy, while elucidating potential new drugs and drug targets for improving outcomes in neuroblastoma treatment. cancer and oncology pediatric cancer neuroblastoma rho/ROCK signaling rho-associated kinases tumor microenvironment cytotoxic T cells neuroblastom pediatrik onkologi rho-kinaser Cancer and Oncology Cancer och onkologi Pediatrics Pediatrik Basic Medicine
104	Differences in tumor volume for treated glioblastoma patients examined with 18F-fluorothymidine PET and contrast-enhanced MRI / Differentiering av glioblastompatienter med avseende på tumörvolym från undersökningar med 18F-fluorothymidine PET och kontrastförstärkt MR Hedman, Karolina January 2020 (has links) Background: Glioblastoma (GBM) is the most common and malignant primary brain tumor. It is a rapidly progressing tumor that infiltrates the adjacent healthy brain tissue and is difficult to treat. Despite modern treatment including surgical resection followed by radiochemotherapy and adjuvant chemotherapy, the outcome remains poor. The median overall survival is 10-12 months. Neuroimaging is the most important diagnostic tool in the assessment of GBMs and the current imaging standard is contrast-enhanced magnetic resonance imaging (MRI). Positron emission tomography (PET) has been recommended as a complementary imaging modality. PET provides additional information to MRI, in biological behavior and aggressiveness of the tumor. This study aims to investigate if the combination of PET and MRI can improve the diagnostic assessment of these tumors. Patients and methods: In this study, 22 patients fulfilled the inclusion criteria, diagnosed with GBM, and participated in all four 18F-fluorothymidine (FLT)-PET/MR examinations. FLT-PET/MR examinations were performed preoperative (baseline), before the start of the oncological therapy, at two and six weeks into therapy. Optimization of an adaptive thresholding algorithm, a batch processing pipeline, and image feature extraction algorithms were developed and implemented in MATLAB and the analyzing tool imlook4d. Results: There was a significant difference in radiochemotherapy treatment response between long-term and short-term survivors’ tumor volume in MRI (p<0.05), and marginally significant (p<0.10) for maximum standard uptake value (SUVmax), PET tumor volume, and total lesion activity (TLA). Preoperative short-term survivors had on average larger tumor volume, higher SUV, and total lesion activity (TLA). The overall trend seen was that long-term survivors had a better treatment response in both MRI and PET than short-term survivors. During radiochemotherapy, long-term survivors displayed shrinking MR tumor volume after two weeks, and almost no remaining tumor volume was left after six weeks; the short-term survivors display marginal tumor volume reduction during radiochemotherapy. In PET, long-term survivors mean tumor volumes start to decrease two weeks into radiochemotherapy. Short-term survivors do not show any PET volume reduction two and six weeks into radiochemotherapy. For patients with more or less than 200 days progression-free survival, PET volume and TLA were significantly different, and MR volume only marginally significant, suggesting that PET possibly could have added value. Conclusion: The combination of PET and MRI can be used to predict radiochemotherapy response between two and six weeks, predicting overall survival and progression-free survival using MR and PET volume, SUVmax, and TLA. This study is limited by small sample size and further research with greater number of participants is recommended. PET/MRI positron emission tomography magnetic resonance imaging brain tumor glioblastoma image segmentation adaptive thresholding feature extraction radiotracer gadolinium image processing image analysis Other Physics Topics Annan fysik Medical Image Processing Medicinsk bildbehandling Cancer and Oncology Cancer och onkologi Neurosciences Neurovetenskaper
105	VALIDERING AV MAY-GRÜNWALD GIEMSA VID FÄRGNING AV CYTOLOGIPROVER : OPTIMERING AV IN VITRO-DIAGNOSTIK, MED ANLEDNING AV NYA EU-KRAV / VALIDATION OF MAY-GRÜNWALD GIEMSA IN THE STAINING OF CYTOLOGY SAMPLES : OPTIMIZATION OF IN VITRO-DIAGNOSTICS, DUE TO NEW EU REQUIREMENTS Svantesson, Karin January 2023 (has links) VALIDERING AV MAY-GRÜNWALD GIEMSA VID FÄRGNING AV CYTOLOGIPROVEROPTIMERING AV IN VITRO-DIAGNOSTIK, MED ANLEDNING AV NYA EU-KRAVKARIN SVANTESSONSvantesson, K. Validering av May-Grünewald Giemsa vid färgning av cytologiprover. Optimering av in vitro-diagnostik, med anledning av nya EU-krav. Examensarbete i biomedicinsk laboratorievetenskap, 15 högskolepoäng. Malmö Universitet: Fakulteten för hälsa och samhälle, institutionen för Biomedicinsk vetenskap, 2023.Cancer uppstår vid onormal celldelning, men uppkommer även vid kronisk inflammation. För att kunna konstatera om patienten har cancer krävs olika typer av diagnostik, där cytologidiagnostik ingår. Med hjälp av olika färglösningar kan cancerceller i serösa vätskor färgas för att upptäckas, således kan den cancerdrabbade patienten behandlas. May-Grünwald Giemsa (MGG) ingår i Romanowsky-färgningsteknikerna och har använts sedan 1800-talet.Färglösningen ger en högkvalitativ visualisering av cellernas morfologi. Färgen används inom histologi-, hematologi- och cytologidiagnostiken. Laboratorier som arbetar med in vitro-diagnostik (IVD) måste arbeta med märkta produkter som är reglerade för IVD. År 2017 fastställdes att inom fem år skall alla laboratorier i Europeiska unionen (EU) som utför IVD, arbeta med in vitro-diagnostik reglerade (IVDR) produkter för att uppnå EU-direktiven. Syftet med studien var att optimera en ny färgblandning av MGG vid färgning av cytologiprover, så att IVDR-kraven uppfylls på Patologen i Skövde. Studien omfattade flera försök för att fastställa vilket av färgprotokollen som gav bästa kvalité på cellerna i cytologiska preparat. Under studiens gång har det även visats att olika faktorer, exempelvis färskheten av provet kan påverka infärgningens kvalité av preparatet. Gammalt eller felhanterat provmaterial kan leda till försämrad infärgning av cellerna. Resultat från studien visade att färgprotokollet Histo Lab (HL) gav goda resultat efter en modifiering av sammansättningen och tiden vid infärgning. / VALIDATION OF MAY-GRÜNWALD GIEMSA IN THE STAINING OF CYTOLOGY SAMPLESOPTIMIZATION OF IN VITRO-DIAGNOSTICS, DUE TO NEW EU REQUIREMENTSKARIN SVANTESSONSvantesson, K. Validation of May-Grünwald Giemsa in the staining of cytology samples. Optimization of in vitro-diagnostics, due to new EU requirements. Degree project in biomedical laboratory science, 15 higher education credits. Malmö University: Faculty of Health and Society, Department of Biomedical Sciences, 2023.Cancer is caused by abnormal cell division, but also occurs by chronic inflammation. In order to determine whether the patient has cancer, different types of diagnostics are required, where cytology diagnostics are included. With thehelp of different dye solutions, cancer cells in serous fluids can be stained and detected, allowing for diagnosis and treatment. May-Grünwald Giemsa (MGG) is part of the Romanowsky staining techniques and has been used since the 19th century. The dye solution provides a high-quality visualization of the cells' morphology and is used in histology-, hematology- and cytology diagnostics.Laboratories that work with in-vitro diagnostics (IVD) must use products that are in vitro-diagnostics regulated (IVDR). In 2017 it was determined that within five years all laboratories in the European Union (EU) performing IVD must work with IVDR labeled products to achieve EU directives. The aim of the study was to optimize a new dye stain of MGG for cytology samples, so that the IVDR requirements are achieved at the pathology laboratory in Skövde. The study included several attempts to determine which of the staining protocols produced the best quality of the cells in cytology preparations. During the study, it has also been shown that various factors can negatively affect the results. If sample material is too old or mishandled, it can lead to poor staining of the cells. Results from the study showed that the Histo Lab (HL) staining protocol gave goodresults after modification of the composition and time of staining. Cancer cytology diagnostics in vitro-diagnostics regulation May-Grunwald Giemsa mesothelial cells Romanowsky staining validation Cancer cytologidiagnostik in vitro-diagnostik reglering May-Grunwald Giemsa mesotelceller Romanowsky-färgning validering Biomedical Laboratory Science/Technology Cell Biology Cellbiologi Cancer and Oncology Cancer och onkologi
106	Impact of ACA’s free screening policy on colorectal cancer outcomes and cost savings : Effect of removal of out-of-pocket cancer screening fee on screening, incidence, mortality, and cost savings Togtokhjav, Oyun January 2023 (has links) Colorectal cancer is the second leading cause of cancer-related deaths worldwide as of 2020. Early detection and diagnosis of colorectal cancer can greatly increase the chances of successful treatment and can also reduce the cost of care including treatment. It’s shown in recent years that the colorectal cancer screening rates have slowed nationwide which impacts the new diagnoses of colorectal cancer (CRC) and the ability to treat it at an early stage to avoid increase in mortality rate. The purpose of this research is to examine the impact of the Affordable Care Act 2010 ‘s policy to remove colorectal cancer screening fee for adults aged 50-75 on screening, incidence, and mortality rate of colorectal cancer using panel data model and employing sequential recursive system of equations method. Since a decision to get screened is an individual’s choice, this study explores methods to increase colorectal cancer screening rate with the help of behavioral economics theories. Results of the study show that Affordable Care Act’s policy to remove colorectal cancer screening fee has a significant impact on both colorectal cancer screening and incidence rates. The ACA’s policy is associated with an increase in colorectal cancer screening rate while associating with a decrease in cancer incidence rate. Relating to the colorectal cancer mortality rate, an effort was made to examine the effect of the Affordable Care Act's policy to remove colorectal cancer screening fee on the overall cost savings resulting from lives saved. However, since this study found no significant impact of the ACA's policy on the mortality rate of colorectal cancer, further exploration in this regard was not pursued. On the other hand, studies conducted to increase colorectal cancer screening rate by applying behavioral economics methods have shown that default method with an opt-out choice and financial incentive with a loss-framed messaging methods are proven effective. Therefore, these methods can be investigated to design and implement a nationwide initiative. colorectal cancer panel data model incidence mortality affordable care act behavioral economics Cancer and Oncology Cancer och onkologi
107	Kvinnans sexuella hälsa efter mastektomi : En litteraturstudie / Women's sexual health after mastectomy : A literature study Nygård Gillberg, Lina, Södervall, Julia January 2022 (has links) Bakgrund: Bröstcancer är ett folkhälsoproblem som i Sverige drabbar cirka 9000 kvinnor årligen. Mastektomi är en behandling mot bröstcancer som orsakar stress, sorg och ångest vilket kan leda till en negativ självbild och minskad livskvalitet. Sexuell hälsa har betydelse på kvinnors generella livskvalitet och bör uppmärksammas. Syfte: Syftet var att belysa den sexuella hälsan hos kvinnor som har genomgått mastektomi efter en bröstcancerdiagnos. Metod: En litteraturstudie med en induktiv ansats, där fem artiklar var kvalitativa och sex var kvantitativa. Resultat: Tre kategorier identifierades: Kroppsuppfattningens betydelse för sexuell hälsa efter mastektomi, värdet av en förtroendefull intim relation för att återfå och bibehålla sexuell hälsa efter mastektomi och betydelsen av stöd för återhämtning från sexuell ohälsa efter mastektomi. Kvinnor som genomfört en mastektomi upplevde sexuell ohälsa i förhållande till en förändrad kroppsbild. Minskad vaginal lubrikation, smärta vid samlag och minskad sexuell lust var några av flertal problem som kvinnorna upplevde. Stöd från anhöriga och vården var väsentligt för en snabbare återhämtning. Konklusion: Kvinnor upplevde att kroppen förändrades, vilket leder till sexuell dysfunktion och sexuell ohälsa. Kvinnorna behövde ensamtid för återhämtning samtidigt som stödet från anhöriga var avgörande för läkningsprocessen. Forskning och kunskap kring sexuell ohälsa är bristande och bör uppmärksammas av hälso- och sjukvårdspersonal. / Background: Breast cancer is a public health problem that in Sweden affects approximately 9,000 women annually. Mastectomy is a treatment for breast cancer that causes stress, sadness and anxiety, which can lead to a negative self-image and reduced quality of life. Sexual health has meaning on women’s general quality of lifeand should be paid attention to. Aim: The aim was to shed light on the sexual health of women who have undergone mastectomy after a breast cancer diagnosis. Method: A literature study with an inductive approach, where five articles were qualitative andsix were quantitative. Results: Three categories were identified: The meaning of body image for sexual health after mastectomy, the value of a trustful intimate relationship to regain and maintain sexual health after a mastectomy and the importance of support for recovery from sexual ill- health after a mastectomy. Women who underwent a mastectomy experienced sexual discomfort in relation to a changed body image. Decreased vaginal lubrication, pain during intercourse and decreased sexual desire are some of many problems the women experienced. Support from relatives and care was felt to be essential for a faster healing process. Conclusion: Women experienced that the body changes in connection with mastectomy, which leads to sexual dysfunction and sexual illness. The women need time alone to recover, while the support of relatives is crucial in the healing process. Research and knowledge about sexual ill-health is lacking and should be paid attention to by healthcare professionals. body image breast cancer mastectomy sexual health sexual ill-health bröstcancer kroppsuppfattning mastektomi sexuell hälsa sexuell ohälsa Cancer and Oncology Cancer och onkologi
108	Radiotherapy treatment strategy for prostate cancer with lymph node involvement / Strålbehandlingsstrategi för prostatacancer med misstänkt involverade lymfkörtlar Östensson, Amanda January 2023 (has links) Radiotherapy is a common and useful method for treating prostate cancer, often using gold fiducial markers in the prostate as guidance. However, when there is a high risk of lymph node involvement, the independent motion of volumes causes complications in patient positioning since there is a choice between position against the gold fiducial markers or the bone anatomy. This leads to expansion of margins for either the prostate or the pelvic lymph nodes. In this thesis two different treatment strategies were performed and compared against given treatment plans. The purpose was to evaluate the standard treatment and to be able to recommend a new clinical approach for treatment of high-risk prostate cancer. Nine high-risk prostate cancer patients with their given treatment plans were used as a baseline. The patients underwent a planning CT and five CBCTs during the treatment. Two new treatment plan setups were done, a robust treatment and a sequential treatment with three and nine different plans respectively. The baseline and the robust treatment used gold fiducial markers as reference, with a prescribed dose of 2.20 Gy over 35 fractions with a VMAT. The sequential treatment used both gold fiducial markers and bone anatomy as reference, done by 35 fractions with a prescribed dose of 0.6 Gy with a single arc and 1.6 Gy with a dual arc respectively. A total of thirteen different treatment plan setups for each patient were simulated 100 times each, resulting in 11700 simulated treatments in total. The resulting simulated treatments were evaluated by the percentage passing nine different clinical goals, as well as dose and percentage volume averages for these goals. The results from the simulated robust treatments showed a decrease in percentage passing and D98 for the prostate and an increase in percentage passing and D98 for the lymph nodes and vesicles compared to the baseline. An increase in percentage passing and D98 was seen in the sequential treatment strategy for both targets compared to the baseline. The rectum had a larger percentage passing the clinical goals and a lower V69, V74 and V59 for both the robust and sequential treatment strategies. The D2 for the external were lower in the robust treatment strategy but higher in the sequential treatment strategy, while the D2 to the femoral heads were lower for both compared to the baseline treatment strategy. In conclusion, an improved dose coverage was seen in the sequential strategy with good sparing of risk organs. The robust treatment strategy showed promising results for sparing risk organs, but with a less robust dose coverage of the prostate. Radiotherapy prostate cancer lymph node gold fiducial marker multiple target Cancer and Oncology Cancer och onkologi Radiologi och bildbehandling Medical Image Processing Medicinsk bildbehandling Other Physics Topics Annan fysik
109	The receptor tyrosine kinase Met and the protein tyrosine phosphatase PTPN2 in breast cancer Veenstra, Cynthia January 2017 (has links) Breast cancer is the most common form of cancer in women worldwide and the second leading cause of cancer death. It is a heterogeneous disease and is subdivided into different subtypes, all with different treatment responses and survival outcomes. Luminal breast cancers are characterised by the expression of oestrogen receptor and generally have a good prognosis. More aggressive tumours are marked by the presence of growth stimulating receptor tyrosine kinase HER2 (HER2-like breast cancer) or the absence of oestrogen receptor, progesterone receptor, and HER2 (triple-negative breast cancer,TNBC). The latter is the most aggressive form and is difficult to treat due to lack of treatment targets. This thesis aimed to explore possible prognostic and predictive biomarkers in different subtypes and study their role in breast cancer. To this aid, breast cancer tumours of pre- and post-menopausal patients enrolled in two cohorts were analysed for gene copy numbers and expression of proteins involved in cell proliferation. Gene copy numbers of receptor tyrosine kinases MET and EGFR, Met’s ligand HGF, and protein tyrosine phosphatase PTPN2 were determined by droplet digital PCR or quantitative PCR in both cohorts. Met, phosphorylated Met (pMet), HGF, and PTPN2 protein expression levels were analysed with immunohistochemical staining in the pre-menopausal cohort. Moreover,the role of the aforementioned proteins was investigated in breast cancer cell lines. Amplification of MET, HGF, and EGFR in breast tissues was found to be low (5-8%). These three genes, all located on chromosome 7, were found to be strongly correlated with eachother and to be associated with shortened distant recurrence-free survival. High protein expression of Met, pMet, and HGF was found in 33%, 53%, and 49% of the breast tumours. MET and EGFR were found to be more often amplified in TNBC disease, correlating with worse survival. Moreover, stromal expression of HGF was associated with shorter survival in TNBC. EGF stimulation in TNBC cell line MDA-MB-468 led to inhibited cell proliferation and migration. Partial knockdown of EGFR caused TNBC cells to proliferate and migrate more upon EGF treatment, mirroring EGFR inhibitor resistance. Knockdown of Met had in part the opposite effects, indicating that Met inhibitors might be useful in the treatment of TNBC. The increase in proliferation and migration upon EGFR depletion could be counteracted with simultaneous knockdown of EGFR and Met, indicating that dual inhibition of these proteins might be a future treatment option in TNBC. Copy loss of PTPN2 was reported in 15% of the cases in both pre- and post-menopausal cohorts. Low cytoplasmic PTPN2 protein expression was found in half of the cases. Loss of PTPN2 gene or protein was associated with a shorter distant recurrence-free survival in Luminal A and HER2-positive tumours, not in TNBC, suggesting a subtype-related prognostic value of PTPN2. Subtype relevance of PTPN2 was further implied by in vitro analyses. Whereas PTPN2 knockdown had no observed effect on TNBC cell lines, knockdown in the Luminal A cell line MCF7 inhibited Met phosphorylation and promoted phosphorylation of Akt, a key regulator of cellular proliferation and survival. The cell growth and survival regulating RAS/MAPK pathway remained unaffected. Knockdown in the HER2-positive cell line SKBR3 led to increased Met phosphorylation and decreased RAS/MAPK-related Erk phosphorylation as well as EGF-mediated transcription factor STAT3 phosphorylation. These results indicate that the role of PTPN2 in breast cancer is subtype-related and needs to be further investigated for future treatment options. Cell Biology Cellbiologi Cancer and Oncology Cancer och onkologi Cell and Molecular Biology Cell- och molekylärbiologi Biochemistry and Molecular Biology Biokemi och molekylärbiologi
110	Preclinical evaluation of immunostimulatory gene therapy for pancreatic cancer Eriksson, Emma January 2017 (has links) Pancreatic cancer is characterized by its desmoplastic tumor microenvironment and the infiltration of immunosuppressive cells. It is a devastating disease where most patients are diagnosed at a late stage and the treatment options are few. The development of new treatments is surly needed. One treatment option explored is the use of immunotherapy with the intent to activate the immune system and change the balance from pro-tumor to anti-tumor. This thesis presents the idea of using oncolytic adenoviruses called LOAd-viruses that are armed with immunostimulatory- and microenvironment-modulating transgenes. For effective treatment of pancreatic cancer, the virus needs to be able to be given in addition to standard therapy, the chemotherapy gemcitabine. In paper I, the immunomodulatory effect of gemcitabine was evaluated in blood from pancreatic cancer patients receiving their first 28-day cycle of treatment with infusions day 1, 8 and 15 followed by a resting period. Gemcitabine reduced the level of immunosup-pressive cells and molecules but the effect did not last throughout the resting period. On the other hand, gemcitabine did not affect the level or proliferative function of effector T cells indicating that gemcitabine could be combined with immunotherapy. The LOAd700 virus expresses a novel membrane-bound trimerized form of CD40L (TMZ-CD40L). In paper II, LOAd700 showed to be oncolytic in pancreatic cancer cell lines as well as being immunostimulatory as shown by its capacity to activate dendritic cells (DCs), myeloid cells, endothelium, and to promote expansion of antigen-specific T cells. In paper III, LOAd703 armed with both 4-1BBL and TMZ-CD40L was evaluated. LOAd703 gave a more profound effect than LOAd700 on activation of DCs and the virus was also capable of reducing factors in stellate cells connected to the desmo-plastic and immunosuppressive microenvironment. In paper IV, LOAd713 armed with TMZ-CD40L in combination with a single-chain variable fragment against IL-6R was evaluated. The virus could kill pancreatic cancer cells lines through oncolysis and could also reduce factors involved in desmoplasia in stellate cells. Most interestingly, LOAd713 could reduce the up-regulation of PD-1/PD-L1 in DCs after CD40 activation. Taken together, LOAd703 and LOAd713 seem to have interesting features with their combination of immunostimulation and microenvironment modulation. At present, LOAd703 is evaluated in a clinical trial for pancreatic cancer (NCT02705196). Pancreatic cancer immunotherapy oncolytic viruses adenoviruses CD40L 4-1BBL IL-6 tumor microenvironment Cancer and Oncology Cancer och onkologi Immunology in the medical area Immunologi inom det medicinska området

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