The Supreme Court should invalidate the patent on human DNA - The Washington Post

Article

"....the Supreme Court has a chance to rectify this genetic injustice. The justices will hear oral argument April 15 over a lower federal court’s decision that human genes can be patented. The case involves Myriad Genetics, which received patents in the 1990s for the exclusive right to examine any isolated DNA that contains the BRCA1 and BRCA2 genes.....

".....Like many scientists, we believe that these patents never should have been granted and that the genes of the human genome, like other natural body parts, belong to their owners, not to companies seeking to exploit monopolies. If the court allows these types of patents to stand, it will put the endeavors of openly researching, preventing and treating lethal diseases on a lower level of importance than a set of ill-conceived property rights.
Because of Myriad’s patents, any American who wants to have his or her DNA tested for the potentially life-threatening BRCA mutations has to use the services of Myriad Genetics. There is no possibility of an independent test. Myriad charges about $3,000 for the testing, but hundreds of clinical laboratories nationwide could do it for less than $200......

Characteristics of Opioid-Users Whose Death Was Related to Opioid-Toxicity

open access

Background

The impact of the prescription opioid public health crisis has been illustrated by the dramatic increase in opioid-related deaths in North America. We aimed to identify patterns and characteristics amongst opioid-users whose cause of death was related to opioid toxicity.

Results

Out of 2330 drug-related deaths in Ontario, 58% were attributed either in whole or in part, to opioids (n = 1359). Oxycodone was involved in approximately one-third of all opioid-related deaths. At least 7% of the entire cohort used opioids that were prescribed for friends and/or family, 19% inappropriately self-administered opioids (injection, inhalation, chewed patch), 3% were recently released from jail, and 5% had been switched from one opioid to another near the time of death. Accidental deaths were significantly associated with personal history of substance abuse, enrollment in methadone maintenance programs, cirrhosis, hepatitis, and cocaine use. Suicides were significantly associated with mental illness, previous suicide attempts, chronic pain, and a history of cancer.

Non-medical use of prescription opioids has culminated in a public health crisis in many North American jurisdictions. The impact of this crisis has been powerfully illustrated by the dramatic increase in opioid-related deaths [1]–[6]: in 2008, prescription opioids were involved in 14,800 accidental deaths in the United States [4]. That there has been a parallel increase in the consumption of prescription opioids and deaths related to opioid drugs is not in dispute......

Genetically modified foods, cancer, and diet: myths and reality

Blogger's Note: debates continue over genetically modified foods; acknowledging the pro's/con's it is (also) important to understand the issues for those countries who suffer from food security

Article

INTRODUCTION

This commentary deconstructs, discredits, and demystifies the paradigm that eating genetically modified foods causes cancer, and appraises the research protocols needed to substantiate claims for cancer therapy.

CONCLUDING REMARKS

Avoiding gmfs will neither stop nor prevent carcinogenesis. Healthy eating from modern mass food production demands informed choice to realize the full benefits of nutrition and to eschew co-factors for cancer. Vaccination against known causes is desirable, and complementary therapies help to palliate cancer morbidity. Scientists are free to express their ideas, but they bear a responsibility to be objective and to provide a full, open, rational, and transparent account of any research evidence procured to substantiate their views.

That is no myth, it’s reality.

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CONFLICT OF INTEREST DISCLOSURES

The author has no financial conflicts of interest to declare

Can treatment success with 5% lidocaine medicated plaster be predicted in cancer pain with neuropathic components or trigeminal neuropathic pain?

Abstract

open access - New perspectives on molecular targeted therapy in ovarian clear cell carcinoma

open access

There is now compelling evidence to suggest that epithelial ovarian cancers (EOCs) represent a heterogeneous group of tumours with distinct subtypes having different tissues of origin, molecular characteristics and outcome (Kurman and Shih, 2010). In Western populations, ovarian clear cell carcinomas (OCCCs) account for about 5–13% of all EOCs (Chan et al, 2008; McCluggage, 2008), whereas in Japan, its prevalence rises to 15–25% (Sugiyama et al, 2000; Itamochi et al, 2008) of all EOCs. It is currently unclear why OCCCs are more common in women of oriental descent, but, regardless of ethnicity, OCCCs have been shown to be associated with a poorer prognosis and are relatively resistant to conventional platinum-based chemotherapy when compared with other EOC subtypes (Tan and Kaye, 2007)......

"....These data suggest that OCCCs are genomically heterogeneous and that the pattern and complexity of genome-wide copy number aberrations are not only of taxonomic interest, but may also underpin the phenotypic differences in OCCCs with regard to clinical outcome. Indeed, it would appear that subgroups of OCCCs may harbour specific copy number changes that render them more chemoresistant than other OCCCs (Tan et al, 2011)......

Anticancer drugs might lead to bone metastasis, according to study

Article

 "...While the compounds are currently being tested in Phase I and II trials, the authors are concerned that the long-term side effects of bone degradation and metastasis might not be noticed: Chang Yang, first author of the study, (Washington University School of Medicine) is wary that “these trials do not necessarily look for long-term effects of the drugs.” Continuing to explain this, Yang mentions that “if the cancer is going to metastasize to bone, it may take 6 months to 2 years to see that outcome. This may not be seen during the clinical trial.”....

Patents Associated with High-Cost Drugs in Australia

open access

"....Our findings show that a multitude of players seek monopoly control over innovations to blockbuster drugs. Consequently, attempts to control drug costs by mitigating misuse of the patent system are likely to miss the mark if they focus only on the patenting activities of originators......

Ovarian Cancer Research from the SGO Annual Meeting | Ovarian Cancer National Alliance

Report

BRAF V600E-specific immunohistochemistry for the exclusion of Lynch syndrome in MSI-H colorectal cancer

Abstract

The differentiation between hereditary and sporadic microsatellite-unstable (MSI-H) colorectal cancer is a crucial step in Lynch syndrome diagnostics. Within MSI-H colorectal cancers, the BRAF V600E mutation is strongly associated with sporadic origin.

Evolving concepts in the management of drug resistant ovarian cancer: Dose dense chemotherapy and the reversal of clinical platinum resistance

Abstract

"Despite the initially high response rate to standard front-line debulking surgery followed by platinum-based chemotherapy, the relapse rate in ovarian cancer is high and many patients will recur within 6 months of completing platinum based treatment. These patients may still require further chemotherapy despite being considered “platinum resistant”. In this setting, response rates to conventionally scheduled second line platinum and non-platinum agents is low, ranging between 5% and 15%. There is an emerging body of evidence that in this scenario, chemotherapeutic activity can be enhanced using unconventionally scheduled “dose-dense” platinum and non-platinum based regimens with improved response rates of up to 65%. Randomised studies to evaluate the impact of this approach on survival in recurrent, platinum resistant disease are urgently required to confirm the promising phase II findings if there is to be a change in the standard of care of patients with platinum resistant disease. In this review we discuss the evolving strategies to overcome resistance in patients with platinum resistant ovarian cancer with a particular focus on alterations in dose schedule as a means of reversing platinum resistance."

(2012) Immunoexpression and prognostic role of p53 in different subtypes of epithelial ovarian carcinoma

Abstract

"We sought to investigate the significance of p53 expression for epithelial ovarian carcinoma. In this study, we used immunohistochemical method to investigate the expression patterns of p53 in different subtypes of epithelial ovarian carcinoma. We found that the expressions of p53 protein in epithelial ovarian cancer (pituita, serosity and intima) were 88.9%, 75% and 100%, respectively, while the recurrence rates among three cancer subtypes were significantly different (33.3%, 12.5% and 0%, respectively; P < 0.05). Compared with patients without lymph node metastasis, the expression of p53 in patients with lymph node metastasis was significantly strong (68.75% and 100%, respectively; P < 0.05). However, the recurrence rate in the patients with lymph node metastasis (40%) was higher than that without lymph node metastasis (6.25%, P < 0.05). The expressions of p53 protein in ovarian cancer between I-II (25%) stage and II-IV stage (100%) were significantly different (P < 0.05), and the recurrence rates between the two groups were significantly different (0% and 31.25%, respectively, P < 0.05). Therefore, p53 protein has an intimate relationship with the malignant degree and the prognosis of ovarian cancer."

Discovery Analysis of TCGA Data Reveals Association between Germline Genotype and Survival in Ovarian Cancer Patients

open access

Conclusions

"Discovery analysis of TCGA data reveals germline genetic variations that may play a role in ovarian cancer survival even among late-stage cases. The significant loci are located near genes previously reported as having a possible relationship to platinum and taxol response. Because the variant alleles at the significant loci are common (frequencies for rs4934282 A/C alleles = 0.54/0.46, respectively; rs1857623 A/G alleles = 0.55/0.45, respectively) and germline variants can be assayed noninvasively, our findings provide potential targets for further exploration as prognostic biomarkers and individualized therapies......

PLOS ONE: Expression of the Glioma-Associated Oncogene Homolog 1 (Gli1) in Advanced Serous Ovarian Cancer Is Associated with Unfavorable Overall Survival

open access

"Recent evidence links aberrant activation of Hedgehog (Hh) signaling with the pathogenesis of several cancers including medulloblastoma, glioblastoma, melanoma as well as pancreas, colorectal, and prostate carcinomas. Here we investigated the role of the transcription factor Gli1 in ovarian cancer. To this end, the expression profile of Gli1 was examined in normal ovaries, ovarian tumors, and ovarian cancer cell lines, and the in vitro effects of a specific Hh-pathway blocker, KAAD-cyclopamine, or a specific Gli1 inhibitor (GANT58) on cell proliferation and on Hh target gene expression were also assessed. Results obtained showed that epithelial cells in ovarian cancer tissue express significantly higher levels of nuclear Gli1 than in normal ovarian tissue, where the protein was almost undetectable.....

Fertility drug use and the risk of ovarian tumors in infertile women: a case-control study

Abstract

Objective

To assess the influence of infertility and fertility drugs on risk of ovarian tumors.

Design

Case-control study (Mayo Clinic Ovarian Cancer Study).

Setting

Ongoing academic study of ovarian cancer.

Patient(s)

A total of 1,900 women (1,028 with ovarian tumors and 872 controls, frequency matched on age and region of residence) who had provided complete information in a self-report questionnaire about history of infertility and fertility drug use.

Intervention(s)

None.

Main Outcome Measure(s)

Effect of infertility history, use of fertility drugs and oral contraception, and gravidity on the risk of ovarian tumor development, after controlling for potential confounders.

Result(s)

Among women who had a history of infertility, use of fertility drugs was reported by 44 (24%) of 182 controls and 38 (17%) of 226 cases. Infertile women who used fertility drugs were not at increased risk of developing ovarian tumors compared with infertile women who did not use fertility drugs; the adjusted odds ratio was 0.64 (95% CI, 0.37, 1.11). The findings were similar when stratified by gravidity and when analyzed separately for borderline versus invasive tumors.

Conclusion(s)

We found no statistically significant association between fertility drug use and risk of ovarian tumors. Further larger, prospective studies are needed to confirm this observation.

Risk-Reducing Appendectomy and the Elimination of BRCA1 -Associated Intraperitoneal CancerRisk-Reducing Appendectomy in BRCA1 Carriers

JAMA - abstract

Risk-reducing bilateral salpingo-oophorectomy (RRBSO) and risk-reducing mastectomy are widely used for BRCA1 and BRCA2 mutation carriers to reduce the risk of ovarian and breast cancer. To our knowledge, no risk-reduction therapy has addressed the BCRA1/2 carrier lifetime risk of intra-abdominal peritoneal carcinoma from an appendix source. We identified a BRCA1 carrier in a hereditary breast and ovarian cancer kindred who developed a low-grade malignant appendiceal mucocele 2 years after risk-reducing salpingo-oophorectomy. Our retrospective meta-analysis assessed the risk of intraperitoneal appendiceal cancer in BRCA1/2 carriers after RRBSO to determine whether elective risk-reduction appendectomy could reduce the incidence of intraperitoneal cancer. Data sources included the case report and 12 reports of BRCA1 and BRCA2 carriers after RRBSO with ovarian, fallopian tube, breast, and peritoneal cancer published from January 1, 1985, through April 30, 2012. Main outcome measures were nonovarian, non–fallopian tube, nonbreast, positive intra-abdominal peritoneal carcinoma in previously cancer-free BRCA1/2 carriers after RRBSO. The source of intraperitoneal cancer in BRCA1/2 carriers after risk-reducing salpingo-oophorectomy is highly likely the appendix. Use of risk-reduction appendectomy with RRBSO in younger BRCA1/2 carriers may reduce lifetime risk of malignant tumor and eliminate intraperitoneal cancer.

Countercurrents: Editorial - A new kind of breast / ovarian cancer gene mutation | Narod | Current Oncology

Article

 S.A. Narod , MD
doi: http://dx.doi.org/10.3747/co.20.1403

" So, is it helpful to add PPM1D to the growing panel of ovarian cancer susceptibility genes?"

"A fascinating article, recently published in Nature and titled “Mosaic PPM1D Mutations Are Associated with Predisposition to Breast and Ovarian Cancer” by Nazneen Rahman and her colleagues1, is a rare example of a discovery that causes a re-evaluation of our assumptions about cancer and cancer genes.

The authors set out along a path well-travelled, intending to look for rare but highly penetrant gene mutations that might help to explain some of the residual heritability in breast and ovarian cancer—that is, to explain cancer families without a BRCA mutation. They used next-generation sequencing to study a panel of 507 genes connected in some shape or form to dna repair. The experiment was an extension of earlier work, made possible by the new technology. The project was facilitated by the collection of 13,462 dna samples from many patients over many years (attesting to the prescience of the British funding authorities; I suspect that this particular experiment was never detailed in full in a grant proposal)........

"In the analysis, one gene stood out: PPM1D (p53-inducible protein phosphate) outranked all the others by sheer statistical force. A PPM1D mutation was found in 18 of 6912 women with breast cancer, in 12 of 1121 women with ovarian cancer, but in only 1 of 5861 control subjects...........First, from a clinical point of view, the risk for ovarian cancer with PPM1D mutation (although not precisely known) looks to be as high as that determined for any risk factor or gene mutation yet discovered. The lifetime risk for a mutation carrier exceeds 60%, and so a preventive oophorectomy is in order. The PPM1D gene appears to be responsible for about 1% of ovarian cancers—fewer than BRCA1 or BRCA2, but comparable to the mismatch repair genes, RAD51C and RAD51D. The clinical scenario is much different, however......

Many mosaic mutations | Foulkes | Current Oncology

article

"Steven Narod’s latest Countercurrents contribution to Current Oncology discusses a new breast and ovarian cancer susceptibility gene known as PPM1D 1. In this accompanying editorial, we put this exciting new finding in context.

MOSAICISM: WHAT IS IT AND HOW DOES IT HAPPEN?

Genetic mosaicism, as the name implies, indicates that the person is a mosaic—that is, composed of more than one genotype. At the time of diagnosis, all cancer patients are mosaics. They are mosaics because they comprise at least two distinct genomes: the genome they were born with, and the genome that they unwillingly acquired as a result of the initiation and growth of cancer. In fact, as discussed next, it may be that all humans are mosaics—but that some of us are more mosaic than others......

media: Ontario wants independent probe into diluted cancer drugs

media

TORONTO - "Ontario will appoint an independent third party to review how watered down chemotherapy drugs were given to more than 1,100 patients, some for as long as a year, Premier Kathleen Wynne said Thursday. “It’s unacceptable that this should have happened, that the doses would not have been accurate,” said Wynne (premier of province).....

" The five hospitals are contacting affected patients to arrange quick appointments with their oncologists. Family members of Ontario patients who died are also being contacted."

"Health Canada, the provincial governments, Cancer Care Ontario and the Ontario College of Pharmacists are investigating. The hospitals are also conducting their own probes."

"Since hospitals buy the drugs, Cancer Care Ontario (Sawka) doesn’t know how many of them mix the drugs themselves or have it done off site, she said."

'" The supplier, Marchese Hospital Solutions, suggested the problem wasn’t how the drugs were prepared, but how they were administered at the hospitals."

Research Recruitment Practices of Critically Ill Patients: A Multicenter, Cross-Sectional Study (The Consent Study)

Abstract
Critical Care Medicine, St. Michael's Hospital, Toronto, Canada, Toronto, Canada.

RATIONALE:

Limited cross-sectional data exist to characterize the challenges of enrolling critically ill patients into research studies.

OBJECTIVES:

We aimed to describe recruitment practices, document factors that impact recruitment, and identify factors that may enhance future research feasibility.

METHODS:

We conducted a prospective, observational study of all critically ill adults eligible to participate in research studies at 23 Canadian intensive care units (ICUs). We characterized eligibility events into one of five consent outcomes, identified reasons why opportunities to recruit were missed or infeasible, and documented decision-maker's rationale for providing or declining consent.

MEASUREMENTS AND MAIN RESULTS:

Only 8.9% of eligible patients made decisions for themselves.

An International Assessment of Ovarian Cancer Incidence and Mortality

Conclusions

Ovarian cancer survival has shown modest improvement from a statistical perspective in the U.S. However, it is difficult to ascertain how clinically relevant these improvements are at the population or patient level.

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Highlights

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We assessed the global epidemiology of ovarian cancer and examined changes in worldwide incidence and mortality.

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There was a modest decrease in incidence and significant increases in 12-, 24-, and 60-month survival in the US.

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There is wide variation in the worldwide incidence of ovarian cancer, with the lowest rates consistently in China.

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Objective

To assess and characterize the temporal variation in ovarian cancer incidence and mortality by age within countries in the Americas, Europe, and Asia.

Methods/Materials

Data from the National Cancer Institute’s Surveillance, Epidemiology, and End Results Program in the United States (U.S.) were used to assess ovarian cancer incidence rates (1998−2008) and mortality rates, (1988−2007 for 12-month survival, 1988−2006 for 24-month survival, and 1988−2003 for 60-month survival), stratified by age at diagnosis. Data from GLOBOCAN  (link = 2008 data)were used to calculate country-specific incidence rates for 2010 and 2020 and case-fatality rates for 2010.

Results

A statistically significant decrease in Annual Percent Change (APC) of ovarian cancer incidence was observed in the U.S. for all women (-1.03%), among women who were diagnosed at < 65 years of age (-1.09%) and among women who were diagnosed at ≥ 65 years of age (-0.95%). There was a statistically significant increase in the observed APC for survival at 12-months (0.19%), 24-months (0.58%), and 60-months (0.72%) for all women; however, 5-year survival for advanced stage (III or IV) disease was low at less than 50% for women < 65 years and less than 30% for women ≥ 65 years. Global results showed a wide range in ovarian cancer incidence rates, with China exhibiting the lowest rates and the Russian Federation and the United Kingdom exhibiting the highest rates.

Conclusions

Ovarian cancer survival has shown modest improvement from a statistical perspective in the U.S. However, it is difficult to ascertain how clinically relevant these improvements are at the population or patient level.

Obstetrics and Gynecology Practices and Patient Insurance Type

 Blogger's Note: the abstract does not indicate if cancer screening specifically was part of the study; however, given the number of women who are not referred to a gyn/onc, if it wasn't it should have been - assumption based on limited information in abstract

Abstract

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Background

Despite research on health disparities based on insurance status, little is known about the differences in practice patterns among physicians who cater to privately and non-privately insured patients. The aim of this study was to assess how obstetrician–gynecologists (ob-gyns) who primarily see patients with private insurance differ from those who see mainly uninsured or publicly insured patients. This could be informative of the needs of these two groups of physicians and patients.

Methods

A questionnaire was mailed or emailed to 1,000 members of the American College of Obstetricians and Gynecologists, 600 of whom participate in the Collaborative Ambulatory Research Network.

Findings

A 56.4% response rate was obtained. Of the valid responders, the 335 reported providing care to a majority of patients with private insurance (“private group”) and the 105 reported providing care to mostly publicly insured or uninsured patients (“non-private group”) were included in our analyses. Differences between groups included that the private group was more likely to see patients before their becoming pregnant and spent more time on well-woman care. The private group was more likely to see patients who are White, Asian, or between the ages of 45 and 64. The non-private group was more likely to see Hispanic patients and those under age 18.

Conclusion

Results reveal that ob-gyns who see mostly privately insured patients have different clinical experiences than those who see mainly uninsured or publicly insured patients in terms of patient characteristics, preconception care, distribution of time on activities, and the of likelihood performing certain procedures and screening tests.

Secondary debulking surgery in ovarian cancer patients with isolated nodal recurrence located in the region above and behind the renal vein

Abstract

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Objective

We describe our early experience with a suprarenal and retrorenal para-aortic lymphadenectomy involving the mobilization of the left kidney.

Methods

Three patients with isolated nodal recurrence located in the region above and behind the renal vein underwent the removal of these metastatic lymph nodes using a left renal mobilization procedure.

Results and Conclusion

The enlarged suprarenal and retrorenal lymph nodes were safely and effectively removed in all 3 patients. Postoperatively, a lymphatic fistula developed in one patient. However, no morbidities related to renal mobilization, including renal ischemia, were observed in the current series. A further large, prospective study is required to evaluate this surgical procedure.

Folate Receptor Alpha (FRA) Expression Remains Unchanged in Epithelial Ovarian and Endometrial Cancer after Chemotherapy

Abstract

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Highlights

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Both epithelial ovarian and endometrial cancer demonstrate high expression of FRA (folate receptor alpha) compared to normal ovarian and endometrial tissue

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FRA expression is not altered by chemotherapy exposure at interval debulking surgery nor at recurrence

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Immunohistochemical FRA staining at diagnosis can guide the decision whether to use FRA targeted therapy upon recurrence

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Objective

Based on its expression profile, folate receptor alpha (FRA) is an attractive candidate for targeted diagnostics and therapeutics. However, applicability of these agents in residual or recurrent disease could be influenced by chemotherapy. We evaluated whether chemotherapy modified FRA expression in non-mucinous epithelial ovarian (EOC) and endometrial carcinoma (EC).

Ovarian surface epithelium as a source of ovarian cancers: Unwarranted speculation or evidence-based hypothesis? (serous)

Abstract

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Highlights

•

Pure cultures of ovarian surface epithelium (OSE) can be transformed tor high and low grade serous carcinomas.

•

OSE-lined inclusion cysts undergoing morphologic and functional serous metaplasia show intermediate transitional stages, thus ruling out implants from fimbrial epithelium.

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Caltretinin and PAX8 are not reliable markers to determine the origin of epithelial inclusion cysts as either OSE or fimbriae.

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Objectives

There has been increasing evidence that high grade serous ovarian carcinomas (HGSOCs), the most common and most lethal of all ovarian cancers, originate in oviductal fimbriae and metastasize to the ovary. The alternate hypothesis, that ovarian carcinomas may originate within the ovarian stroma in inclusion cysts lined by ovarian surface epithelium (OSE), has been criticized and often dismissed on the basis of the OSE’s embryonic origin, mesothelial phenotype, tissue-specific markers, questionable ability to undergo metaplasia, and the lack of identifiable precursor lesions. This review analyses these criticisms and summarizes evidence indicating that OSE as a source of ovarian cancers cannot be ruled out.

Prophylactic salpingectomy in premenopausal low-risk women for ovarian cancer: Primum Non Nocere

Abstract

Highlights

•

Ovarian function is not compromised by adding bilateral salpingectomy to TLH ( total laparoscopic hysterectomy (TLH) )

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Laparoscopic bilateral salpingectomy is a safe procedure when added to TLH

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Premenopausal prophylactic salpingectomy is a safe procedure for preventing HGSC

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Objective

The objective of this study is to compare ovarian function and surgical outcomes between patients affected by benign uterine pathologies submitted to total laparoscopic hysterectomy (TLH) plus salpingectomy and women in which standard TLH with adnexal preservation was performed.