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Thứ Hai, 8 tháng 10, 2012

GIẢI NOBEL Y HỌC 2012


Hai nhà khoa học John B.Gurdon và Shinya Yamanaka đã đoạt giải Nobel Y học năm nay 2012 nhờ việc phát hiện tế bào trưởng thành có thể tái lập trình để trở thành tế bào vạn năng (pluripotent).
 
 

Theo thông báo từ Ủy ban Nobel, Gurdon và Yamanaka đã nhận thấy các tế bào trưởng thành, chuyên biệt hoá có thể được can thiệp và lập trình lại để trở thành các tế bào gốc, chưa trưởng thành vốn có khả năng phát triển thành tất cả các dạng mô trong cơ thể. Nghiên cứu này đã “cách mạng hóa” nhận thức về cơ chế phát triển của tế bào và cơ quan sinh học.

Năm 1962, ông Gurdon đã phát hiện tế bào có một khả năng đặc biệt là đảo chiều. Trong một thí nghiệm kinh điển, ông đã thay thế nhân tế bào chưa trưởng thành trong một tế bào trứng ếch bằng nhân của một tế bào ruột trưởng thành. Kết quả là tế bào trứng biến đổi vẫn phát triển thành một con nòng nọc bình thường. DNA của tế bào trưởng thành vẫn có tất cả các thông tin cần thiết để phát triển mọi tế bào trong cơ thể ếch.

Hơn 40 năm sau, năm 2006, Shinya Yamaka phát hiện các tế bào trưởng thành nguyên dạng ở chuột có thể được lập trình để trở thành các tế bào gốc chưa trưởng thành. Bằng cách can thiệp và biến đổi chỉ một vài gene, ông đã có thể tái lập trình các tế bào trưởng thành trở thành tế bào gốc vạn năng hay tế bào gốc đa hiệu (pluripotent stem cell). Đây là thuật ngữ chỉ những tế bào chưa trưởng thành có khả năng phát triển thành mọi dạng tế bào khác nhau trong cơ thể.

Những phát kiến mang tính đột phá này, theo Ủy ban Nobel, đã làm thay đổi hoàn toàn cách nhìn nhận của khoa học về sự phát triển cũng như chuyên biệt hóa ở cấp độ tế bào. “Tế bào trưởng thành không phải giam mình mãi mãi với một chức năng cụ thể và chuyên biệt nào. Bằng cách tái lập trình tế bào người, các nhà khoa học đã mở ra cơ hội mới để nghiên cứu nhiều loại bệnh cũng như phát triển phương pháp chẩn đoán và điều trị mới”.

Ứng dụng
 
Tế bào gốc có khả năng ứng dụng chữa trị nhiều bệnh từ ung thư, tiểu đường, để thay thế các mô và nội tạng bị hỏng của cơ thể nhờ khả năng phát triển thành mọi loại tế bào thay thế những tế bào bệnh tật. Nó có thể sửa chữa một trái tim sau cơn đột quỵ hoặc đảo ngược tiến trình phát triển của bệnh Alzheimer.
Nghiên cứu được trao giải Nobel y học năm nay đã mở ra một phương cách mới để có được tế bào gốc mà không phải dùng đến phôi thai, một vấn đề gây nhiều tranh cãi đạo đức. “Thiếu nội tạng để cấy ghép là một vấn đề lớn tại nhiều quốc gia hiện nay” - ông Yamanaka nhấn mạnh.
Một trong các ứng dụng thực tế khác của nghiên cứu này là khả năng nghiên cứu tận gốc rễ các căn bệnh thông qua tế bào của người mắc bệnh để tìm ra biện pháp chữa trị. “Tế bào da có thể được lấy từ người bệnh mắc nhiều căn bệnh khác nhau, tái lập trình và xem xét trong phòng thí nghiệm để xem chúng khác với những tế bào khỏe mạnh như thế nào”, Ủy ban Nobel cho biết.

Thứ Sáu, 5 tháng 10, 2012

Different Sonographic Features of Triple-Negative Breast Cancer and Non-TNBC

Abstract

Objectives—Triple-negative breast cancer (TNBC) is known to have unique molecular, clinical, and pathologic characteristics. The growth pattern of this cancer may also affect its appearance on sonography. Our study evaluated the sonographic features of TNBC according to the American College of Radiology Breast Imaging Reporting and Data System sonographic classification system and compared these features with those of non-TNBC.
Methods—Data from 315 consecutive breast cancer cases were collected. The images were reevaluated by an examiner blinded to the patients’ characteristics and histologic results according to the Breast Imaging Reporting and Data System. The sonographic features of TNBC (n = 33) and non-TNBC (n = 282) were compared.
 
Conclusions—Triple-negative breast cancer and non-TNBC have different sonographic features. This finding can be explained by the pathologic profile of this breast cancer subtype. Some of the distinct sonographic criteria for TNBC are more likely to be associated with benign masses. Knowledge of the distinct sonographic features of TNBC would help the examiner avoid false-negative classification of this tumor type.

         
Discussion

Early Detection of TNBC
Triple-negative breast cancer is known to be an especially aggressive subtype of breast cancer. It is characterized by the complete absence of ER, PR, and HER2 over expression. However, this definition only tackles the phenotype and merely scratches the surface of the underlying processes within breast cancer cells.
Nowadays, we have a much deeper insight into the molecular backgrounds of the different subtypes of breast cancer. From gene expression profiles, we have learned that there are at least 5 different intrinsic subtypes of breast cancer (luminal A, luminal B, claudin low, HER2 enriched, and basal like).57 Basal-like breast cancer is not synonymous with TNBC, although there is overlap, and most basal-like breast cancers are triple negative and vice versa. There is also a strong association with BRCA gene mutations in both TNBC and basal-like breast cancer.24 Although we are just starting to determine the molecular basis of TNBC, this type of breast cancer remains an extraordinary challenge for the clinicians who treat patients with TNBC in primary care.

Triple-negative breast cancer is known to occur in younger woman, as shown in our study. The overall outcome is poor because patients with TNBC are at higher risk of early relapse and distant visceral metastases. Endocrine treatment for endocrine-responsive disease and HER2-directed treatment in cases of HER2 overexpression provide the most effective available treatment for suitable patients with breast cancer.25,26 Unfortunately, these treatment options do not exist for patients with TNBC. Therefore, chemotherapy remains the only systemic option for improving the prognosis and is usually necessary for patients with TNBC, as illustrated in our data set. New therapeutic agents, such as poly(ADP-ribose) polymerase inhibitors, are under development but have not yet been approved for the treatment of TNBC.27 As shown in neoadjuvant trials, TNBC responds relatively well to different chemotherapeutic agents, but paradoxically, the overall prognosis remains poor, and whenever a pathologically complete response cannot be achieved, the prognosis is even worse.2830

Therefore, early detection of this aggressive subtype of breast cancer has an important prognostic relevance. Against this background, breast sonography plays an essential and specific role by adding more diagnostic accuracy to the mammogram. Lesion evaluation with sonography thus plays a crucial role in the diagnostic and therapeutic pathway of patients with breast cancer. False-negative results in evaluations of breast cancers may result in a delayed diagnosis and a worse outcome.


Sonographic Features of TNBC in the Literature

In the literature, we found 3 related publications describing sonographic characteristics of TNBC, although to our knowledge, there has never been a systematic evaluation according to the BI-RADS sonographic classification and a comparison to non-TNBC. Dogan et al31 reviewed 44 patients with TNBC. They noted that TNBC may be occult on mammography and sonography and frequently has benign features. In contrast, magnetic resonance imaging identified all 44 cases correctly and showed features that had a high positive predictive value for malignancy. Ko et al32 retrospectively reviewed mammographic and sonographic findings of 245 patients from January 2007 to October 2008. Triple-negative breast cancers occurred in 35.5% of the cases (n = 87), and these cancers were more likely to have circumscribed margins, more likely to be markedly hypoechoic, and less likely to show posterior shadowing. Kojima and Tsunoda33 reported on 88 patients with TNBC. In their retrospective analysis of cases from January 2007 to April 2010, they observed that TNBC was more likely to present as a mass and less likely to show attenuating posterior echoes. These 3 studies already mentioned a few of the sonographic characteristics, and the results correlate well with our own findings.

Sonographic Features of TNBC in Our Study

The aim of our study was to scrutinize the distinct sonographic features of TNBC according to the BI-RADS sonographic classification, and our results show that TNBC is characterized by typical sonographic criteria that are to a certain degree different from those of non-TNBC (Table 4). The shape of TNBC was more likely to be oval or round, and the echogenic halo was observed significantly less often compared to non-TNBC. Furthermore, Cooper ligaments were displaced (rather than disrupted) significantly more often in TNBC. This finding can be explained by the typical growth pattern of TNBC, which is described as a “pushing border” in the absence of an infiltrating margin. This smooth appearance is usually associated with noninfiltrative processes of the breast but also occurs in TNBC as an expression of rapid tumor escalation. We believe that our observation on sonography is the macroscopic correlate of this histopathologic behavior. This kind of smooth mass margin has also been described for TNBC on magnetic resonance imaging.34
The pathologic phenomenon of a pushing margin at which the tumoredge shows a circumscribed boundary also explains the elevated rate of lobulated or microlobulated margins on sonography. The echogenic halo is an expression of a desmoplastic response and inflammation. Desmoplasia is thought to be a critical event in cancer progression and a prognostic indicator and is regularly found in TNBC.35 We were notable to find a sonographic-morphologic correlate for the desmoplastic reaction. On the contrary, an echogenic halo was observed significantly less often in our TNBC group. We suppose that the aforementioned rapid tumor progression dominates the appearance of the tumors on sonography. Hence, desmoplasia is actually present in triple-negative tumors but has no sonographic correlation.

The particularly disordered growth of malignant tumors leads to an increase in tissue layers with different impedances and consequently an increase in reflected, absorbed, and scattered echoes. In invasive ductal carcinoma, a trabecular appearance is common, and a syncytial growth pattern is rare. As a result, malignant tumors are usually associated with posterior acoustic shadowing. We found a significantly increased rate of posterior acoustic enhancement (instead of shadowing, unchanged echoes, or a mixed pattern) in our TNBC group. This feature is usually associated with benign nodules that are growing in a regular and controlled manner or with cystic lesions. As shown in recent studies, TNBC shows a syncytial growth pattern in about 56% of cases.36 In this pattern, tumor cells are closely apposed and nestled against one another and lack distinct cytoplasmic membranes, consequently forming a large syncytium. This growth pattern creates fewer layers than the trabecular pattern and may therefore explain the improved propagation of the ultrasonic waves.


Clinical Features of TNBC in Our Study

The prevalence of TNBC in our study cohort was 10.5% and was slightly lower than reported in the literature (11.2%–39.9% in certain ethnic groups).3,4 Because we did not select the cases and censoring due to missing data was a random event, this decreased prevalence can be considered a general effect due to the population that we serve in our community (97.6% European white, 1.7% Central and East Asian, 0.4% African, and 0.3% other). It might also be due to the strict definition of TNBC in our study, with a cutoff for ER and PR levels of 1% or greater for endocrine responsiveness, whereas other authors have used cutoffs of up to 10% or greater.4 However, our definition is consistent with the American Society of Clinical Oncology/College of American Pathologists recommendations.37

We observed a trend for higher breast density in the TNBC group. This result was most probably biased by the unbalanced age distribution, with the TNBC group being considerably younger than the non-TNBC group. Younger patients are more likely to have dense breast tissue. Yang et al1 reported no correlation between triple negativity and breast density in their age-adjusted collection of patients.

With regard to the final tumor stage, there was no difference in the T classification of the two groups. Regarding the N classification, we found a significantly higher rate of positive axillary lymph nodes in the TNBC group. As shown by previous studies, even small breast cancers tend to disseminate axillary lymph node metastases if a biologically unfavorable type of breast cancer is present. Maibenco et al38 reported an increasing rate of axillary lymph node metastases with higher histologic grades. Most cases of TNBC are reported to be grade 3, as found in our study. Furthermore, the intrinsic characteristics of TNBC that are determined by its unique molecular profile are known to determine its aggressive behavior, which may explain the increased lymph node involvement in the TNBC group.

Limitations of Our Study

The main limitation of our study was the relatively small sample size. Thus, although we were able to show significant differences for some sonographic features of TNBC and non-TNBC, for other features there was only a trend. We believe that significant differences for these features could be revealed with a larger sample size. Furthermore, we did not assess the combination of characteristics because that approach was not planned. Another limitation was the fact that only a single observer evaluated the sonograms. Data on interobserver concordance were not generated. This factor should be investigated further. An analogous study comparing other immunohistochemical subtypes of breast cancer (eg, HER2 positive versus HER2 negative) would also be beneficial. Investigation of the correlation with the intrinsic subtype would also be interesting. We were not able to determine the intrinsic subtype for our patients and thus were restricted to describing the TNBC phenotype.

Summary

We found that TNBC has distinct sonographic features compared to non-TNBC. These features can be explained by the typical growth pattern of this tumor type. Therefore, TNBC may lack some of the characteristic criteria for malignancy and may even mimic a benign lesion. Being familiar with this behavior would help the examiner avoid false-negative classification of TNBC in the future.
          FURTHER READING:


Study Divides Breast Cancer Into Four Distinct Types

By GINA KOLATA  The New York Times, Health
Published: September 23, 2012

In findings that are fundamentally reshaping the scientific understanding of breast cancer, researchers have identified four genetically distinct types of the cancer. And within those types, they found hallmark genetic changes that are driving many cancers.

These discoveries, published online on Sunday in the journal Nature, are expected to lead to new treatments with drugs already approved for cancers in other parts of the body and new ideas for more precise treatments aimed at genetic aberrations that now have no known treatment.

The study is the first comprehensive genetic analysis of breast cancer, which kills more than 35,000 women a year in the United States. The new paper, and several smaller recent studies, are electrifying the field.

“This is the road map for how we might cure breast cancer in the future,” said Dr. Matthew Ellis of Washington University, a researcher for the study.

Researchers and patient advocates caution that it will still take years to translate the new insights into transformative new treatments. Even within the four major types of breast cancer, individual tumors appear to be driven by their own sets of genetic changes. A wide variety of drugs will most likely need to be developed to tailor medicines to individual tumors.

“There are a lot of steps that turn basic science into clinically meaningful results,” said Karuna Jaggar, executive director of Breast Cancer Action, an advocacy group. “It is the ‘stay tuned’ story.”

The study is part of a large federal project, the Cancer Genome Atlas, to build maps of genetic changes in common cancers. Reports on similar studies of lung and colon cancer have been published recently. The breast cancer study was based on an analysis of tumors from 825 patients.

“There has never been a breast cancer genomics project on this scale,” said the atlas’s program director, Brad Ozenberger of the National Institutes of Health.

The investigators identified at least 40 genetic alterations that might be attacked by drugs. Many of them are already being developed for other types of cancer that have the same mutations. “We now have a good view of what goes wrong in breast cancer,” said Joe Gray, a genetic expert at Oregon Health & Science University, who was not involved in the study. “We haven’t had that before.”

The study focused on the most common types of breast cancer that are thought to arise in the milk duct. It concentrated on early breast cancers that had not yet spread to other parts of the body in order to find genetic changes that could be attacked, stopping a cancer before it metastasized.

The study’s biggest surprise involved a particularly deadly breast cancer whose tumor cells resemble basal cells of the skin and sweat glands, which are in the deepest layer of the skin. These breast cells form a scaffolding for milk duct cells. This type of cancer is often called triple negative and accounts for a small percentage of breast cancer.

But researchers found that this cancer was entirely different from the other types of breast cancer and much more resembles ovarian cancer and a type of lung cancer.

“It’s incredible,” said Dr. James Ingle of the Mayo Clinic, one of the study’s 348 authors, of the ovarian cancer connection. “It raises the possibility that there may be a common cause.”

There are immediate therapeutic implications. The study gives a biologic reason to try some routine treatments for ovarian cancer instead of a common class of drugs used in breast cancer known as anthracyclines. Anthracyclines, Dr. Ellis said, “are the drugs most breast cancer patients dread because they are associated with heart damage and leukemia.”

A new type of drug, PARP inhibitors, that seems to help squelch ovarian cancers, should also be tried in basal-like breast cancer, Dr. Ellis said.

Basal-like cancers are most prevalent in younger women, in African-Americans and in women with breast cancer genes BRCA1 and BRCA2.

Two other types of breast cancer, accounting for most cases of the disease, arise from the luminal cells that line milk ducts. These cancers have proteins on their surfaces that grab estrogen, fueling their growth. Just about everyone with estrogen-fueled cancer gets the same treatment. Some do well. Others do not.

The genetic analysis divided these cancers into two distinct types. Patients with luminal A cancer had good prognoses while those with luminal B did not, suggesting that perhaps patients with the first kind of tumor might do well with just hormonal therapy to block estrogen from spurring their cancers while those with the second kind might do better with chemotherapy in addition to hormonal therapy.

In some cases, genetic aberrations were so strongly associated with one or the other luminal subtype that they appeared to be the actual cause of the cancer, said Dr. Charles Perou of the University of North Carolina, who is the lead author of the study. And he called that “a stunning finding.”

“We are really getting at the roots of these cancers,” he said.

After basal-like cancers, and luminal A and B cancers, the fourth type of breast cancer is what the researchers called HER2-enriched. Breast cancers often have extra copies of a gene, HER2, that drives their growth. A drug, Herceptin, can block the gene and has changed the prognosis for these patients from one of the worst in breast cancer to one of the best.

Yet although Herceptin is approved for every breast cancer patient whose tumor makes too much HER2, the new analysis finds that not all of these tumors are alike. The HER2-enriched should respond readily to Herceptin; the other type might not.

The only way to know is to do a clinical trial, and one is already being planned. Herceptin is expensive and can occasionally damage the heart. “We absolutely only want to give it to patients who can benefit,” Dr. Perou said.

For now, despite the tantalizing possibilities, patients will have to wait for clinical trials to see whether drugs that block the genetic aberrations can stop the cancers. And it could be a vast undertaking to get all the drug testing done. Because there are so many different ways a breast cancer cell can go awry, there may have to be dozens of drug studies, each focusing on a different genetic change.

One of Dr. Ellis’s patients, Elizabeth Stark, 48, has a basal-type breast cancer. She has gone through three rounds of chemotherapy, surgery and radiation over the past four years. Her disease is stable now and Dr. Stark, a biochemist at Pfizer, says she knows it will take time for the explosion of genetic data to produce new treatments that might help her.

“In 10 years it will be different,” she said, adding emphatically, “I know I will be here in 10 years.”