Prostate Restored
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For instance, Al-Azab et al assessed prostate volumes of 1796 patients using transrectal ultrasound (TRUS) and concluded that “men with a large prostate volume (larger than 72cc) had a 20.5% risk of prostate cancer on biopsies compared to men with the smallest prostate volume (less than 38cc) who had 65.8% risk of ...
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Read More »Table 2 Summary of Histologic Composition and Embryologic Origins of the Different Zones of the Prostate Gland It is well documented in anatomical and imaging studies that BPH originates in the TZ while 80–85% of PCa originates in the PZ.11,12 A recent review article summarized that the “histo-anatomical changes within the peripheral zone caused by BPH growth lead to significant tissue transformation within the peripheral zone”.12 This transformation causes thickening of the prostatic capsule secondary to fibrosis which is also called the surgical capsule by urologists due to the distinctive plane between the TZ and PZ in large BPH prostates which is much less evident in small prostates. This process causes epithelial cell atrophy within the PZ due to direct pressure-related tissue injury and reduced blood flow caused by the expanding TZ in growing BPH. Due to this process, gland atrophy is seen within the PZ. As 80% of PCa originates from the glandular epithelium within the PZ this supports the hypothesis that these dynamic interactions between the growing TZ and compressed PZ explain the decreased incidence of PCa in large BPH prostates.13,14 Sellers et al performed multiparametric MRI prostate studies on biopsy naïve patients. This study focused on specific PZ measurements which demonstrated compression of the PZ in large prostates compared to smaller prostates: Small and mid-size prostates had a huge range of PZ thickness whereas large prostates with a total volume around 90 mL or above showed a noticeable drop in PZ thickness suggesting the PZ can resist pressure from the TZ growth to a certain point only.15 This inverse relationship may also explain the results of the Prostate Cancer Prevention Trial, where almost 19,000 patients received continuous Finasteride medication. The treatment arm showed a more than a twofold increase in high grade aggressive PCa. Finasteride is known to affect and reduce the growth of the TZ, thus giving the glandular epithelium of the PZ more room within the prostate to grow and expand.16 This clinical observation has been confirmed by Lorenzo et al in mathematical simulation studies analyzing the controversial effects of 5α reductase inhibitors (5ARIs), and found that “the shrinkage of the prostate induced by 5ARIs reduced the hydrostatic stress that had accumulated over years of BPH in prostatic tissue, which led to a mechanical state that favored the development of PCa”.17 Many studies listed in Table 1 have reported that prostate volume is one of the most significant predictive factors for the detection of prostate cancer both in univariate and multivariate analysis. Historically, prostate-specific antigen (PSA) alone has not proven to be a good diagnostic tool in detecting PCa but combining or adjusting it with gland volume, prostate-specific antigen density (PSAD), has improved its diagnostic value.18,19 Elliott et al demonstrated that PSA performance was significantly better in men with smaller prostates at detecting both low-grade and high-grade PCa.20 Al-Azab et al suggested that a smaller prostate volume may be the strongest predictor of cancer detection in the PSA range of 2.0 to 9.0 ng/mL, and that adjusting for the patient’s prostate volume may help with earlier detection and decrease the need for repeated prostate biopsies.8 Previous studies have shown the amount of BPH, and not cancer, is the major factor responsible for the elevation of PSA. However, elevated PSA is the reason for many patients with large prostates to undergo biopsies which are often unnecessary and only lead to overdiagnosis and subsequent overtreatment.21 PSAD performance in detecting PCa is affected by prostate volume. The predictive value of PSAD in detecting PCa is higher in small- and medium-sized prostates compared to larger glands. Therefore, many clinical researchers and investigators have recommended that clinicians should counsel patients with large prostates and elevated PSA to consider conservative management such as sequential PSA measurements and not to proceed with biopsies.22,23 As outlined in this systemic review, many recent, statistically significant and powerful studies are confirming that BPH may be protective against prostatic cancer supporting the proposed mathematical model by Lorenzo et al that growth of the TZ due to BPH causes increased hydrostatic pressure and compresses the PZ (where 80–85% of PCa originates). As mentioned earlier, this histo-anatomical process leads to fibrosis and glandular atrophy of the PZ, and thus likely lowers the risk of clinically significant PCa.24 This hypothesis is well illustrated by the histo-anatomical study of Guzman et al in showing a decrease in gland density and increase in tissue fibrosis within the PZ in larger prostates when compared to smaller prostates (see Figure 3A and B).25 Figure 3 H&E-stained slides of different sized prostate specimens at 50× magnification: (A) Small Prostate Specimen (24 g). The external, posterior margin is inked and marked with an asterisk*. A decent number of hyperplastic glands (as indicated by arrows) are present and easily visible in the peripheral zone (PZ) close to the thin capsule (black line). Reproduced with permission from Dove Medical Press Limited, Guzman JA, Sharma P, Smith LA et al. Histological changes of the peripheral zone in small and large prostates and possible clinical implications. Res Rep Urol. 2019;11:77–81.25 (B) Large Prostate Specimen (100 g). The external, posterior margin is also inked and marked with an asterisk*. The arrow is indicating an atrophic gland within the extended fibrotic layer/ surgical capsule (black line). This capsule is much thicker in comparison to Figure 2A, and no hyperplastic glands are present. Reproduced with permission from Dove Medical Press Limited, Guzman JA, Sharma P, Smith LA et al. Histological changes of the peripheral zone in small and large prostates and possible clinical implications. Res Rep Urol. 2019;11:77–81.25
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Read More »We are aware of some limitations as this systematic review includes a relatively small number of articles that met the inclusion criteria. Furthermore, the selected studies, although statistically significant, carried large heterogeneity. When reviewing the histo-anatomical studies, the anatomical reconstruction of the prostate by histological specimen slides can be challenging. Gross examination techniques vary greatly among pathologists, with some using coronal cuts, while others use sagittal or transverse cuts, leading to differences in the orientation of the different portions of the prostate specimen. Due to the nature of the prostate, localizing the precise boundaries between the different zones by imaging can be challenging and operator-dependent (ie, TRUS). This is much less an issue with MRI. Another limitation is the variability in biopsy protocol. Sextant and extended needle biopsies have been shown to yield different diagnostic power. Some studies have suggested increasing the number of biopsies for larger prostates may improve the detection of PCa. However, studies have proven that past a certain gland volume the detection rate of PCa differs minimally between number of biopsies.26,27 Furthermore, most of the studies listed in our review were cross-sectional and observational studies which can cause bias in different categories and are difficult to further investigate. Therefore, additional bias assessment on these individual studies were not performed. In this context publication bias should also be mentioned as our review was limited to the PubMed database and the expertise of the authors involved. Even when considering the limitations mentioned above, this systematic review of clinical studies within the last 30 years strongly supports the hypothesis of protective benefits of BPH against development and progression of clinically significant PCa. With increased use of multiparametric MRI of the prostate in the diagnostic and management of PCa, future studies will likely further elucidate this relationship, in particular because MRI/Ultrasound Fusion biopsies allow increased precision in the diagnosis of clinically significant PCa.28,29 This will likely decrease the problem of sampling error experienced with systematic TRUS prostatic biopsy that tends to be more prevalent in larger (BPH associated) prostates.30 As MRI technology and its use in the diagnosis of PCa becomes more accessible, future studies will rectify and decrease the impact of sampling error bias associated with this hypothesis. If the described disease process of BPH-induced atrophy of the PZ glandular tissue and its subsequent protective potential against PCa is confirmed through future research and studies, it will have important clinical implications related to the diagnosis and treatment of BPH and PCa.
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