Hi, I am sorry for my typo. I meant to say sympathize.
One thing I can recommend is to ask your cancer center about genomic analysis. The genomic analysis will find which bladder cancer-related gene mutations are found in your cancer cells. The genomic analysis of your bladder cancer cells can tell what type of cancer it is from a molecular point of view. It should complement the diagnosis which had been completed so far.
There was a study done in Korea for 29 young (5-20 yrs old) who were diagnosed with bladder cancer. 28 had LG and 1 had HG. All young patients were alive during a median follow up period of 62 months (range 2-153 months). No young patients progressed to muscle vs 6.7% of adult NMIBCs progressed to muscle. Three young patients had a recurrence. It is noted that the size of tumors of those young patients ranged (0.5cm - 5cm).
So, the prognosis of young patients with LG looks very good even it is greater than 3 cm.
The main goal of the study was to compare gene mutations in cancer cells of young patients and adult patients.
What they found was that there were mutations in genes that affect growth and divisions of cells but not many
mutations in the genes which suppress the formation of cancer cells. An analogy is that young bladder cancer patients had broken components in their accelerator system of the car but they found that the components of their breaking system were not broken. It is noted that in muscle invasive bladder cancer, the faulty braking system is often found. So, if the genome analysis of your bladder cancer cell shows similar gene mutation patterns as those young patients, your prognosis looks good even without BCG treatment.
Some examples of the genes which affect cell growth/division are FGFR(1,2,3,4), RAS (KRAS,HRAS, NRAS). An example of the genes which affect the suppression of cancer cells is TP53.
In the study, they found 47.6% of young patients had HRAS mutation but only 3.4% in adults NMIBC and 3.4% in adults with MIBC. They also found FGFR3 mutation was the most commonly mutated genes (79%) in adults NMIBC patients, but rarely found in young patients. But FGFR3 fusion was found over 30% in young patients but almost none in adult patients. So, if your bladder cancer has a similar profile of gene mutations as of those young patients you should expect a similar prognosis with the young patients, which is good.
The conclusion of the study is as follows
YBC (young bladder cancer patients) had distinct driver genetic alterations such as HRAS mutation and FGFR3 gene fusion and showed good prognosis. YBCs and ABCs (Adults Bladder cancer patients) with YBC-like mutations showed no progression to muscle-invasive tumors. Therefore, bladder cancer with YBC-like genetic alterations represented an indolent bladder tumor, regardless of age, and may be managed with less aggressive treatment.
FYI,
Because the paper did not say if young patients with TaLG had any treatment or not,
I have sent an email to an author of the paper to find out if any young patients with TaLG, especially the patient who had 5 cm tumor had any treatment such as BCG treatment. I will let post it if and when I receive the response.
Below is the link to the study.
www.ncbi.nlm.nih.gov/pmc/articles/PMC7073191/#app1-cancers-12-00307