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Review paper

Six fractions weekly as accelerated fraction radiotherapy: Is it applicable for nasopharyngeal cancer? A review

Arundito Widikusumo
1
,
Schandra Purnamawati
2

1.
Department of Radiotherapy, Prof. Dr. Margono Soekarjo General Hospital, Purwokerto, Indonesia
2.
Faculty of Medicine, Universitas Jenderal Soedirman, Purwokerto, Indonesia
Contemp Oncol (Pozn) 2019; 23 (3): 127-132
Online publish date: 2019/10/30
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Introduction

Nasopharyngeal cancer (NPC) is a nasopharyngeal epithelial cell-derived malignancy. NPC has low global incidence, only 86,691 new cases yearly, comprising 0.6% of total malignancy worldwide [1]. This malignancy is mostly distributed in Southern China and South East Asia, followed by North Africa, the Middle East, North America, and the Arctic region. Endemically, NPC is mostly associated with Epstein-Barr virus (EBV) infection, particularly with World Health Organization (WHO) histological type 2 and 3 [13].

NPC is a radioresponsive type malignancy [46]. Radiotherapy has been the therapy of choice for NPC since 1950. The use of Radiotherapy as a single modality gives a relatively high overall five-year survival rate for early stages, which ranges from 60% to 85%. However, the outcome for locally advanced stage is not as satisfying, with an overall five-year survival rate of only 37% [58]. Administration of chemotherapy as combined therapy with radiotherapy (concurrent chemoradiation) may improve the therapeutic ratio. Concurrent chemoradiation may improve locoregional control as well as the survival rate. For stage II NPC, concurrent chemoradiation gave a three-year local control rate equal to stage I treated with radiotherapy alone. For overall locally advanced stage, concurrent chemoradiation enhance the five-year locoregional control by as much as 30%, and thus concurrent chemoradiation for locally advanced stage gave equally good outcomes as those of early stage disease treated only with radiotherapy [813]. Platinum-derived chemotherapeutic drugs, particularly cisplatin, is the drug of choice to be used in concurrent chemoradiation for NPC because this drug group shows superiority compared to chemotherapeutic drugs from other groups [912]. Today, the standard therapy for locally advanced stage NPC is concurrent chemoradiation. Nevertheless, the outcomes still fall far short of expectations, and so methods to improve radiotherapy outcome are required, one of which is by fractionation modification (altered fraction).

The basic mechanism of altered fractions

Altered fractions should take into account cancer tissue curability as well as the effect on normal tissue. Radiotherapy has to pay attention to the precision of total dose administration (TD), the dosing of each fraction (d), and the number of fractionations (n). Some cancers show variable response: occasionally a cancer shows radiotherapy responsiveness, while others show resistance to the same modality. This is determined by the α/β ratio of the cancer [5].

Biological mechanisms that influence tumour response to radiotherapy are redistribution (cell cycle), re-oxygenation, cell repair, and repopulation, as well as other differences of radio sensitivity [14, 15]. The cell cycle comprises four phases where Gap2 phase (G2) and mitoses phase (M) which are the most sensitive phase to radiotherapy compared to the remaining [14]. Cellular repair during those phases is lower. Cancer cells do not have an optimal self-repair ability like normal cells; therefore, cancer cells undergoing sublethal damage will die when exposed the a subsequent radiotherapy fractionation.

Cancer tissue vasculature is worse than that of healthy tissue, leading to hypoxic conditions. This interferes with the cell destruction process through indirect or free radical pathway (H+ and OH), which is derived from water ionisation due to radiotherapy exposure. The hypoxic area of cancer tissue is usually located in its centre. With radiotherapy fractionation, the peripheral cancer tissue (oxide area) will be damaged and reduce the volume of cancer tissue. Other intrinsic cancer conditions may also influence the outcome of radiotherapy. Overexpression of EGFR leads to cancer radio resistance, which brings an opportunity for administration of target therapy. DNA base damage due to radiotherapy will activate p53. This activation will stimulate the cell cycle checkpoint and prevent the G1 phase from entering the synthesis phase, which leads to the cell repair process. When cell repair fails, the cell will enter the apoptotic phase [1418].

The α and β ratio

Cellular damage due to radiotherapy results from DNA strand damage, either single or double damage (α and β ratio). This is the final biological mechanism resulting from a radiotherapy dosage [5]. Thereby, the α/β ratio is the effect value of a radiotherapy dose, which is calculated to destroy cancer cells according to a quadratic linear approach. On conventional radiotherapy dose administration (1.8–2 Gy/fraction), the tumour cells’ destructive effect is higher than the late destructive effect of normal cells. Vice versa, high-dose radiotherapy (beyond 2 Gy/fraction) will cause a higher late destructive effect of normal cells. This occurs especially in cancers with a high α/β ratio. The higher cancer proliferation will lead to a higher ratio of α/β of the respective cancer. Utilisation of a high radiotherapy dose per fraction on cancers with high proliferation will cause disadvantageous effects on healthy tissue.

There are three aspects to take into account in radiotherapy dosing when considering the α/β ratio. They are normal tissue acute effects, normal tissue late effects, and the cancer tissue itself. The acute side effect is the destructive cellular responses which occur a few moments to several weeks after radiotherapy. The α/β ratio of acute side effect ranges from 7 to 20 Gy. The late side effect is the destructive cellular response responses that occur several months to years after radiotherapy. The α/β ratio of late side effects ranges from 0.5–6 Gy. On conventional radiotherapy fractionation, clonogenic cell regeneration between each radiotherapy fraction may occur optimally so as to cause minimal normal tissue damage. Today, the standard fractionation of conventional radiotherapy is five fractions weekly (one fraction each day). The dosage of each fraction is 1.8–2 Gy. Despite the difference in the α/β ratio between cancer and healthy tissue, it was determined that for the acute effect the α/β ratio of cancer tissue and normal tissue is 10 Gy while for late effect of normal tissue it is 3 Gy [5, 14]. Those threshold value of the α/β ratio was determined for use on conventional fractionation.

Accelerated fractions

An increasing radiotherapy dose has a linear correlation to the number of cancer cell deaths. The increase of radiotherapy dose per fraction may be applied to slowly developing malignancies, using a more accurate radiotherapy technique according to tumour shape (3DRT, IMRT, SRT/SBRT, SRS, VMAT, helical tomotherapy, etc).

For fast developing cancer, the choice of radiotherapy strategy is by enhancing the cumulative radiotherapy total dose. However, we must pay attention to the cancer cell accelerated repopulation phenomenon. This occurs due to prolonged radiotherapy overall treatment time (OTT), resulting in compensation of clonogenic cancer, which accelerates their regeneration during the course of radiotherapy [5, 1921]. This phenomenon may reduce post radiotherapy locoregional control. To overcome this problem, we need to prevent the radiotherapy OTT from being prolonged [20, 21].

NPC is a cancer well known for having a relatively high α/β ratio (16 Gy). Therefore, altered fractions may be applied to NPC by decreasing the dose for each fractionation followed by administration of more than one fraction per day or accelerated OTT [5, 19, 22]. The two most famous methods for altered fractions is the hyperfraction regimen and accelerated fraction regimen. Hyperfractions can be interpreted as using a smaller radiotherapy dose per fraction compared to those of conventional fractionation, which is applied more than once daily (usually twice per day) without prolongation of OTT [5, 22]. The radiotherapy dose per fraction is 1.1–1.3 Gy. Cancer tissue can be given a higher total dose (14–30%) than conventional fractionation as long as it is given with equal OTT [2227]. According to the RTOG 9003 study, hyperfractions gave a better five-year locoregional control result when compared to conventional fractionation [28]. Acute side effects are mostly medium to severe mucositis/pharyngitis and dermatitis [2328]. Pharyngitis side effects will require specific nutrition intervention [25].

The principle of accelerated fractions is to shorten the OTT. The aim is to prevent a fast repopulation of tumour cells. There are two methods of accelerated fractions: hybrid accelerated fractions and pure accelerated fractions.

Hybrid accelerated fractions

This method is principally the enhancement of the number of fractions, the dose per fraction, and the total radiotherapy dose. It has become the basic method for several fractionation regimens such as CHART, CHARTWEL, concomitant boost, and dynamic fractionation [28, 29]. The two first-mentioned regimens have good tumour control outcomes, but also have severe side effects. In general, almost all patients will require hospitalisation after having a total course of radiotherapy. The last two methods are considered equally good when compared to hyperfractions. Hybrid accelerated fractions, according to Teo et al., may enhance the incidence of temporal lobe necrosis two-fold compared to conventional fractionation [30]. Necrosis occurred six months after radiotherapy.

Pure accelerated fractions

The basic principal of the method is not fractionation addition but acceleration of OTT. Radiotherapy was given at 2 Gy per fraction daily. Radiotherapy can be given in seven fractions weekly (including Saturday and Sunday) or six fractions weekly (the sixth radiotherapy was given on Friday afternoon or Saturday). This regimen gave good results for three-year local control and regional control, which are above 80% [31]. For a regimen of seven fractions weekly we can expect severe side effects, as in the hybrid accelerated fraction regimen [32, 33]. Six fractions weekly is considered the best tolerated accelerated fraction method.

Accelerated radiotherapy regimen of six fractions weekly

A multi-centric study by IAEA-ACC in the year 2010 reported the use of six fractions weekly for head and neck cancer, and the result from this study was imporved locoregional control when compared to conventional fraction radiotherapy with five fraction weekly (42% vs. 30%, p = 0.004). The survival rate was also better in the six fractions weekly group (50% vs. 40%, p = 0.03), even when there are no differences in overall survival. The largest advantage is on the primary tumour compared to regional metastasis. Side effects commonly encountered in six fractions weekly radiotherapy comprise mucositis and dysphagia, but these effects are reported to be tolerable. The late effect of six fraction weekly radiotherapy did not increase [34]. The results of the study above are similar to the DAHANCA 6 and 7 studies, in which locoregional control was also better in radiotherapy with six fractions weekly compared to five fractions weekly (70% vs. 60%, p = 0.0005) (Table 1).

Table 1

Accelerated fraction for nasopharyngeal cancer

Author(s)/yearPeriod of study (year)No. of casesResult(s)
Overgaard et al. 2010 (IAEA-ACC study)5.2908The 5-year actuarial rate of LRC was 42% in the AF group versus 30% in CF group (hazard ratio [HR] 0.63, 95% CI 0.49–0.83; p = 0.004). Acute morbidity in the form of confluent mucositis was noted in 45 patients in the AF group and 22 patients in the CF group (2.15, 1.27–3.35); severe skin reactions were noted in 87 patients in the AF group and 50 patients in the CF group (1.91, 1.31–2.79)
Overgaard et al. 2003 (DAHANCA 6 & 7 study)6.111485Overall 5-year LRC rates were 70% and 60% for the AF and CF groups, respectively (p = 0.0005). DFS improved (73% vs. 66% for AF and CF, p = 0.01) but not OS. Acute morbidity was significantly more frequent with AF than with CF but was transient
Lee et al. 2011 (NPC-9902 study)5189The AF + C group achieved significantly higher failure-free rate (88% at 5 years) than the CF group (63%; p = 0.013), the AF group (56%; p = 0.001) and the CF + C group (65%; p = 0.027). As compared with CF alone, the increase in late toxicity was statistically insignificant (36% vs. 20%; p = 0.25). Deaths due to cancer progression decreased (7% vs. 33%; p = 0.011), but deaths due to incidental causes increased (9% vs. 2%; p = 0.62). Improvement in overall survival reached borderline significance (85% vs. 66%; p = 0.058)
Lee et al. 2012 (NPC-0501 study)2.4803Accelerated 6 fractions weekly radiotherapy has no benefit when combined with chemotherapy. PFS and OS is 76% vs. 80% (p = 0.68) and 89% vs. 88% (p = 0.55)
Bourhis et al. 2012 (GORTEC 99-02 study)7.3840Head and neck cancer patient. AF + C had no benefit when compared with CF + C (HR 1.02, 95% CI 0.84–1.23; p = 0.88). CF + C is better than AF only
Matuschek et al. 2018988Meta-analysis study. Post-operative AF for head and neck cancer did not improve LRC and OS when compared to CF
Fan TY et al. 20132.1145Advanced technique with accelerated radiotherapy (SMART) + concurrent chemoradiation. DFS and OS was 93.3% and 95.5%, respectively
Tang JM et al. 20146.397Advanced technique with accelerated radiotherapy (SMART) + concurrent chemoradiation or induction/adjuvant chemotherapy. Five years LRC, DMFS, and OS was 93.3%, 90.3%, and 91.6%, respectively

[i] AF – accelerated fractions, CF – conventional fractions, C – chemotherapy, SMART – simultaneous modulated accelerated radiation therapy, LRC – locoregional control, DFS – disease-free survival, OS – overall survival, DMFS – distant metastases-free survival, PFS – progression-free survival

The greatest advantage is in primary tumour treatment (76% vs. 64%, p = 0.0001). There are no differences in terms of overall survival. The side effect of mucositis is associated more with the six fractions weekly regimen [35]. All studies from IAEA and DAHANCA 6 and 7 on head and neck cancer show improvement of locoregional control from radiotherapy with six fractions weekly.

In a small unpublished RCT study conducted in Indonesia in 2012, 17 NPC patients were divided into two groups, receiving six weekly fractions or five weekly fractions of radiotherapy. There were no differences in radiotherapy response even when clinically there was a tendency for better outcome on six fractions weekly for locally advanced stage NPC (stage T4, N+). Acute side effects comprising dysphagia, dermatitis, and leucopaenia were more commonly found in the six fractions weekly regimen group. The study used the conventional 2D radiotherapy technique. All patients received weekly 40 mg/m2 concurrent cisplatin chemoradiation.

Lee et al. in 2011 conducted a study (NPC-9902) that compared four groups of intervention given to NPC stage T3-4 N0-1 M0, which are conventional fraction radiotherapy (CF), CF in combination with chemotherapy (CF + C), six fractions weekly radiotherapy (AF), and AF in combination with chemotherapy (AF + C). The chemotherapy given in this study was cisplatin 100 mg/m2 every three weeks, followed by adjuvant cisplatin 80 mg/m2 and 5 fluorouracil 5FU 1000 mg/m2 every four weeks. The mean five-year disease-free survival was significantly higher in the AF + C intervention group compared to the remaining three groups. The greatest advantage was seen in stage T4. The incidence of side effects was the same (p = 0.59) for the AF + C and CF + C intervention groups. No incidence of temporal lobe necrosis was found in the study [36].

An opposite result occurred in the NPC-0501 study [37] with a bigger sample, involving 803 subjects. The use of radiotherapy with six fractions weekly in patients undergoing chemotherapy did not give better results when compared to conventional fraction radiotherapy combined with chemotherapy. Progression-free survival and overall survival were 76% vs. 80% (p = 0.68) and 89% vs. 88%, respectively (p = 0.55).

A similar result can be observed in the GORTEC 99-02 study [38]. The use of accelerated fraction radiotherapy in combination with chemotherapy gave no benefit when compared to conventional fraction radiotherapy and chemotherapy. Three-year progression-free survival and overall survival were as high as 34.1% vs. 37.6% (p = 0.88) and 39.4% vs. 42.6% (p = 0.60), respectively. On the other hand, the use of accelerated fractions was still inferior when compared to conventional fraction radiotherapy and chemotherapy. Three-year progression-free survival and overall survival of conventional fraction radiotherapy and chemotherapy when compared to accelerated fraction radiotherapy was as much as 36.7% vs. 32.2% (p = 0.041) and 42.6% vs. 36.5% (p = 0.040). However, this study was conducted in head and neck cancer patients (without nasopharyngeal involvement) and using accelerated fractions with hybrid accelerated fraction radiotherapy (concomitant boost).

In tumours with a high α/β ratio, the calculation for the tumour biological effectiveness dose (tBED) is 64.75 Gy. Hence, when chemotherapy is added as an adjuvant (chemoradiation), tBED will become 73.55 Gy. Meanwhile, accelerated fraction radiotherapy may give a higher tBED value, i.e. 77.1 Gy [31]. Nevertheless, the conclusion from several studies involving head and neck cancer (with or without nasopharyngeal involvement) general supports that accelerated fraction radiotherapy was no better than concurrent chemoradiation [37, 39]. Furthermore, the combination of accelerated fraction radiotherapy and chemotherapy results in a significantly increased tBED value, which may indicate a higher risk for acute radiotherapy effect. This may lead to interruption of radiotherapy which may impede the overall therapeutic result.

Despite the overall success of NPC therapy with concurrent chemoradiation in enhancing locoregional control in the previously mentioned study, subsequent NPC studies in Hong Kong (NPC-9901) and Taiwan (Cheng et al.) do not support the similar outcome of concurrent chemoradiation in all NPC stages [40, 41]. A subgroup analysis of the NPC-9901 randomised control trials concluded that concurrent chemoradiation enhances locoregional control particularly for stage T1-2 N2-3 M0, but not for stage T3-4 N2-3 M0. Similarly, Cheng et al. reported concurrent chemoradiation to be effective for stage II and III but not for stage IV. It appears that the use of six fractions of radiotherapy per week may bring greater benefits only for primary tumours of nasopharyngeal cancers (T3 or T4) when compared to nodal sites. Some studies are starting to use advanced radiotherapy techniques, which are more highly conformal for implementation of accelerated fractions [4244].

In conclusion, opportunities are still available to apply accelerated fractions with six fractions of radiotherapy weekly for NPC stage T3-4 N–/+ M0. The range from conventional 2D radiotherapy technique to advance technique may be applied on accelerated fractions with six fractions of radiotherapy weekly.

Conclusions

Accelerated six fraction weekly radiotherapy is useful for treating NPC, particularly for locally advanced stage in which the range from conventional 2D radiotherapy technique to advance technique may be applied. Despite the relatively similar side effects from accelerated six fraction weekly radiotherapy with or without concurrent chemoradiation, compared to concurrent chemoradiation with standard fractions (five fractions weekly), we still recommend the use of an accelerated regimen of six fractions of radiotherapy weekly for locally advanced stage with contraindication to concurrent chemoradiation.

Notes

[2] Conflicts of interest The authors declare no conflict of interest.

References

1 

GLOBOCAN v.1.0 , author. Cancer incidence and mortality worldwide: IARC Cancer Base No. 11. 2012. Lyon, France: International Agency for Research on Cancer. Available online: urihttp://globocan.iarc.frhttp://globocan.iarc.fr .

2 

Chang ET, Adami HO , authors. The enigmatic epidemiology of nasopharyngeal carcinoma. Cancer Epidemiol Biomarkers Prev. 2006. 15:p. 1765–1777

3 

Ou SHI, Zell JA, Ziogas A, Anton-Culver H , authors. Epidemiology of nasopharyngeal carcinoma in the United States: improved survival of Chinese patients within the keratinizing squamous cell carcinoma histology. Ann Oncol. 2007. 18:p. 29–35

4 

Wouters BG, Begg AC , authors; Joiner MC, van der Kogel AJ , editors. Irradiation-induced damage and the DNA damage response. Basic clinical radiobiology. 2009. 4th ed. London, UK: Hodder Arnold; p. 11–26

5 

Pedraza MV , author. The biological basis of fractionation in radiotherapy. Rev Oncol. 2001. 4:p. 161–165

6 

Chow E, Payne D, O’Sullivan B, Pintilie M, Liu FF, Waldron J, Warde P, Cummings B , authors. Radiotherapy alone in patients with advanced nasopharyngeal cancer: comparison with an intergroup study. Is combined modality treatment really necessary? Radiother Oncol. 2002. 63:p. 269–274

7 

Ove R, Allison RR, Lu JJ , authors; Lu JJ, Cooper JS, Lee AW , editors. Early stage nasopharyngeal cancer: A Highly curative disease with radiation therapy. Nasopharyngeal cancer. Multidisciplinary management. 2010. Heidelberg, Germany: Springer-Verlag; p. 137–147

8 

Hansen O, Overgaard J, Hansen HS, Overgaard M, Hoyer M, Jörgensen KE, Bastholt L, Berthelsen A , authors. Importance of overall treatment time for the outcome of radiotherapy of head and neck carcinoma: dependency of tumor differentiation. Radiother Oncol. 1997. 43:p. 47–51

9 

Lee AMW, Perez CA, Law SCK, Chua DTT, Wei WI, Chong V , authors; Halperin EC, Perez CA, Brady LW , editors. Nasopharynx. Perez and Bradys principles and practice of radiation oncology. 2010. 5th ed. Philadelphia: Lippincott Williams & Wilkins; p. 820–857

10 

Nishimura Y , author. Rationale for chemoradiotherapy. Int J Clin Oncol. 2004. 9:p. 414–420

11 

Zhang L, Zhao C, Ghimire B, et al. , authors. The role of concurrent chemoradiotherapy in the treatment of locoregionally advanced nasopharyngeal carcinoma among endemic population: a meta-analysis of the phase III randomized trials. BMC Cancer. 2010. 58:p. 1–22

12 

Baujat B, Audry H, Bourhis J, et al. , authors. Chemotherapy in locally advanced nasopharyngeal carcinoma: An individual patient data meta-analysis of eight randomized trials and 1753 patients. Int J Radiat Oncol Biol Phys. 2006. 64:p. 47–56

13 

Wee J , author; Lu JJ, Cooper JS, Lee AWM , editors. Concurrent chemotherapy enhanced radiation: Trial and conclusions. Nasopharyngeal cancer. Multidisciplinary management. 2010. Heidelberg, Germany: Springer-Verlag; p. 167–181

14 

Hall EJ, Cox JD , authors; Cox JD, Ang KK , editors. Physical and biologic basis of radiation therapy. Radiation oncology rationale technique results. 2010. 9th ed. Philadelphia: Mosby Elsevier; p. 3–49

15 

Peacock J, Ashton A, Bliss J, Bush C, Eady J, Jackson C, et al. , authors. Cellular radiosensitivity and complication risk after curative radiotherapy. Radiother Oncol. 2000. 55:p. 173–178

16 

Rodemann HP, Baumann M, Bodis S, Dikomey E , authors. Molecular radiation biology/oncology. Radiother Oncol. 2004. 72:p. 247–249

17 

Yarnold J , author. Molecular aspects of cellular responses to radiotherapy. Radiother Oncol. 1997. 44:p. 1–7

18 

Dewey WC, Ling CC, Meyn RE , authors. Radiation-induced apoptosis: relevance to radiotherapy. Int J Radiat Oncol Biol Phys. 1995. 33:p. 781–796

19 

Pedraza Muriel V , author. The impact of oncology of the interaction of radiation therapy and radiobiology. Clin Transl Oncol. 2006. 8:p. 83–93

20 

Withers HR, Taylor JMG, Maciejewski B , authors. The hazard of accalerated tumor clonogen repopulation during radiotherapy. Acta Oncol. 1988. 27:p. 131–146

21 

Trott KR , author. The mechanisms of acceleration of repopulation in squamous epithelia during daily irradiation. Acta Oncol. 1999. 38:p. 153–157

22 

Baumann M, Gregoir V , authors; Joiner MC, van der Kogel AJ , editors. Modified fractionantion. Basic clinical radiobiology. 2009. 4th ed. London, UK: Hodder Arnold; p. 135–148

23 

Fu KK, Pajak TF, Trotti A, et al. , authors. A Radiation therapy oncology group (RTOG) phase III randomized study to compare hyperfractionation and two varians of accelerated fractionation to standard fractionation radiotherapy for head and neck squamous cell carcinomas: first report of RTOG 9003. Int J Radiat Oncol Biol Phys. 2000. 48:p. 7–16

24 

Jen YM, Lin YS, Su WF, et al. , authors. Dose escalation using twice-daily radiotherapy for nasopharyngeal carcinoma: does heavier dosing result in a happier ending? Int J Radiat Oncol Biol Phys. 2002. 54:p. 14–22

25 

Isobe K, Uno T, Kawakami H, et al. , authors. Hyperfractionated radiation therapy for locoregionally advanced nasopharyngeal cancer. Jpn J Clin Oncol. 2005. 35:p. 116–120

26 

Jereczek-Fossa BA, Morra A, DeBraud F, et al. , authors. Hyperfractionated radiotherapy in locally advanced nasopharyngeal cancer. An analysis of 43 consecutive patients. Strahlenther Onkol. 2004. 180:p. 425–433

27 

Jian JJM, Cheng SH, Tsai SYC, et al. , authors. Improvement of local control of T3 and T4 nasopharyngeal carcinoma by hyperfractionated radiotherapy and concomintant chemotherapy. Int J Radiat Oncol Biol Phys. 2002. 53:p. 344–352

28 

Fowler JF, Harari PM , authors. Confirmation of improved local-regional control with altered fractionation in head and neck cancer. Int J Radiat Oncol Biol Phys. 2000. 48:p. 3–6

29 

Orton CG , author; Khan FM , editor. Fractionation: radiobiologic principles and clinical practice. Treatment planning in radiation oncology. 2007. 2nd ed. Philadelphia: Lippincott Williams & Wilkins; p. 268–280

30 

Teo PML, Leung SF, Chan ATC, et al. , authors. Final report of a randomized trial on altered-fractionated radiotherapy in nasopharyngeal carcinoma prematurely terminated by significant increase in neurologic complications. Int J Radiat Oncol Biol Phys. 2000. 48:p. 1311–1322

31 

Hosni A, Alawady M, Nooreldeen A, Sakr H , authors. Accelerated fractionation radiotherapy in treating patients with locally advanced head and neck squamous cell carcinoma. J Cancer Prev Curr Res. 2017. 8:p. 00277

32 

Skladowsky K, Maciejewsky B, Golen M, Tarnawski R, Slosarek K, Suwinski R, Sygula M, Wygoda A , authors. Continous accelerated 7-days-a-week radiotherapy for head-and-neck cancer: long-term results of phase III clinical trial. Int J Radiat Oncol Biol Phys. 2006. 66:p. 706–713

33 

Wygoda A, Maciejewsky B, Skladowsky K, Hutnik M, Pilecki B, Golen M, Rutkowski T , authors. Pattern analysis of acute mucosal reactions in patients with head and neck cancer treated with conventional and accelerated irradiation. Int J Radiat Oncol Biol Phys. 2009. 73:p. 384–390

34 

Overgaard J, Mohanti BK, Begum N, et al. , authors. Five versus six fractions of radiotherapy per week for squamous-cell carcinoma of the head and neck (IAEA-ACC study): A Randomised multicenter trial. Lancet Oncol. 2010. 11:p. 553–560

35 

Overgaard J, Hansen HS, Specht L, et al. , authors. Five compared with six fractions per week of conventional radiotherapy of squamous-cell carcinoma of head and neck: DAHANCA 6&7 randomised controlled trial. Lancet. 2003. 362:p. 933–940

36 

Lee AWM, Tung SY, Chan ATC, et al. , authors. A randomized trial on addition of concurrent-adjuvant chemotherapy and/or accelerated fractionation for locally-advanced nasopharyngeal carcinoma. Radiother Oncol. 2011. 98:p. 15–22

37 

Lee AWM, Ngan RKC, Tung SY, et al. , authors. Preliminary results of trial NPC-0501 evaluating the therapeutic gain by changing from concurrent-adjuvant to induction-concurrent chemoradiotherapy, changing from fluorouracil to capecitabine, and changing from conventional to accelerated radiotherapy fractionation in patients with locoregionally advanced nasopharyngeal carcinoma. Cancer. 2015. 121:p. 1328–1338

38 

Bourhis J, Sire C, Graff P, et al. , authors. Concomitant chemoradiotherapy versus acceleration of radiotherapy with or without concomitant chemotherapy in locally advanced head and neck carcinoma (GORTEC 99-02): an open-label phase 3 randomised trial. Lancet Oncol. 2012. 13:p. 145–153

39 

Mallick S, Benson R, Julka PK, Rath GK , authors. Altered fractionation radiotherapy in head and neck squamous cell carcinoma. J Egypt Natl Canc Inst. 2016. 28:p. 73–80

40 

Lee AW, Tung SY, Chua DTT, et al. , authors. Randomized trial of radiotherapy plus concurrent-adjuvant chemotherapy vs radiotherapy alone for regionally advanced nasopharyngeal carcinoma. J Natl Cancer Inst. 2010. 102:p. 1188–1198

41 

Cheng SH, Jian JJM, Tsai SYC, et al. , authors. Long term survival of nasopharyngeal carcinoma following concomitant radiotherapy and chemotherapy. Int J Radiat Oncol Biol Phys. 2000. 48:p. 1323–1330

42 

Fan TY, Xing J, Lu J, et al. , authors. Phase I/II study of induction chemotherapy plus concurrent chemotherapy and SMART-IMRT-based radiotherapy in locoregionally-advanced nasopharyngeal cancer. Oncol Lett. 2013. 5:p. 889–895

43 

Tang JM, Ma XM, Hou YL, Dai LY, Cao HB, Ye M, Bai YR , authors. Analysis of simultaneous modulated accelerated radiotherapy (SMART) for nasopharyngeal carcinomas. J Radiat Res. 2014. 55:p. 794–802

44 

Haberer-Guillerm S, Touboul E, Huguet F , authors. Intensity modulated radiation therapy in nasopharyngeal carcinoma. Eur Ann Otorhinolaryngol Head Neck Dis. 2015. 132:p. 147–151

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